thalidomide and Arthritis, Psoriatic studies

Thalidomide: A piperidinyl isoindole originally introduced as a non-barbiturate hypnotic, but withdrawn from the market due to teratogenic effects. It has been reintroduced and used for a number of immunological and inflammatory disorders. Thalidomide displays immunosuppressive and anti-angiogenic activity. It inhibits release of TUMOR NECROSIS FACTOR-ALPHA from monocytes, and modulates other cytokine action.
thalidomide : A racemate comprising equimolar amounts of R- and S-thalidomide.
2-(2,6-dioxopiperidin-3-yl)-1H-isoindole-1,3(2H)-dione : A dicarboximide that is isoindole-1,3(2H)-dione in which the hydrogen attached to the nitrogen is substituted by a 2,6-dioxopiperidin-3-yl group.

Arthritis, Psoriatic: A type of inflammatory arthritis associated with PSORIASIS, often involving the axial joints and the peripheral terminal interphalangeal joints. It is characterized by the presence of HLA-B27-associated SPONDYLARTHROPATHY, and the absence of rheumatoid factor.

Research Excerpts

Excerpt	Relevance	Reference
"Following a review of the literature, a panel of dermatologists with expertise in the management of psoriasis considered 5 scenarios in which the evidence supporting the use of apremilast to treat moderate psoriasis is insufficient or controversial."	9.05	The Use of Apremilast in Psoriasis: A Delphi Study. ( Ara, M; Belinchón, I; Bustinduy, M; Carrascosa, JM; Herranz, P; Rivera, R, 2020)
"We report the "real-life" use of apremilast in the treatment of multimorbid patients with hidradenitis suppurativa and review its potential role in the management of this severe condition."	9.05	Apremilast for the treatment of hidradenitis suppurativa associated with psoriatic arthritis in multimorbid patients: Case report and review of literature. ( De Simone, C; Garcovich, S; Giovanardi, G; Malvaso, D; Peris, K, 2020)
"To review the pharmacology, efficacy, and safety of apremilast and determine its role relative to other agents in the treatment of psoriasis and psoriatic arthritis."	8.93	Apremilast: A Novel Drug for Treatment of Psoriasis and Psoriatic Arthritis. ( Bank, M; Haber, SL; Hamilton, S; Leong, SY; Pierce, E, 2016)
"Apremilast (Otezla(®)) is an oral phosphodiesterase 4 inhibitor indicated for the twice-daily treatment of adults with psoriasis and psoriatic arthritis (PsA)."	8.91	Apremilast: A Review in Psoriasis and Psoriatic Arthritis. ( Deeks, ED, 2015)
"This real-world safety analysis was requested by the European Medicines Agency following approval of apremilast, an oral treatment for psoriasis or psoriatic arthritis."	8.12	Safety of Apremilast in Patients with Psoriasis and Psoriatic Arthritis: Findings from the UK Clinical Practice Research Datalink. ( Cordey, M; Jick, S; Paris, M; Persson, R, 2022)
"Apremilast is a small molecule approved for the treatment of plaques psoriasis and adult psoriatic arthritis."	8.02	Long-term efficacy and safety of apremilast in the treatment of plaques psoriasis: A real-world, single-center experience. ( Bobyr, I; Campanati, A; Diotallevi, F; Giannoni, M; Martina, E; Offidani, A; Radi, G; Rizzetto, G, 2021)
"Real-world treatment patterns among psoriasis patients with and without psoriatic arthritis (PsA) newly initiating treatment with a biologic or apremilast were assessed."	8.02	Real-world biologic and apremilast treatment patterns in patients with psoriasis and psoriatic arthritis. ( Feldman, SR; Hoit Marchlewicz, E; Lopez-Gonzalez, L; Martinez, DJ; Mendelsohn, AM; Shrady, G; Zhang, J; Zhao, Y, 2021)
"We conducted two separate cohort studies of psoriasis and PsA patients treated with apremilast, tumour necrosis factor inhibitor biologics, interleukin-17, -23 or -12/23 inhibitor biologics, conventional DMARDs or systemic corticosteroids in the United States MarketScan database."	7.96	The risk of treated anxiety and treated depression among patients with psoriasis and psoriatic arthritis treated with apremilast compared to biologics, DMARDs and corticosteroids: a cohort study in the United States MarketScan database. ( Hagberg, KW; Jick, S; Persson, R; Vasilakis-Scaramozza, C, 2020)
"Ex vivo stimulated cell analysis identified that post-apremilast (IL-10+CD19+) B10 cells were increased in all PsA and psoriasis patients and correlated with psoriatic skin and joint clinical improvement."	7.91	Apremilast increases IL-10-producing regulatory B cells and decreases proinflammatory T cells and innate cells in psoriatic arthritis and psoriasis. ( Bogdanos, DP; Brotis, AG; Katsiari, CG; Liaskos, C; Mavropoulos, A; Roussaki-Schulze, A; Sakkas, LI; Simopoulou, T; Zafiriou, E, 2019)
"The aim of the study was to determine the safety of apremilast in combination of biologic therapies in the treatment of plaque psoriasis and psoriatic arthritis."	7.91	Combination Therapy of Apremilast and Biologic Agent as a Safe Option of Psoriatic Arthritis and Psoriasis. ( Chen, C; Gettas, T; Messiah, R; Metyas, S; Quismorio, A; Tomassian, C, 2019)
" On arrival, laboratory test results were significant for hypokalemia, hyperchloremic metabolic acidosis, low uric acid concentration, positive urine anion gap, and proteinuria, which resolved on discontinuation of the drug."	7.85	Proximal Renal Tubular Acidosis (Fanconi Syndrome) Induced by Apremilast: A Case Report. ( Afridi, F; Kar, P; King-Morris, K; Komarla, A; Perrone, D, 2017)
"Apremilast is a substrate of cytochrome P450 isoenzyme 3A4 and accumulates in patients with renal failure."	6.53	Apremilast (Otezla). No progress in plaque psoriasis or psoriatic arthritis. ( , 2016)
"Psoriasis is a chronic inflammatory skin disease, most commonly resulting in the occurrence of red and silver scaly plaques."	6.49	New developments in the management of psoriasis and psoriatic arthritis: a focus on apremilast. ( McCann, FE; McNamee, KE; Palfreeman, AC, 2013)
"Psoriasis is a common inflammatory skin condition, affecting 2-4% of the worldwide population."	5.56	Real life experience of apremilast in psoriasis and arthritis psoriatic patients: Preliminary results on metabolic biomarkers. ( Bianchi, L; Campione, E; Cesaroni, GM; Chiaramonte, C; Chimenti, MS; Cosio, T; Dattola, A; Galluzzo, M; Gaziano, R; Gisondi, P; Lanna, C; Mazzilli, S; Palumbo, V; Zangrilli, A, 2020)
"Apremilast is an orally available targeted PDE4 inhibitor that modulates a wide array of inflammatory mediators involved in psoriasis and psoriatic arthritis, including decreases in the expression of inducible nitric oxide synthase, TNF-α, and interleukin (IL)-23 and increases IL-10."	5.38	Apremilast mechanism of action and application to psoriasis and psoriatic arthritis. ( Schafer, P, 2012)
"Apremilast, a small molecule that acts by inhibition of the phosphodiesterase-4 enzyme, has been approved by the US Food and Drug Administration for the management of psoriatic arthritis, plaque psoriasis and Behçet disease."	5.22	Evolving utility of apremilast in dermatological disorders for off-label indications. ( Dogra, S; Mehta, H; Sharma, A, 2022)
"Following a review of the literature, a panel of dermatologists with expertise in the management of psoriasis considered 5 scenarios in which the evidence supporting the use of apremilast to treat moderate psoriasis is insufficient or controversial."	5.05	The Use of Apremilast in Psoriasis: A Delphi Study. ( Ara, M; Belinchón, I; Bustinduy, M; Carrascosa, JM; Herranz, P; Rivera, R, 2020)
"We report the "real-life" use of apremilast in the treatment of multimorbid patients with hidradenitis suppurativa and review its potential role in the management of this severe condition."	5.05	Apremilast for the treatment of hidradenitis suppurativa associated with psoriatic arthritis in multimorbid patients: Case report and review of literature. ( De Simone, C; Garcovich, S; Giovanardi, G; Malvaso, D; Peris, K, 2020)
"Apremilast is an oral inhibitor of phosphodiesterase-4 (PDE4) that is licensed for the second-line treatment of psoriasis and psoriatic arthritis."	5.01	[Gastrointestinal side effects of apremilast : Characterization and management]. ( Beigel, F; Beissert, S; Gerdes, S; Homey, B; Körber, A; Mössner, R; Pinter, A; Radtke, MA; Staubach-Renz, P, 2019)
"Biological disease modifying antirheumatic drugs and apremilast had a small effect on fatigue at 24 weeks in psoriatic arthritis randomized controlled trials and a higher effect on pain."	4.98	Effect of biologics on fatigue in psoriatic arthritis: A systematic literature review with meta-analysis. ( Fautrel, B; Gossec, L; Mitrovic, S; Reygaerts, T, 2018)
"To review the pharmacology, efficacy, and safety of apremilast and determine its role relative to other agents in the treatment of psoriasis and psoriatic arthritis."	4.93	Apremilast: A Novel Drug for Treatment of Psoriasis and Psoriatic Arthritis. ( Bank, M; Haber, SL; Hamilton, S; Leong, SY; Pierce, E, 2016)
"Apremilast (Otezla(®)) is an oral phosphodiesterase 4 inhibitor indicated for the twice-daily treatment of adults with psoriasis and psoriatic arthritis (PsA)."	4.91	Apremilast: A Review in Psoriasis and Psoriatic Arthritis. ( Deeks, ED, 2015)
"2 kg/m2), apremilast was associated with a mean weight loss of 2."	4.12	Effect of the phosphodiesterase 4 inhibitor apremilast on cardiometabolic outcomes in psoriatic disease-results of the Immune Metabolic Associations in Psoriatic Arthritis study. ( Brooksbank, K; Brown, R; Cathcart, S; Ferguson, LD; Gao, X; Harvie, J; McInnes, IB; Paterson, C; Radjenovic, A; Rimmer, D; Sattar, N; Semple, G; Siebert, S; Welsh, P, 2022)
"Apremilast is an oral small molecule approved for the treatment of psoriasis, psoriatic arthritis and oral ulcers associated with Behçet's disease."	4.12	Apremilast and biologics: Characteristics of patients treated with apremilast before, during, or after a biological treatment. ( García-Verdú, E; González-Cañete, M; Lario, AR; Medina-Montalvo, S; Pinto-Pulido, EL; Piteiro-Bermejo, AB; Polo-Rodríguez, I; Trasobares-Marugán, L; Vega-Díez, D, 2022)
"This real-world safety analysis was requested by the European Medicines Agency following approval of apremilast, an oral treatment for psoriasis or psoriatic arthritis."	4.12	Safety of Apremilast in Patients with Psoriasis and Psoriatic Arthritis: Findings from the UK Clinical Practice Research Datalink. ( Cordey, M; Jick, S; Paris, M; Persson, R, 2022)
"Real-world treatment patterns among psoriasis patients with and without psoriatic arthritis (PsA) newly initiating treatment with a biologic or apremilast were assessed."	4.02	Real-world biologic and apremilast treatment patterns in patients with psoriasis and psoriatic arthritis. ( Feldman, SR; Hoit Marchlewicz, E; Lopez-Gonzalez, L; Martinez, DJ; Mendelsohn, AM; Shrady, G; Zhang, J; Zhao, Y, 2021)
"Apremilast is a small molecule approved for the treatment of plaques psoriasis and adult psoriatic arthritis."	4.02	Long-term efficacy and safety of apremilast in the treatment of plaques psoriasis: A real-world, single-center experience. ( Bobyr, I; Campanati, A; Diotallevi, F; Giannoni, M; Martina, E; Offidani, A; Radi, G; Rizzetto, G, 2021)
" The objective of this study was to quantify the risk of myocardial infarction (MI), stroke and revascularizations in people with apremilast-treated PsA compared with patients receiving other PsA treatments."	4.02	The risks of major cardiac events among patients with psoriatic arthritis treated with apremilast, biologics, DMARDs or corticosteroids. ( Hagberg, KW; Jick, S; Persson, R; Qian, Y; Vasilakis-Scaramozza, C, 2021)
" Apremilast is an oral phosphodiesterase-4 inhibitor which is approved for the treatment of chronic plaque psoriasis and psoriatic arthritis."	3.96	Refractory palmoplantar pustulosis succesfully treated with apremilast. ( Carrascosa de Lome, R; Conde Montero, E; de la Cueva Dobao, P, 2020)
"We conducted two separate cohort studies of psoriasis and PsA patients treated with apremilast, tumour necrosis factor inhibitor biologics, interleukin-17, -23 or -12/23 inhibitor biologics, conventional DMARDs or systemic corticosteroids in the United States MarketScan database."	3.96	The risk of treated anxiety and treated depression among patients with psoriasis and psoriatic arthritis treated with apremilast compared to biologics, DMARDs and corticosteroids: a cohort study in the United States MarketScan database. ( Hagberg, KW; Jick, S; Persson, R; Vasilakis-Scaramozza, C, 2020)
"The aim of the study was to determine the safety of apremilast in combination of biologic therapies in the treatment of plaque psoriasis and psoriatic arthritis."	3.91	Combination Therapy of Apremilast and Biologic Agent as a Safe Option of Psoriatic Arthritis and Psoriasis. ( Chen, C; Gettas, T; Messiah, R; Metyas, S; Quismorio, A; Tomassian, C, 2019)
"Ten Caucasian individuals (6 male, 4 females; mean age 69,3; range 53-81 years) affected by moderate to severe plaque psoriasis (PASI≥10 e/o DLQI≥10 e/O BSA≥10) were treated with apremilast, following dosing regimen of technical data sheet and clinically evaluated both after 12 weeks (T12) and 16 weeks (T16)."	3.91	Skin involvement in patients with psoriatic arthritis: preliminary results of treatment with apremilast in real world setting. ( Campanati, A; Diotallevi, F; Molinelli, E; Offidani, A; Radi, G, 2019)
"Ex vivo stimulated cell analysis identified that post-apremilast (IL-10+CD19+) B10 cells were increased in all PsA and psoriasis patients and correlated with psoriatic skin and joint clinical improvement."	3.91	Apremilast increases IL-10-producing regulatory B cells and decreases proinflammatory T cells and innate cells in psoriatic arthritis and psoriasis. ( Bogdanos, DP; Brotis, AG; Katsiari, CG; Liaskos, C; Mavropoulos, A; Roussaki-Schulze, A; Sakkas, LI; Simopoulou, T; Zafiriou, E, 2019)
" On arrival, laboratory test results were significant for hypokalemia, hyperchloremic metabolic acidosis, low uric acid concentration, positive urine anion gap, and proteinuria, which resolved on discontinuation of the drug."	3.85	Proximal Renal Tubular Acidosis (Fanconi Syndrome) Induced by Apremilast: A Case Report. ( Afridi, F; Kar, P; King-Morris, K; Komarla, A; Perrone, D, 2017)
" One patient was treated with lenalidomide (Revlimid) for multiple myeloma, 2 received infliximab, and 1 received etanercept for severe rheumatoid arthritis; the last patient was in a clinical trial of adalimumab for psoriatic arthritis."	3.73	Interstitial granulomatous dermatitis associated with the use of tumor necrosis factor alpha inhibitors. ( Badros, A; Deng, A; Gaspari, A; Harvey, V; Junkins-Hopkins, JM; Oghilikhan, M; Samuels, A; Sina, B; Strobel, D, 2006)
"Apremilast-treated patients with baseline ModDA had higher probability of achieving cDAPSA treatment targets than patients with HDA."	3.11	Baseline Disease Activity Predicts Achievement of cDAPSA Treatment Targets With Apremilast: Phase III Results in DMARD-naïve Patients With Psoriatic Arthritis. ( Bergman, M; Gladman, DD; Jardon, S; Kavanaugh, A; Mease, PJ; Ogdie, A; Richter, S; Smolen, JS; Teng, L; Wells, AF, 2022)
" Pharmacodynamic effects of apremilast on plasma biomarkers associated with inflammation were evaluated in a PALACE 1 substudy."	2.80	The pharmacodynamic impact of apremilast, an oral phosphodiesterase 4 inhibitor, on circulating levels of inflammatory biomarkers in patients with psoriatic arthritis: substudy results from a phase III, randomized, placebo-controlled trial (PALACE 1). ( Chen, P; Chopra, R; Fang, L; Schafer, PH; Wang, A, 2015)
"Apremilast was effective in the treatment of psoriatic arthritis, improving signs and symptoms and physical function."	2.79	Treatment of psoriatic arthritis in a phase 3 randomised, placebo-controlled trial with apremilast, an oral phosphodiesterase 4 inhibitor. ( Adebajo, AO; Gladman, DD; Gomez-Reino, JJ; Hall, S; Hochfeld, M; Hough, D; Hu, C; Kavanaugh, A; Lespessailles, E; Mease, PJ; Schett, G; Stevens, RM; Wollenhaupt, J, 2014)
"Treatment with apremilast at a dosage of 20 mg twice per day or 40 mg once per day demonstrated efficacy in comparison with placebo and was generally well tolerated in patients with active PsA."	2.77	Oral apremilast in the treatment of active psoriatic arthritis: results of a multicenter, randomized, double-blind, placebo-controlled study. ( de Vlam, KL; Hu, C; Joos, R; Papp, K; Rodrigues, JF; Schett, G; Stevens, R; Vessey, AR; Wollenhaupt, J, 2012)
"Apremilast is a small-molecule biologic approved by the US Food and Drug Administration (FDA) for use in plaque psoriasis, psoriatic arthritis, and Behçet disease."	2.72	Apremilast Uses and Relevance to the Military. ( Hathaway, NE; Lyford, WH, 2021)
"Apremilast is an oral PDE4 inhibitor approved for the treatment of active PsA patients with inadequate response to synthetic immunosuppressants."	2.72	Inhibition of Phosphodiesterase-4 in Psoriatic Arthritis and Inflammatory Bowel Diseases. ( Conti, F; Laganà, B; Picchianti-Diamanti, A; Rosado, MM; Spinelli, FR, 2021)
"Apremilast is an anti-inflammatory agent."	2.72	Analytical Methods for Determination of Apremilast from Bulk, Dosage Form and Biological Fluids: A Critical Review. ( Deshpande, A; Kulkarni, P, 2021)
"Apremilast is an orally administered small molecule that specifically inhibits the phosphodiesterase-4 enzyme and modulates the immune system by increasing the levels of intracellular cyclic adenosine monophosphate (cAMP) and inhibiting IL-2 & 8, interferon-γ and tumor necrosis factor (TNF) production."	2.66	Apremilast in dermatology: A review of literature. ( Alajmi, A; Jfri, A; Nassim, D; Pehr, K, 2020)
" Data were extracted for ACR20/50, HAQ-DI, SF-36 and adverse/serious adverse events after 16-24 weeks."	2.61	Efficacy and safety of systemic treatments in psoriatic arthritis: a systematic review, meta-analysis and GRADE evaluation. ( Dressler, C; Eisert, L; Nast, A; Pham, PA, 2019)
"In patients with active psoriatic arthritis, tofacitinib 10 mg and apremilast 30 mg were the most efficacious interventions and were not associated with a significant risk of serious adverse events."	2.61	Comparison of the Efficacy and Safety of Tofacitinib and Apremilast in Patients with Active Psoriatic Arthritis: A Bayesian Network Meta-Analysis of Randomized Controlled Trials. ( Lee, YH; Song, GG, 2019)
" The number of serious adverse events was not significantly different among the apremilast, secukinumab, ustekinumab, and placebo groups."	2.58	Relative efficacy and safety of apremilast, secukinumab, and ustekinumab for the treatment of psoriatic arthritis. ( Lee, YH; Song, GG, 2018)
"Apremilast is a well-tolerated and effective phosphodiesterase type 4 inhibitor that is indicated for the treatment of moderate-to-severe plaque psoriasis and psoriatic arthritis."	2.53	Apremilast in the therapy of moderate-to-severe chronic plaque psoriasis. ( Girolomoni, G; Gisondi, P, 2016)
"Apremilast is a substrate of cytochrome P450 isoenzyme 3A4 and accumulates in patients with renal failure."	2.53	Apremilast (Otezla). No progress in plaque psoriasis or psoriatic arthritis. ( , 2016)
"Apremilast has been approved by both the United States FDA and European Medicines Agency for treatment of PsA."	2.52	Apremilast: a PDE4 inhibitor for the treatment of psoriatic arthritis. ( Abdulrahim, H; Adebajo, AO; Edwards, C; Shaw, T; Thistleton, S; Wells, A, 2015)
"Apremilast is an orally available small molecule that targets PDE4."	2.52	Drug safety evaluation of apremilast for treating psoriatic arthritis. ( Busa, S; Kavanaugh, A, 2015)
"Apremilast is a novel therapy that inhibits phosphodiesterase 4, increases intracellular cAMP levels, and modulates expression of inflammatory mediators in favor of anti-inflammatory activity."	2.52	Apremilast for the treatment of psoriatic arthritis. ( Gómez-Reino, JJ; Souto, A, 2015)
"Apremilast is an orally available phosphodiesterase type 4 inhibitor that may block the pathogenic inflammatory Th17 and Th1 pathways upstream of current biologics, which target extracellular molecules of the immunological response."	2.50	Apremilast for the treatment of psoriatic arthritis. ( Gottlieb, AB; Tintle, SJ; Varada, S, 2014)
"Apremilast is indicated for the treatment of active psoriatic arthritis in adults."	2.50	Apremilast: first global approval. ( Ballantyne, AD; Poole, RM, 2014)
"Psoriasis is a chronic inflammatory skin disease, most commonly resulting in the occurrence of red and silver scaly plaques."	2.49	New developments in the management of psoriasis and psoriatic arthritis: a focus on apremilast. ( McCann, FE; McNamee, KE; Palfreeman, AC, 2013)
"Apremilast is a novel oral agent that has recently been made available to dermatologists for the treatment of moderate-to-severe plaque psoriasis and psoriatic arthritis."	1.72	Psoriatic patients with a history of cancer: A real-life experience with Apremilast treatment for 104 weeks. ( Bernardini, N; Maddalena, P; Mambrin, A; Marchesiello, A; Marraffa, F; Potenza, C; Proietti, I; Rossi, G; Skroza, N; Tolino, E; Volpe, S, 2022)
" Apremilast was well tolerated and the reported adverse events were in line with the known safety profile."	1.72	Real-World Efficacy and Safety of Apremilast in Belgian Patients with Psoriatic Arthritis: Results from the Prospective Observational APOLO Study. ( de Vlam, K; Di Romana, S; Kaiser, MJ; Lories, R; Remans, P; Toukap, AN; Van den Berghe, M; Van den Bosch, F; Vanhoof, J, 2022)
" At least one adverse event was experienced by 56/96 patients, and 11/56 events required drug withdrawal."	1.56	Long-term efficacy and safety of apremilast in psoriatic arthritis: Focus on skin manifestations and special populations. ( Balato, A; Bianchi, L; Campione, E; Cirillo, T; Fabbrocini, G; Malara, G; Trifirò, C, 2020)
"Psoriasis is a common inflammatory skin condition, affecting 2-4% of the worldwide population."	1.56	Real life experience of apremilast in psoriasis and arthritis psoriatic patients: Preliminary results on metabolic biomarkers. ( Bianchi, L; Campione, E; Cesaroni, GM; Chiaramonte, C; Chimenti, MS; Cosio, T; Dattola, A; Galluzzo, M; Gaziano, R; Gisondi, P; Lanna, C; Mazzilli, S; Palumbo, V; Zangrilli, A, 2020)
" Recently, apremilast, a selective inhibitor of phosphodiesterase E4 has been suggested to be a safe and effective therapeutic option in HIV-infected population with psoriatic arthritis."	1.51	Apremilast efficacy and safety in a psoriatic arthritis patient affected by HIV and HBV virus infections. ( Bianchi, L; Campione, E; Esposito, M; Giunta, A; Manfreda, V, 2019)
"Apremilast is an oral nonbiologic medication approved for the treatment of adult patients with active psoriatic arthritis and for patients with moderate to severe plaque psoriasis."	1.43	Apremilast, an oral phosphodiesterase 4 (PDE4) inhibitor: A novel treatment option for nurse practitioners treating patients with psoriatic disease. ( Roebuck, HL; Young, M, 2016)
"Apremilast is an orally available targeted PDE4 inhibitor that modulates a wide array of inflammatory mediators involved in psoriasis and psoriatic arthritis, including decreases in the expression of inducible nitric oxide synthase, TNF-α, and interleukin (IL)-23 and increases IL-10."	1.38	Apremilast mechanism of action and application to psoriasis and psoriatic arthritis. ( Schafer, P, 2012)

Research

Studies (126)

Authors

Clinical Trials (14)

Trial Overview

Trial Outcomes

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 16

Timeframe	Studies, this research(%)	All Research%
pre-1990	0 (0.00)	18.7374
1990's	0 (0.00)	18.2507
2000's	1 (0.79)	29.6817
2010's	71 (56.35)	24.3611
2020's	54 (42.86)	2.80

Authors	Studies
Radi, G	2
Campanati, A	2
Diotallevi, F	2
Rizzetto, G	1
Martina, E	1
Bobyr, I	1
Giannoni, M	1
Offidani, A	2
Feldman, SR	2
Zhang, J	1
Martinez, DJ	1
Lopez-Gonzalez, L	1
Hoit Marchlewicz, E	1
Shrady, G	1
Zhao, Y	1
Mendelsohn, AM	1
de Vlam, K	1
Toukap, AN	1
Kaiser, MJ	1
Vanhoof, J	1
Remans, P	1
Van den Berghe, M	1
Di Romana, S	1
Van den Bosch, F	2
Lories, R	1
Bernardini, N	1
Skroza, N	1
Marchesiello, A	1
Mambrin, A	1
Proietti, I	1
Tolino, E	1
Maddalena, P	1
Marraffa, F	1
Rossi, G	1
Volpe, S	1
Potenza, C	1
Arias de la Rosa, I	1
López-Montilla, MD	1
Román-Rodríguez, C	1
Pérez-Sánchez, C	1
Gómez-García, I	1
López-Medina, C	1
Ladehesa-Pineda, ML	1
Ábalos-Aguilera, MDC	1
Ruiz, D	1
Patiño-Trives, AM	1
Luque-Tévar, M	1
Añón-Oñate, I	1
Pérez-Galán, MJ	1
Guzmán-Ruiz, R	1
Malagón, MM	1
López-Pedrera, C	1
Escudero-Contreras, A	1
Collantes-Estévez, E	1
Barbarroja, N	1
Pina Vegas, L	3
Claudepierre, P	3
Sbidian, E	4
Suruki, RY	1
Desai, RJ	1
Davis, KJ	1
Berlin, JA	1
Gagne, JJ	1
Mease, PJ	8
Kavanaugh, A	8
Ogdie, A	3
Wells, AF	2
Bergman, M	1
Gladman, DD	5
Richter, S	2
Teng, L	5
Jardon, S	1
Smolen, JS	3
Torre Alonso, JC	1
Almodóvar González, R	1
Montilla Morales, C	2
Sanz Sanz, J	1
Díaz González, F	1
Pascual Alfonso, E	1
Gratacós, J	1
Romita, P	1
Foti, C	1
Calianno, G	1
Chiricozzi, A	1
Torrente-Segarra, V	1
Bonet, M	1
Ouyang, F	1
Garbayo Salmons, P	1
Expósito Serrano, V	1
Romaní de Gabriel, J	1
Ribera Pibernat, M	1
Tsilimidos, G	1
Blum, S	1
Aliotta, A	1
Dumusc, A	1
Alberio, L	1
Ariani, A	2
Parisi, S	1
Del Medico, P	1
Farina, A	1
Visalli, E	2
Molica Colella, AB	1
Lumetti, F	2
Caccavale, R	1
Scolieri, P	1
Andracco, R	1
Girelli, F	1
Bravi, E	1
Colina, M	1
Volpe, A	1
Ianniello, A	1
Franchina, V	1
Platè, I	1
Di Donato, E	2
Amato, G	2
Salvarani, C	1
Lucchini, G	2
De Lucia, F	1
Molica Colella, F	1
Santilli, D	2
Ferrero, G	1
Marchetta, A	1
Arrigoni, E	1
Mozzani, F	2
Foti, R	3
Sandri, G	1
Bruzzese, V	1
Paroli, M	1
Fusaro, E	1
Becciolini, A	2
Mehta, H	1
Sharma, A	1
Dogra, S	1
Pinto-Pulido, EL	1
Lario, AR	1
Vega-Díez, D	1
González-Cañete, M	1
García-Verdú, E	1
Polo-Rodríguez, I	1
Piteiro-Bermejo, AB	1
Medina-Montalvo, S	1
Trasobares-Marugán, L	1
Persson, R	3
Cordey, M	1
Paris, M	3
Jick, S	3
Dal Bosco, Y	1
Baccano, G	1
Natsis, NE	1
Merola, JF	2
Weinberg, JM	1
Wu, JJ	2
Orbai, AM	1
Bagel, J	1
Gottlieb, AB	3
Loft, ND	1
Egeberg, A	1
Rasmussen, MK	1
Bryld, LE	1
Gniadecki, R	1
Dam, TN	1
Iversen, L	1
Skov, L	1
Gandjour, A	1
Ostwald, DA	1
Capri, S	1
Migliore, A	1
Loconsole, F	1
Barbieri, M	1
Carrascosa, JM	1
Belinchón, I	1
Rivera, R	1
Ara, M	1
Bustinduy, M	1
Herranz, P	1
Coates, LC	2
Behrens, F	1
McInnes, I	1
Queiro, R	1
Guerette, B	4
Brunori, M	1
Carrascosa de Lome, R	1
Conde Montero, E	1
de la Cueva Dobao, P	1
Vasilakis-Scaramozza, C	2
Hagberg, KW	2
Garcovich, S	1
Giovanardi, G	1
Malvaso, D	1
De Simone, C	1
Peris, K	1
Kulkarni, P	1
Deshpande, A	1
Caso, F	3
Navarini, L	1
Ruscitti, P	1
Chimenti, MS	4
Girolimetto, N	2
Del Puente, A	4
Giacomelli, R	1
Scarpa, R	3
Costa, L	3
Pelletier, C	2
Ung, B	1
Tian, M	2
Khilfeh, I	2
Curtis, JR	1
Mazzilli, S	1
Lanna, C	1
Chiaramonte, C	1
Cesaroni, GM	1
Zangrilli, A	1
Palumbo, V	1
Cosio, T	1
Dattola, A	2
Gaziano, R	1
Galluzzo, M	1
Gisondi, P	2
Bianchi, L	4
Campione, E	3
Balato, A	1
Cirillo, T	1
Malara, G	1
Trifirò, C	1
Fabbrocini, G	1
Nigro, O	1
Pinotti, G	1
Gueli, R	1
Grigioni, E	1
Santis, M	1
Ceribelli, A	1
Selmi, C	1
Venerito, V	1
Natuzzi, D	1
Bizzoca, R	1
Lacarpia, N	1
Cacciapaglia, F	1
Lopalco, G	1
Iannone, F	1
Olisova, OY	1
Anpilogova, EM	1
Svistunova, DA	1
Queiro Silva, R	1
Armesto, S	1
González Vela, C	1
Naharro Fernández, C	1
González-Gay, MA	1
Nassim, D	1
Alajmi, A	1
Jfri, A	1
Pehr, K	1
Sandhu, VK	1
Eder, L	1
Yeung, J	1
Price, AD	1
Wagler, VD	1
Donaldson, C	1
Mastin, PJ	1
Bansal, P	1
Goyal, A	1
Cusick, A	1
Aslam, F	1
Qian, Y	1
Liu, M	1
Glynn, M	1
Emeanuru, K	1
Harrold, LR	1
Degboé, Y	1
Sunzini, F	1
Sood, S	1
Bozec, A	1
Sokolova, MV	1
Zekovic, A	1
McInnes, IB	3
Schett, G	6
Goodyear, CS	1
Picchianti-Diamanti, A	1
Spinelli, FR	4
Rosado, MM	1
Conti, F	4
Laganà, B	1
Giordano, S	1
Riva, M	1
Hathaway, NE	1
Lyford, WH	1
Ferguson, LD	1
Cathcart, S	1
Rimmer, D	1
Semple, G	1
Brooksbank, K	1
Paterson, C	1
Brown, R	1
Harvie, J	1
Gao, X	1
Radjenovic, A	1
Welsh, P	1
Sattar, N	1
Siebert, S	1
Edwards, CJ	3
Kivitz, AJ	1
Bird, P	2
Delev, N	3
Aelion, JA	2
Kaplan, DL	1
Ung, BL	1
Udeze, C	1
Le Corvoisier, P	1
Penso, L	2
Paul, M	1
Lucchetti, R	3
Ceccarelli, F	3
Cipriano, E	2
Perricone, C	4
Alessandri, C	3
Bergqvist, C	1
Meyer, A	1
Herlemont, P	1
Weill, A	1
Zureik, M	1
Dray-Spira, R	1
Martin, BC	1
Thomas, LW	1
Dann, FJ	1
Song, GG	2
Lee, YH	2
Perrone, D	1
Afridi, F	1
King-Morris, K	1
Komarla, A	1
Kar, P	1
Persons, B	1
Chawla, R	1
Carter, J	1
Peluso, R	2
Tasso, M	1
Caso, P	2
Sabbatino, V	1
Benigno, C	1
Bertolini, N	1
Perricone, R	1
van Mens, LJJ	1
van de Sande, MGH	1
Baeten, DLP	1
Bottiglieri, P	1
Ballegaard, C	1
Jørgensen, TS	1
Skougaard, M	1
Strand, V	2
Kristensen, LE	1
Dreyer, L	1
Gottlieb, A	1
de Wit, M	2
Christensen, R	1
Tarp, S	1
Abignano, G	3
Fadl, N	2
Merashli, M	2
Wenham, C	1
Freeston, J	2
McGonagle, D	3
Marzo-Ortega, H	4
Kawalec, P	1
Holko, P	1
Moćko, P	1
Pilc, A	1
Nash, P	2
Ohson, K	1
Walsh, J	1
Nguyen, D	1
Gómez-Reino, JJ	4
Reygaerts, T	1
Mitrovic, S	1
Fautrel, B	1
Gossec, L	2
Truglia, S	2
Miranda, F	2
Scrivo, R	2
Valesini, G	2
Elman, SA	1
Weinblatt, M	1
Molinelli, E	1
Ritchlin, C	1
Choy, EH	1
Kanters, S	1
Thom, H	1
Gandhi, K	1
Pricop, L	1
Jugl, SM	1
Laws, P	1
Del Galdo, F	1
Metyas, S	1
Tomassian, C	1
Messiah, R	1
Gettas, T	1
Chen, C	1
Quismorio, A	1
Graceffa, D	1
De Felice, C	1
Lora, V	1
Morrone, A	1
Bonifati, C	1
Pham, PA	2
Dressler, C	2
Eisert, L	2
Nast, A	2
Werner, RN	1
Manfreda, V	1
Esposito, M	1
Giunta, A	1
Vandevelde, C	1
Damiani, G	1
Bragazzi, NL	1
Grossi, E	1
Petrou, S	1
Radovanovic, D	1
Rizzi, M	1
Atzeni, F	2
Sarzi-Puttini, P	2
Santus, P	1
Pigatto, PD	1
Franchi, C	1
Pinter, A	1
Beigel, F	1
Körber, A	1
Homey, B	1
Beissert, S	1
Gerdes, S	1
Staubach-Renz, P	1
Radtke, MA	1
Mössner, R	1
Pelletier, CL	1
Wilson, KL	1
Mehta, RK	1
Brouillette, MA	1
Smith, D	1
Bonafede, MM	1
Mavropoulos, A	1
Zafiriou, E	1
Simopoulou, T	1
Brotis, AG	1
Liaskos, C	1
Roussaki-Schulze, A	1
Katsiari, CG	1
Bogdanos, DP	1
Sakkas, LI	1
Riccieri, V	1
Di Franco, M	1
Palfreeman, AC	1
McNamee, KE	1
McCann, FE	1
Hu, C	4
Stevens, RM	4
Adebajo, AO	3
Wollenhaupt, J	3
Lespessailles, E	2
Hall, S	2
Hochfeld, M	2
Hough, D	1
Varada, S	1
Tintle, SJ	2
Poole, RM	1
Ballantyne, AD	1
FitzGerald, O	1
Morrow, T	1
Hansen, RB	1
Krause, A	1
Märker-Hermann, E	1
Teng, LL	1
Felquer, ML	1
Soriano, ER	2
Busa, S	1
Abdulrahim, H	1
Thistleton, S	1
Shaw, T	1
Edwards, C	1
Wells, A	1
Schafer, PH	1
Chen, P	1
Fang, L	1
Wang, A	1
Chopra, R	1
Deeks, ED	1
Souto, A	1
Betts, KA	1
Griffith, J	1
Friedman, A	1
Zhou, ZY	1
Signorovitch, JE	1
Ganguli, A	1
Haber, SL	1
Hamilton, S	1
Bank, M	1
Leong, SY	1
Pierce, E	1
Blanco, FJ	1
Crowley, J	1
Birbara, CA	1
Jaworski, J	1
Aelion, J	1
Vessey, A	1

Trial	Phase	Enrollment	Study Type	Start Date	Status
An Observational Study of the Real-life Management of Psoriatic Arthritis Patients Treated With Otezla® (Apremilast) in Belgium[NCT03096990]		106 participants (Actual)	Observational	2017-04-21	Completed
A Phase 3, Multicenter, Randomized, Double-blind, Placebo-controlled, Parallel-group, Efficacy and Safety Study of Two Doses of Apremilast (CC-10004) in Subjects With Active Psoriatic Arthritis Who Have Not Been Previously Treated With Disease-modifying A[NCT01307423]	Phase 3	529 participants (Actual)	Interventional	2010-12-09	Completed
A Phase 3, Multicenter, Randomized, Double-blind, Placebo-controlled, Parallel-group, Efficacy and Safety Study of Two Doses of Apremilast (CC-10004) in Subjects With Active Psoriatic Arthritis[NCT01212757]	Phase 3	488 participants (Actual)	Interventional	2010-09-27	Completed
A Phase 3, Multicenter, Randomized, Double-blind, Placebo-controlled, Parallel-group, Efficacy and Safety Study of Two Doses of Apremilast (CC-10004) in Subjects With Active Psoriatic Arthritis[NCT01172938]	Phase 3	504 participants (Actual)	Interventional	2010-06-02	Completed
A Phase 3, Multicenter, Randomized, Double-blind, Placebo-controlled, Parallel-group, Efficacy and Safety Study of Two Doses of Apremilast (CC-10004) in Subjects With Active Psoriatic Arthritis and a Qualifying Psoriasis Lesion[NCT01212770]	Phase 3	505 participants (Actual)	Interventional	2010-09-30	Completed
A Phase 3b, Multicenter, Randomized, Double-blind, Placebo-controlled, Parallel-group Study to Evaluate the Efficacy and Safety of Apremilast (CC-10004) Monotherapy in Subjects With Active Psoriatic Arthritis[NCT01925768]	Phase 3	219 participants (Actual)	Interventional	2013-09-04	Completed
A Phase 1 Multi-Center, Open-Label, Dose-Escalation Study to Determine the Pharmacokinetics and Safety of Pomalidomide When Given in Combination With Low Dose Dexamethasone in Subjects With Relapsed or Refractory Multiple Myeloma and Impaired Renal Functi[NCT01575925]	Phase 1	25 participants (Actual)	Interventional	2012-06-01	Completed
A PHASE 3, MULTICENTER, RANDOMIZED, DOUBLE-BLIND, PLACEBO-CONTROLLED, PARALLEL-GROUP STUDY TO EVALUATE THE EFFICACY AND SAFETY OF APREMILAST (CC-10004) IN THE TREATMENT OF ACTIVE ANKYLOSING SPONDYLITIS[NCT01583374]	Phase 3	490 participants (Actual)	Interventional	2012-05-02	Completed
A Phase II, Multicenter, Randomized, Double-blind, Placebo-controlled, Parallel-group, Efficacy and Safety Study of Two Dose Regimens of CC-10004 in Subjects With Active Psoriatic Arthritis[NCT00456092]	Phase 2	204 participants (Actual)	Interventional	2007-03-05	Completed
Molecular Effects of Apremilast in the Synovium of Psoriatic Arthritis Patients (MEAS Study)[NCT04645420]		19 participants (Actual)	Interventional	2020-11-12	Completed
Safety and Efficacy of Tofacitinib vs Methotrexate in the Treatment of Psoriatic Arthritis[NCT03736161]	Phase 3	61 participants (Actual)	Interventional	2017-09-15	Completed
A Pilot Study to Evaluate the Efficacy and Safety of Apremilast in Patients of Chronic and Recurrent Erythema Nodosum Leprosum[NCT04822909]	Phase 4	10 participants (Actual)	Interventional	2019-09-15	Completed
A Phase 1 Study of CC-11050 in Human Immunodeficiency Virus-1-Infected Adults With Suppressed Plasma Viremia on Antiretroviral Therapy[NCT02652546]	Phase 1	38 participants (Actual)	Interventional	2016-01-09	Completed
Efficacy and Safety of Apremilast in Patients With Moderate to Severe Chronic Plaque Psoriasis[NCT06032858]	Phase 4	30 participants (Actual)	Interventional	2022-03-06	Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). SF-36 domain scores were first calculated to range from 0 to100 and then transformed to norm-based scores (the norm-based scores in the US general population have an average of 50 and a standard deviation of 10). Norm-based scores were used in analyses, with higher scores indicating a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from baseline score indicates an improvement. (NCT01307423)
Timeframe: Baseline and Week 16

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	0.01
Apremilast 20 mg	2.39
Apremilast 30 mg	3.19

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 16

Intervention	units on a scale (Least Squares Mean)
Placebo	0.16
Apremilast 20 mg	2.13
Apremilast 30 mg	3.88

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: • 28 tender joint count (TJC), • 28 swollen joint count (SJC), • Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; • Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8 Low Disease Activity: > 2.8 and ≤ 10 Moderate Disease Activity: > 10 and ≤ 22 High Disease Activity: > 22 (NCT01307423)
Timeframe: Baseline and Week 16

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	-1.98
Apremilast 20 mg	-6.89
Apremilast 30 mg	-7.63

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: • 28 tender joint count (TJC), • 28 swollen joint count (SJC), • Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; • Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8; Low Disease Activity: > 2.8 and ≤ 10; Moderate Disease Activity: > 10 and ≤ 22; High Disease Activity: > 22. (NCT01307423)
Timeframe: Baseline and Week 24

Change From Baseline in Dactylitis Severity Score at Week 16

Intervention	units on a scale (Least Squares Mean)
Placebo	-2.23
Apremilast 20 mg	-7.30
Apremilast 30 mg	-7.36

Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet will be rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01307423)
Timeframe: Baseline to Week 16

Change From Baseline in Dactylitis Severity Score at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	-1.0
Apremilast 20 mg	-1.9
Apremilast 30 mg	-1.7

Change From Baseline in Disease Activity Score (DAS 28) at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	-1.0
Apremilast 20 mg	-2.0
Apremilast 30 mg	-1.7

The DAS28 measures the severity of disease at a specific time and is derived from the following variables: • 28 tender joint count • 28 swollen joint count, which do not include the DIP joints, the hip joint, or the joints below the knee; • C-reactive protein (CRP) • Patient's global assessment of disease activity. DAS28(CRP) scores range from 0 to approximately 10, with the upper bound dependent on the highest possible level of CRP. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. (NCT01307423)
Timeframe: Baseline and Week 24

Change From Baseline in Health Assessment Questionnaire - Disability Index (HAQ-DI) at Week 52

Intervention	units on a scale (Least Squares Mean)
Placebo	-0.22
Apremilast 20 mg	-0.69
Apremilast 30 mg	-0.68

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative changes from Baseline in the overall score indicate improvement in functional ability. (NCT01307423)
Timeframe: Baseline and Week 52

Change From Baseline in Health Assessment Questionnaire- Disability Index [HAQ-DI]) at Week 16

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-0.21
Placebo / Apremilast 30 mg	-0.25
Apremilast 20 mg	-0.32
Apremilast 30 mg	-0.39

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative changes from baseline in the overall score indicate improvement in functional ability. (NCT01307423)
Timeframe: Baseline and Week 16

Change From Baseline in Health Assessment Questionnaire- Disability Index [HAQ-DI]) at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	0.012
Apremilast 20 mg	-0.156
Apremilast 30mg	-0.205

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 16

Intervention	units on a scale (Least Squares Mean)
Placebo	0.012
Apremilast 20 mg	-0.156
Apremilast 30 mg	-0.207

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01307423)
Timeframe: Baseline and Week 16

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	-0.5
Apremilast 20 mg	-0.5
Apremilast 30 mg	-1.5

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 52

Intervention	units on a scale (Least Squares Mean)
Placebo	-0.6
Apremilast 20 mg	-0.9
Apremilast 30 mg	-1.5

Change From Baseline in Participants Assessment of Pain at Week 24

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-1.7
Placebo/Apremilast 30 mg	-1.8
Apremilast 20 mg	-1.5
Apremilast 30 mg	-1.8

"The participant was asked to place a vertical line on a 100-mm visual analog scale on which the left-hand boundary (score = 0 mm) represents no pain, and the right-hand boundary (score = 100 mm) represents pain as severe as can be imagined. The distance from the mark to the left-hand boundary was recorded in millimeters." (NCT01307423)
Timeframe: Baseline and Week 24

Change From Baseline in Patient's Assessment of Pain at Week 16

Intervention	mm (Least Squares Mean)
Placebo	-3.8
Apremilast 20 mg	-9.4
Apremilast 30 mg	-9.6

Change From Baseline in the CDAI Score at Week 52

Intervention	mm (Least Squares Mean)
Placebo	-2.6
Apremilast 20 mg	-7.7
Apremilast 30 mg	-10.5

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: 28 tender joint count (TJC), 28 swollen joint count (SJC), Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8 Low Disease Activity: > 2.8 and ≤ 10 Moderate Disease Activity: > 10 and ≤ 22 High Disease Activity: > 22. (NCT01307423)
Timeframe: Baseline and Week 52

Change From Baseline in the Dactylitis Severity Score at Week 52

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-11.0
Placebo / Apremilast 30 mg	-14.67
Apremilast 20 mg	-14.32
Apremilast 30 mg	-13.98

Change From Baseline in the DAS28 at Week 52

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-2.2
Placebo / Apremilast 30 mg	-2.9
Apremilast 20 mg	-2.2
Apremilast 30 mg	-2.9

Change From Baseline in the Disease Activity Score (DAS28) After 16 Weeks of Treatment

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-1.08
Placebo / Apremilast 30 mg	-1.28
Apremilast 20 mg	-1.37
Apremilast 30 mg	-1.39

Change From Baseline in the FACIT-Fatigue Scale Score at Week 52

Intervention	units on a scale (Least Squares Mean)
Placebo	-0.15
Apremilast 20 mg	-0.61
Apremilast 30 mg	-0.68

"The FACIT-Fatigue scale is a 13-item self-administered questionnaire that assesses both the physical and functional consequences of fatigue. Each question is answered on a 5-point scale, where 0 means not at all, and 4 means very much. The FACIT-Fatigue scale score ranges from 0 to 52, with higher scores denoting lower levels of fatigue. A positive change from baseline score indicates an improvement." (NCT01307423)
Timeframe: Baseline and Week 52

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 16

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	6.03
Placebo / Apremilast 30 mg	4.27
Apremilast 20 mg	2.39
Apremilast 30 mg	5.89

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 24

Intervention	units on a scale (Least Squares Mean)
Placebo	0.07
Apremilast 20 mg	1.19
Apremilast 30 mg	2.62

Change From Baseline in the Participants Assessment of Pain Using the Visual Analog Scale at Week 52

Intervention	units on a scale (Least Squares Mean)
Placebo	0.25
Apremilast 20 mg	1.37
Apremilast 30 mg	2.58

Change From Baseline in the SF-36v2 Physical Functioning Scale Score at Week 52

Intervention	mm (Mean)
Placebo/Apremilast 20 mg	-13.1
Placebo / Apremilast 30 mg	-18.9
Apremilast 20 mg	-15.6
Apremilast 30 mg	-14.2

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 24

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	7.76
Placebo / Apremilast 30 mg	6.87
Apremilast 20 mg	5.68
Apremilast 30 mg	5.87

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 24 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01307423)
Timeframe: Baseline and Week 24

Percentage of Participants Achieving a MASES Score of Zero at Week 24

Intervention	percentage of participants (Number)
Placebo	35.6
Apremilast 20 mg	46.1
Apremilast 30 mg	40.5

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01307423)
Timeframe: Baseline and Week 24

Percentage of Participants Achieving Good or Moderate EULAR Response at Week 52

Intervention	percentage of participants (Number)
Placebo	22.6
Apremilast 20 mg	29.1
Apremilast 30 mg	37.8

The EULAR response criteria classify each subject as a good, moderate or non-responder to treatment based on the degree of improvement from baseline and the level of disease activity at the endpoint. EULAR response is derived using the individual subject's DAS28 as the measure of severity of disease. A Good response is defined as follows: Good response: DAS28 at the time point ≤ 3.2 and improvement from baseline > 1.2 A Moderate Response is defined as either: an improvement (decrease) in the DAS28 of greater than 0.6 and less than or equal to 1.2 and attainment of a DAS28 score of less than or equal to 5.1 or, an improvement (decrease) in the DAS28 of more than 1.2 and attainment of a DAS28 score of greater than 3.2. Two-sided 95% confidence interval is based on the Clopper-Pearson method (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With ≥ 20% Improvement in Maastricht Ankylosing Spondylitis Entheses Score at Week 16

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	64.5
Placebo / Apremilast 30 mg	73.5
Apremilast 20 mg	75.4
Apremilast 30 mg	79.0

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With a ACR 20 Response at Week 52

Intervention	percentage of participants (Number)
Placebo	46.1
Apremilast 20 mg	48.7
Apremilast 30 mg	63.1

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: ≥ 20% improvement in 78 tender joint count; ≥ 20% improvement in 76 swollen joint count; and ≥ 20% improvement in at least 3 of the 5 following parameters: Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); Patient's global assessment of disease activity (measured on a 100 mm VAS); Physician's global assessment of disease activity (measured on a 100 mm VAS); Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With a ACR 50 Response at Week 16

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	59.7
Placebo / Apremilast 30 mg	56.7
Apremilast 20 mg	53.4
Apremilast 30 mg	58.7

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); Patient's global assessment of disease activity (measured on a 100 mm VAS); Physician's global assessment of disease activity (measured on a 100 mm VAS); Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); C-Reactive Protein. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With a ACR 50 Response at Week 24

Intervention	Percentage of participants (Number)
Placebo	4.5
Apremilast 20 mg	11.4
Apremilast 30 mg	11.4

Percentage of Participants With a ACR 70 Response at Week 16

Intervention	percentage of participants (Number)
Placebo	6.3
Apremilast 20 mg	16.0
Apremilast 30 mg	12.5

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); Patient's global assessment of disease activity (measured on a 100 mm VAS); Physician's global assessment of disease activity (measured on a 100 mm VAS); Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); C-Reactive Protein. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With a ACR 70 Response at Week 24

Intervention	percentage of participants (Number)
Placebo	1.1
Apremilast 20 mg	4.0
Apremilast 30 mg	4.0

Percentage of Participants With a Modified PsARC Response at Week 52

Intervention	percentage of participants (Number)
Placebo	4.0
Apremilast 20 mg	4.0
Apremilast 30mg	4.5

Measure Description: Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0=lowest disease activity and 100=highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0=lowest disease activity and 100=highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 16

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	73.8
Placebo / Apremilast 30 mg	79.1
Apremilast 20 mg	75.6
Apremilast 30 mg	75.9

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0=lowest disease activity and 100=highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0=lowest disease activity and 100=highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 24

Intervention	percentage of participants (Number)
Placebo	24.4
Apremilast 20 mg	38.9
Apremilast 30 mg	45.5

Percentage of Participants With an ACR 20 Response at Week 24

Intervention	percentage of participants (Number)
Placebo	17.0
Apremilast 20 mg	36.6
Apremilast 30 mg	35.2

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); Patient's global assessment of disease activity (measured on a 100 mm VAS); Physician's global assessment of disease activity (measured on a 100 mm VAS); Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); C-Reactive Protein. (NCT01307423)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 50 Response at Week 52

Intervention	percentage of participants (Number)
Placebo	13.1
Apremilast 20 mg	29.1
Apremilast 30 mg	24.4

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: ≥ 50% improvement in 78 tender joint count; ≥ 50% improvement in 76 swollen joint count; and ≥ 50% improvement in at least 3 of the 5 following parameters: o Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); Patient's global assessment of disease activity (measured on a 100 mm VAS); Physician's global assessment of disease activity (measured on a 100 mm VAS); Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With an ACR 70 Response at Week 52

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	30.6
Placebo / Apremilast 30 mg	25.4
Apremilast 20 mg	27.1
Apremilast 30 mg	31.9

A participant was a responder if the following 3 criteria for improvement from Baseline were met: ≥ 70% improvement in 78 tender joint count; ≥ 70% improvement in 76 swollen joint count; and ≥ 70% improvement in at least 3 of the 5 following parameters: Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); Patient's global assessment of disease activity (measured on a 100 mm VAS); Physician's global assessment of disease activity (measured on a 100 mm VAS); Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With an American College of Rheumatology 20% (ACR20) Response at Week 16

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	8.2
Placebo / Apremilast 30 mg	10.3
Apremilast 20 mg	13.7
Apremilast 30 mg	18.1

A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: -Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); -Patient's global assessment of disease activity (measured on a 100 mm VAS); -Physician's global assessment of disease activity (measured on a 100 mm VAS); -Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); -C-Reactive Protein. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 16

Intervention	percentage of participants (Number)
Placebo	15.9
Apremilast 20mg	28.0
Apremilast 30mg	30.7

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improved by ≥ 1 after 16 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 24

Intervention	percentage of participants (Number)
Placebo	60.0
Apremilast 20 mg	66.3
Apremilast 30 mg	61.9

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improved by ≥ 1 after 24 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01307423)
Timeframe: Baseline and Week 24

Percentage of Participants With Good or Moderate EULAR Response at Week 24

Intervention	percentage of participants (Number)
Placebo	57.8
Apremilast 20 mg	69.7
Apremilast 30 mg	63.1

The EULAR response reflects an improvement in disease activity and an attainment of a lower degree of disease activity based on th DAS-28. Good or moderate response is defined as follows: Good response: DAS28 at the time point ≤ 3.2 and improvement from baseline > 1.2 Moderate response: DAS28 at the time point > 3.2 and improvement from baseline > 1.2, or DAS28 at the time point ≤ 5.1 and improvement from baseline > 0.6 and ≤ 1.2 A Moderate Response is defined as either: • an improvement (decrease) in the DAS28 of greater than 0.6 and less than or equal to 1.2 and attainment of a DAS28 score of less than or equal to 5.1 or, • an improvement (decrease) in the DAS28 of more than 1.2 and attainment of a DAS28 score of greater than 3.2. (NCT01307423)
Timeframe: Baseline and Week 24

Percentage of Participants With Good or Moderate European League Against Rheumatism (EULAR) Response at Week 16

Intervention	percentage of participants (Number)
Placebo	17.0
Apremilast 20 mg	34.9
Apremilast 30 mg	28.4

The EULAR response criteria classify each subject as a good, moderate or non-responder to treatment based on the degree of improvement from baseline and the level of disease activity at the endpoint. EULAR response is derived using the individual subject's DAS28 as the measure of severity of disease. Good or moderate response is defined as follows: Good response: DAS28 at the time point ≤ 3.2 and improvement from baseline > 1.2 Moderate response: DAS28 at the time point > 3.2 and improvement from baseline > 1.2, or DAS28 at the time point ≤ 5.1 and improvement from baseline > 0.6 and ≤ 1.2 (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 24

Intervention	percentage of participants (Number)
Placebo	25.0
Apremilast 20 mg	41.1
Apremilast 30 mg	44.3

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01307423)
Timeframe: Baseline and Week 24

Percentage of Participants With MASES Improvement ≥ 20% at Week 52

Intervention	percentage of participants (Number)
Placebo	48.7
Apremilast 20 mg	54.7
Apremilast 30 mg	66.7

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 52 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With Pre-existing Dactylitis Whose Dactylitis Severity Score Improves From Baseline by ≥ 1 at Week 52

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	70.7
Placebo / Apremilast 30 mg	81.0
Apremilast 20 mg	65.9
Apremilast 30 mg	69.4

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improved by ≥ 1 after 52 weeks. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With Pre-existing Dactylitis Whose Dactylitis Severity Score Improves From Baseline to 0 at Week 52

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 52 weeks. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit and ranges from 0 to 20. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Percentage of Participants With Pre-existing Dactylitis Whose Dactylitis Severity Score Improves to 0 at Week 16

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 16 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With Pre-existing Enthesopathy Whose Maastricht Ankylosing Spondylitis Entheses Score Improves to 0 at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01307423)
Timeframe: Baseline and Week 16

Percentage of Participants With Pre-existing Enthesopathy Whose MASES Improves From Baseline to 0 at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Achilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval was based on the Clopper-Pearson method. (NCT01307423)
Timeframe: Baseline and Week 52

Number of Participants With Treatment Emergent Adverse Events During the Apremilast Exposure Period

A TEAE is an adverse event (AE) with a start date on or after the date of the first dose of investigational product (IP) and no later than 28 days after the last dose of IP. An AE is any noxious, unintended, or untoward medical occurrence that may appear or worsen in a subject during the course of a study. A serious AE is any AE that results in death; is life-threatening; requires inpatient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; or constitutes an important medical event. For both AEs and SAEs the investigator assessed the severity of the event according to the grading scale: Mild: asymptomatic or with mild symptoms, Moderate: symptoms causing moderate discomfort or Severe: symptoms causing severe discomfort or pain. (NCT01307423)
Timeframe: Week 0 to Week 260; median duration of exposure to apremilast 20 mg BID was 168.93 weeks and 229.36 weeks for apremilast 30 mg BID

Number of Participants With Treatment Emergent Adverse Events During the Placebo Controlled Phase

A TEAE is an adverse event (AE) with a start date on or after the date of the first dose of investigational product (IP) and no later than 28 days after the last dose of IP. An AE is any noxious, unintended, or untoward medical occurrence that may appear or worsen in a subject during the course of a study. A serious AE is any AE that results in death; is life-threatening; requires inpatient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; or constitutes an important medical event. For both AEs and SAEs the investigator assessed the severity of the event according to the grading scale: Mild: asymptomatic or with mild symptoms, Moderate: symptoms causing moderate discomfort or Severe: symptoms causing severe discomfort or pain. (NCT01307423)
Timeframe: Week 0 to Week 16 for placebo participants who entered EE at Week 16 and up to Week 24 for all other participants (placebo participants who remained on placebo through week 24 and participants randomized to the APR 20 mg BID or APR 30 mg BID)

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 16

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01212757)
Timeframe: Baseline and Week 16

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 24

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01212757)
Timeframe: Baseline and Week 24

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 16

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: - 28 tender joint count (TJC), - 28 swollen joint count (SJC), - Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; - Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8 Low Disease Activity: > 2.8 and ≤ 10 Moderate Disease Activity: > 10 and ≤ 22 High Disease Activity: > 22. (NCT01212757)
Timeframe: Baseline and Week 16

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 24

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: • 28 tender joint count (TJC), • 28 swollen joint count (SJC), • Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; • Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8; Low Disease Activity: > 2.8 and ≤ 10; Moderate Disease Activity: > 10 and ≤ 22; High Disease Activity: > 22. (NCT01212757)
Timeframe: Baseline and Week 24

Change From Baseline in Dactylitis Severity Score at Week 16

Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet will be rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Baseline and Week 16

Change From Baseline in Dactylitis Severity Score at Week 24

Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet will be rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Baseline and Week 24

Change From Baseline in Health Assessment Questionnaire - Disability Index (HAQ-DI) at Week 52

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01212757)
Timeframe: Baseline and Week 52

Change From Baseline in Health Assessment Questionnaire- Disability Index (HAQ-DI) at Week 16

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01212757)
Timeframe: Baseline and Week 16

Change From Baseline in Health Assessment Questionnaire- Disability Index (HAQ-DI) at Week 24

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01212757)
Timeframe: Baseline and Week 24

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 16

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Baseline and Week 16

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 24

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Baseline and Week 24

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 52

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Baseline and Week 52

Change From Baseline in Patient's Assessment of Pain at Week 16

Change From Baseline in Patient's Assessment of Pain at Week 24

Change From Baseline in the CDAI Score at Week 52

Change From Baseline in the Dactylitis Severity Score at Week 52

Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet will be rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Baseline and Week 52

Change From Baseline in the DAS28 at Week 52

Change From Baseline in the Disease Activity Score (DAS28) at Week 16

The DAS28 measures the severity of disease at a specific time and is derived from the following variables: - 28 tender joint count - 28 swollen joint count, which do not include the distal interphalangeal (DIP) joints, the hip joint, or the joints below the knee; - C-reactive protein (CRP) - Patient's global assessment of disease activity. DAS28(CRP) scores range from 0 to approximately 10, with the upper bound dependent on the highest possible level of CRP. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. (NCT01212757)
Timeframe: Baseline and Week 16

Change From Baseline in the Disease Activity Score (DAS28) at Week 24

Change From Baseline in the FACIT-Fatigue Scale Score at Week 52

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 16

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 24

Change From Baseline in the Patient Assessment of Pain at Week 52

Change From Baseline in the SF-36 Physical Functioning Scale Score at Week 52

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 16

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 16 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Week 16

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 24

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 24 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Week 24

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 52

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 52 weeks. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Week 52

Percentage of Participants Achieving a MASES Score of Zero at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Week 16

Percentage of Participants Achieving a MASES Score of Zero at Week 24

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Week 24

Percentage of Participants Achieving a MASES Score of Zero at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Week 52

Percentage of Participants Achieving Good or Moderate EULAR Response at Week 52

A EULAR response reflects an improvement in disease activity and an attainment of a lower degree of disease activity based on the DAS-28 score. A Good Response is defined as an improvement (decrease) in the DAS28 of more than 1.2 compared with Baseline and attainment of a DAS28 score less than or equal to 3.2. A Moderate Response is defined as either: • an improvement (decrease) in the DAS28 of greater than 0.6 and less than or equal to 1.2 and attainment of a DAS28 score of less than or equal to 5.1 or, • an improvement (decrease) in the DAS28 of more than 1.2 and attainment of a DAS28 score of greater than 3.2. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants With a ACR 20 Response at Week 52

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants With a ACR 50 Response at Week 16

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: o Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); o Patient's global assessment of disease activity (measured on a 100 mm VAS); o Physician's global assessment of disease activity (measured on a 100 mm VAS); o Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); o C-Reactive Protein. (NCT01212757)
Timeframe: Baseline and Week 16

Percentage of Participants With a ACR 70 Response at Week 24

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦C-Reactive Protein. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With a Modified PsARC Response at Week 52

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 16

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: - 78 tender joint count, - 76 swollen joint count, - Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; - Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. (NCT01212757)
Timeframe: Baseline and Week 16

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 24

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 20 Response at Week 24

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦C-Reactive Protein. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 50 Response at Week 24

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: o Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); o Patient's global assessment of disease activity (measured on a 100 mm VAS); o Physician's global assessment of disease activity (measured on a 100 mm VAS); o Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); o C-Reactive Protein. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 50 Response at Week 52

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants With an ACR 70 Response at Week 16

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: o Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); o Patient's global assessment of disease activity (measured on a 100 mm VAS); o Physician's global assessment of disease activity (measured on a 100 mm VAS); o Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); o C-Reactive Protein. (NCT01212757)
Timeframe: Baseline and Week 16

Percentage of Participants With an ACR 70 Response at Week 52

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants With an American College of Rheumatology 20% (ACR20) Response at Week 16

Percentage of participants with an ACR20 response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦C-Reactive Protein. (NCT01212757)
Timeframe: Baseline and Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 16

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improved by ≥ 1 after 16 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Baseline and Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 24

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improved by ≥ 1 after 24 weeks of treatment. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 52

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improved by ≥ 1 after 52 weeks. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Baseline and Week 52

Percentage of Participants With Good or Moderate EULAR Response at Week 24

EULAR response reflects an improvement in disease activity and an attainment of a lower degree of disease activity based on the DAS-28 score. A Good Response is defined as an improvement (decrease) in the DAS28 of more than 1.2 compared with Baseline and attainment of a DAS28 score less than or equal to 3.2. A Moderate Response is defined as either: • an improvement (decrease) in the DAS28 of greater than 0.6 and less than or equal to 1.2 and attainment of a DAS28 score of less than or equal to 5.1 or, • an improvement (decrease) in the DAS28 of more than 1.2 and attainment of a DAS28 score of greater than 3.2. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With Good or Moderate European League Against Rheumatism (EULAR) Response at Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Baseline and Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 24

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212757)
Timeframe: Baseline and Week 24

Percentage of Participants With MASES Improvement ≥ 20% at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 52 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212757)
Timeframe: Baseline and Week 52

Number of Participants With TEAEs During the Apremilast-Exposure Period

"A treatment emergent adverse event (TEAE) is an AE with a start date on or after the date of the first dose of Investigational Product (IP). The severity of each adverse event (AE) and serious AE (SAE) was assessed by the investigator and graded based on a scale from Mild - mild symptoms to Severe AEs (non-serious or serious). A serious adverse event (SAE) is any AE which:~Resulted in death~Was life-threatening~Required inpatient hospitalization or prolongation of existing hospitalization~Resulted in persistent or significant disability/incapacity~Was a congenital anomaly/birth defect~Constituted an important medical event" (NCT01212757)
Timeframe: Week 0 to week 260; overall median duration of exposure to apremilast 20 mg and 30 mg BID was 198 weeks

Number of Participants With Treatment Emergent Adverse Events During the Placebo-Controlled Phase

"A treatment emergent adverse event (TEAE) is an AE with a start date on or after the date of the first dose of Investigational Product (IP). The severity of each adverse event (AE) and serious AE (SAE) was assessed by the investigator and graded based on a scale from Mild - mild symptoms to Severe AEs (non-serious or serious). A serious adverse event (SAE) is any AE which:~Resulted in death~Was life-threatening~Required inpatient hospitalization or prolongation of existing hospitalization~Resulted in persistent or significant disability/incapacity~Was a congenital anomaly/birth defect~Constituted an important medical event" (NCT01212757)
Timeframe: Week 0 to Week 16 for placebo participants who entered EE at Week 16 and up to Week 24 for all other participants (placebo participants who remained on placebo through week 24 and participants randomized to the APR 20 mg BID or APR 30 mg BID)

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 16

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01172938)
Timeframe: Baseline and Week 16

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 16

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: • 28 tender joint count (TJC), • 28 swollen joint count (SJC), • Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; • Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0 to 76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8 Low Disease Activity: > 2.8 and ≤ 10 Moderate Disease Activity: > 10 and ≤ 22 High Disease Activity: > 22. (NCT01172938)
Timeframe: Baseline and Week 16

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 24

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: • 28 tender joint count (TJC), • 28 swollen joint count (SJC), • Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; • Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8; Low Disease Activity: > 2.8 and ≤ 10; Moderate Disease Activity: > 10 and ≤ 22; High Disease Activity: > 22. (NCT01172938)
Timeframe: Baseline and Week 24

Change From Baseline in Dactylitis Severity Score at Week 16

Change From Baseline in Dactylitis Severity Score at Week 24

Change From Baseline in Health Assessment Questionnaire - Disability Index (HAQ-DI) at Week 52

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01172938)
Timeframe: Baseline and Week 52

Change From Baseline in Health Assessment Questionnaire- Disability Index (HAQ-DI) at Week 16

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01172938)
Timeframe: Baseline and Week 16

Change From Baseline in Health Assessment Questionnaire- Disability Index (HAQ-DI) at Week 24

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01172938)
Timeframe: Baseline and Week 24

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 16

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Baseline and Week 16

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 24

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Baseline and Week 24

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 52

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Baseline and week 52

Change From Baseline in Patient's Assessment of Pain at Week 16

Change From Baseline in Patient's Assessment of Pain at Week 24

Change From Baseline in SF-36 Physical Function at Week 24

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01172938)
Timeframe: Baseline and Week 24

Change From Baseline in the CDAI Score at Week 52

Change From Baseline in the Dactylitis Severity Score at Week 52

Change From Baseline in the DAS28 at Week 52

Change From Baseline in the Disease Activity Score (DAS28) at Week 16

The DAS28 measures the severity of disease at a specific time and is derived from the following variables: • 28 tender joint count • 28 swollen joint count, which do not include the distal interphalangeal (DIP) joints, the hip joint, or the joints below the knee; • C-reactive protein (CRP) • Patient's global assessment of disease activity. DAS28(CRP) scores range from 0 to approximately 10, with the upper bound dependent on the highest possible level of CRP. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. (NCT01172938)
Timeframe: Baseline and Week 16

Change From Baseline in the Disease Activity Score (DAS28) at Week 24

Change From Baseline in the FACIT-Fatigue Scale Score at Week 52

"The FACIT-Fatigue scale is a 13-item self-administered questionnaire that assesses both the physical and functional consequences of fatigue. Each question is answered on a 5-point scale, where 0 means not at all, and 4 means very much. The FACIT-Fatigue scale score ranges from 0 to 52, with higher scores denoting lower levels of fatigue. A positive change from Baseline score indicates an improvement." (NCT01172938)
Timeframe: Baseline and Week 52

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 16

"The FACIT-Fatigue scale is a 13-item self-administered questionnaire that assesses both the physical and functional consequences of fatigue. Each question is answered on a 5-point scale, where 0 means not at all, and 4 means very much. The FACIT-Fatigue scale score ranges from 0 to 52, with higher scores denoting lower levels of fatigue. A positive change from Baseline score indicates an improvement." (NCT01172938)
Timeframe: Baseline and Week 16

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 24

"The FACIT-Fatigue scale is a 13-item self-administered questionnaire that assesses both the physical and functional consequences of fatigue. Each question is answered on a 5-point scale, where 0 means not at all, and 4 means very much. The FACIT-Fatigue scale score ranges from 0 to 52, with higher scores denoting lower levels of fatigue. A positive change from Baseline score indicates an improvement." (NCT01172938)
Timeframe: Baseline and Week 24

Change From Baseline in the Patient Assessment of Pain at Week 52

Change From Baseline in the SF-36 Physical Functioning Domain at Week 52

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01172938)
Timeframe: Baseline and Week 52

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 16

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 24

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 52

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 52 weeks. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01172938)
Timeframe: Week 52

Percentage of Participants Achieving a MASES Score of Zero at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Week 16

Percentage of Participants Achieving a MASES Score of Zero at Week 24

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Week 24

Percentage of Participants Achieving a MASES Score of Zero at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01172938)
Timeframe: Week 52

Percentage of Participants Achieving Good or Moderate EULAR Response at Week 52

Percentage of Participants With a ACR 20 Response at Week 52

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and Week 52

Percentage of Participants With a ACR 50 Response at Week 16

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and Week 16

Percentage of Participants With a ACR 70 Response at Week 24

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and week 24

Percentage of Participants With a Modified PsARC Response at Week 52

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from Baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from Baseline by ≥ 20 mm VAS. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01172938)
Timeframe: Baseline and Week 52

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 16

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from Baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from Baseline by ≥ 20 mm VAS. (NCT01172938)
Timeframe: Baseline and Week 16

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 24

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: •78 tender joint count, •76 swollen joint count, •Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; •Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. (NCT01172938)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 20 Response at Week 24

Percentage of participants with an American College of Rheumatology 20% (ACR20) response at Week 24. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 50 Response at Week 24

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 50 Response at Week 52

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01172938)
Timeframe: Baseline and Week 52

Percentage of Participants With an ACR 70 Response at Week 16

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and Week 16

Percentage of Participants With an ACR 70 Response at Week 52

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01172938)
Timeframe: Baseline and Week 52

Percentage of Participants With an American College of Rheumatology 20% (ACR20) Response at Week 16

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01172938)
Timeframe: Baseline and Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 24

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 52

Percentage of Participants With Good or Moderate EULAR Response at Week 24

Percentage of Participants With Good or Moderate European League Against Rheumatism (EULAR) Response at Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Baseline and Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 24

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01172938)
Timeframe: Baseline and Week 24

Percentage of Participants With MASES Improvement ≥ 20% at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 52 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01172938)
Timeframe: Baseline and Week 52

Number of Participants With Adverse Events During the Apremilast-Exposure Period

A TEAE is an AE with a start date on or after the date of the first dose of Investigational Product (IP) and no later than 28 days after the last dose of IP. An AE is any noxious, unintended, or untoward medical occurrence, that may appear or worsen in a participant during the course of study. It may be a new intercurrent illness, a worsening concomitant illness, an injury, or any concomitant impairment of the participant's health, including laboratory test values regardless of etiology. Any worsening (ie, any clinically significant adverse change in the frequency or intensity of a preexisting condition) was considered an AE. A serious AE (SAE) is any untoward adverse event that is fatal, life-threatening, results in persistent or significant disability or incapacity, requires or prolongs existing in-patient hospitalization, is a congenital anomaly or birth defect, or a condition that may jeopardize the patient or may require intervention to prevent one of the outcomes listed above. (NCT01172938)
Timeframe: Baseline to Week 260; median total exposure to Apremilast was 170 weeks

Number of Participants With Adverse Events During the Placebo-Controlled Period

A Treatment Emergent Adverse Event (TEAE) is an AE with a start date on or after the date of the first dose of Investigational Product (IP). An AE is any noxious, unintended, or untoward medical occurrence, that may appear or worsen in a participant during the course of study. It may be a new intercurrent illness, a worsening concomitant illness, an injury, or any concomitant impairment of the participant's health, including laboratory test values regardless of etiology. Any worsening (ie, any clinically significant adverse change in the frequency or intensity of a preexisting condition) was considered an AE. A serious AE (SAE) is any untoward adverse event that is fatal, life-threatening, results in persistent or significant disability or incapacity, requires or prolongs existing in-patient hospitalization, is a congenital anomaly or birth defect, or a condition that may jeopardize the patient or may require intervention to prevent one of the outcomes listed above. (NCT01172938)
Timeframe: Week 0 to Week 16 for placebo participants who entered early escape at Week 16 and up to Week 24 for all other participants (placebo participants who remained on placebo through week 24 and participants randomized to the APR 20 mg BID or APR 30 mg BID)

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 16

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01212770)
Timeframe: Baseline and Week 16

Change From Baseline in 36-item Short Form Health Survey (SF-36) Physical Functioning Domain at Week 24

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01212770)
Timeframe: Baseline and Week 24

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 16

Change From Baseline in Clinical Disease Activity Index (CDAI) at Week 24

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: • 28 tender joint count (TJC), • 28 swollen joint count (SJC), • Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; • Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8; Low Disease Activity: > 2.8 and ≤ 10; Moderate Disease Activity: > 10 and ≤ 22; High Disease Activity: > 22. (NCT01212770)
Timeframe: Baseline and Week 24

Change From Baseline in Dactylitis Severity Score at Week 16

Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. (NCT01212770)
Timeframe: Baseline and Week 16

Change From Baseline in Dactylitis Severity Score at Week 24

Change From Baseline in Health Assessment Questionnaire - Disability Index (HAQ-DI) at Week 52

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01212770)
Timeframe: Baseline and Week 52

Change From Baseline in Health Assessment Questionnaire- Disability Index (HAQ-DI) at Week 16

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01212770)
Timeframe: Baseline and Week 16

Change From Baseline in Health Assessment Questionnaire- Disability Index (HAQ-DI) at Week 24

The Health Assessment Questionnaire - Disability Index is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. Negative mean changes from Baseline in the overall score indicate improvement in functional ability. (NCT01212770)
Timeframe: Baseline and Week 24

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 16

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Baseline and Week 16

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 24

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Baseline and week 24

Change From Baseline in Maastricht Ankylosing Spondylitis Entheses Score (MASES) at Week 52

The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Baseline and Week 52

Change From Baseline in Patient's Assessment of Pain at Week 16

Change From Baseline in Patient's Assessment of Pain at Week 24

Change From Baseline in the CDAI Score at Week 52

The Clinical Disease Activity Index (CDAI) is a composite index that is calculated as the sum of the: •28 tender joint count (TJC), •28 swollen joint count (SJC), •Patient's Global Assessment of Disease Activity measured on a 10 cm visual analog scale (VAS), where 0 cm = lowest disease activity and 10 cm = highest; •Physician's Global Assessment of Disease Activity -measured on a 10 cm VAS, where 0 cm = lowest disease activity and 10 cm = highest. The CDAI score ranges from 0-76 where lower scores indicate less disease activity. The following thresholds of disease activity have been defined for the CDAI: Remission: ≤ 2.8 Low Disease Activity: > 2.8 and ≤ 10 Moderate Disease Activity: > 10 and ≤ 22 High Disease Activity: > 22. (NCT01212770)
Timeframe: Baseline and Week 52

Change From Baseline in the Dactylitis Severity Score at Week 52

Change From Baseline in the DAS28 at Week 52

The DAS28 measures the severity of disease at a specific time and is derived from the following variables: •28 tender joint count •28 swollen joint count, which do not include the DIP joints, the hip joint, or the joints below the knee; •C-reactive protein (CRP) •Patient's global assessment of disease activity. DAS28(CRP) scores range from 0 to approximately 10, with the upper bound dependent on the highest possible level of CRP. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. (NCT01212770)
Timeframe: Baseline and Week 52

Change From Baseline in the Disease Activity Score (DAS28) at Week 16

Change From Baseline in the Disease Activity Score (DAS28) at Week 24

Change From Baseline in the FACIT-Fatigue Scale Score at Week 52

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 16

Change From Baseline in the Functional Assessment of Chronic Illness Therapy-Fatigue (FACIT-Fatigue) Score at Week 24

Change From Baseline in the Patient Assessment of Pain at Week 52

Change From Baseline in the SF-36 Physical Functioning Scale Score at Week 52

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01212770)
Timeframe: Baseline and Week 52

Percentage of Participants Achieving a ≥ 75% Improvement in Psoriasis Area and Severity Index Score (PASI75) at Week 16

The percentage of participants with Baseline psoriasis body surface area (BSA) involvement ≥ 3% who achieved 75% or greater improvement from Baseline in Psoriasis Area and Severity Index (PASI) score after 16 weeks of treatment. The Psoriasis Area and Severity Index (PASI) score is a combination of the intensity of psoriasis, assessed by erythema (reddening), induration (plaque thickness) and desquamation (scaling) scored on a scale from 0 (none) to 4 (very severe), together with the percentage of the area affected, rated on a scale from 0 (no involvement) to 6 (90% to 100% involvement). PASI scoring is performed at four body areas, the head, arms, trunk, and legs. The total PASI score ranges from 0 to 72. The higher the total score, the more severe the disease. (NCT01212770)
Timeframe: Baseline and Week 16

Percentage of Participants Achieving a ≥ 75% Improvement in Psoriasis Area and Severity Index Score (PASI75) at Week 24

The percentage of participants with Baseline psoriasis body surface area (BSA) involvement ≥ 3% who achieved 75% or greater improvement from Baseline in Psoriasis Area and Severity Index (PASI) score after 24 weeks of treatment. The Psoriasis Area and Severity Index (PASI) score is a combination of the intensity of psoriasis, assessed by erythema (reddening), induration (plaque thickness) and desquamation (scaling) scored on a scale from 0 (none) to 4 (very severe), together with the percentage of the area affected, rated on a scale from 0 (no involvement) to 6 (90% to 100% involvement). PASI scoring is performed at four body areas, the head, arms, trunk, and legs. The total PASI score ranges from 0 to 72. The higher the total score, the more severe the disease. (NCT01212770)
Timeframe: Baseline and Week 24

Percentage of Participants Achieving a ≥ 75% Improvement in Psoriasis Area and Severity Index Score (PASI75) at Week 52

The percentage of participants with Baseline psoriasis body surface area (BSA) involvement ≥ 3% who achieved 75% or greater improvement from Baseline in Psoriasis Area and Severity Index (PASI) score after 52 weeks. The Psoriasis Area and Severity Index (PASI) score is a combination of the intensity of psoriasis, assessed by erythema (reddening), induration (plaque thickness) and desquamation (scaling) scored on a scale from 0 (none) to 4 (very severe), together with the percentage of the area affected, rated on a scale from 0 (no involvement) to 6 (90% to 100% involvement). PASI scoring is performed at four body areas, the head, arms, trunk, and legs. The total PASI score ranges from 0 to 72. The higher the total score, the more severe the disease. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Baseline and Week 52

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 16

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 24

Percentage of Participants Achieving a Dactylitis Score of Zero at Week 52

Percentage of participants with pre-existing dactylitis whose dactylitis severity score improves to zero after 52 weeks. Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated as zero for no dactylitis or 1 for dactylitis present. The dactylitis severity score is the sum of the individual scores for each digit. The dactylitis severity score, ranging from 0 to 20, is the number of digits on the hands and feet with dactylitis present. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Week 52

Percentage of Participants Achieving a MASES Score of Zero at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Week 16

Percentage of Participants Achieving a MASES Score of Zero at Week 24

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Week 24

Percentage of Participants Achieving a MASES Score of Zero at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improves to 0 after 24 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Week 52

Percentage of Participants Achieving Good or Moderate EULAR Response at Week 52

Percentage of Participants With a ACR 50 Response at Week 16

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01212770)
Timeframe: Baseline and Week 16

Percentage of Participants With a ACR 70 Response at Week 24

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01212770)
Timeframe: Baseline and Week 24

Percentage of Participants With a Modified PsARC Response at Week 52

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Baseline and Week 52

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 16

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. (NCT01212770)
Timeframe: Baseline and Week 16

Percentage of Participants With a Modified Psoriatic Arthritis Response Criteria (PsARC) Response at Week 24

Modified PsARC response is defined as improvement in at least 2 of the 4 measures, at least one of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • 78 tender joint count, • 76 swollen joint count, • Patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • Physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Improvement or worsening in joint counts is defined as decrease or increase, respectively, from baseline by ≥ 30%, and improvement or worsening in global assessments is defined as decrease or increase, respectively, from baseline by ≥ 20 mm VAS. (NCT01212770)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 20 Response at Week 24

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01212770)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 20 Response at Week 52

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Baseline and Week 52

Percentage of Participants With an ACR 50 Response at Week 24

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01212770)
Timeframe: Baseline and Week 24

Percentage of Participants With an ACR 50 Response at Week 52

Percentage of participants with an American College of Rheumatology 50% (ACR50) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 50% improvement in 78 tender joint count; • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Baseline and Week 52

Percentage of Participants With an ACR 70 Response at Week 16

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01212770)
Timeframe: Baseline and Week 16

Percentage of Participants With an ACR 70 Response at Week 52

Percentage of participants with an American College of Rheumatology 70% (ACR70) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 70% improvement in 78 tender joint count; • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Baseline and Week 52

Percentage of Participants With an American College of Rheumatology 20% (ACR20) Response at Week 16

Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met: • ≥ 20% improvement in 78 tender joint count; • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-Reactive Protein. (NCT01212770)
Timeframe: Baseline and Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 16

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 24

Percentage of Participants With Dactylitis Improvement ≥ 1 Point at Week 52

Percentage of Participants With Good or Moderate EULAR Response at Week 24

Percentage of Participants With Good or Moderate European League Against Rheumatism (EULAR) Response at Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 16

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 16 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Baseline and Week 16

Percentage of Participants With MASES Improvement ≥ 20% at Week 24

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 24 weeks of treatment. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. (NCT01212770)
Timeframe: Baseline and Week 24

Percentage of Participants With MASES Improvement ≥ 20% at Week 52

Percentage of participants with pre-existing enthesopathy whose MASES improved by ≥ 20% from Baseline after 52 weeks. The Maastricht Ankylosing Spondylitis Enthesitis Score quantitates inflammation of the entheses (enthesitis) by assessing pain at the following entheses (sites where tendons or ligaments insert into the bone): 1st costochondral joints left/right; 7th costochondral joints left/right; posterior superior iliac spine left/right; anterior superior iliac spine left/right; iliac crest left/right; 5th lumbar spinous process; and the proximal insertion of the Archilles tendon left/right. The MASES, ranging from 0 to 13, is the number of painful entheses out of 13 entheses. Two-sided 95% confidence interval is based on the Clopper-Pearson method. (NCT01212770)
Timeframe: Baseline and Week 52

Number of Participants With Treatment Emergent Adverse Events (TEAEs) During the Placebo-Controlled Phase

A TEAE is an adverse event (AE) with a start date on or after the date of the first dose of investigational product (IP) and no later than 28 days after the last dose of IP. An adverse event (AE) is any noxious, unintended, or untoward medical occurrence that may appear or worsen in a subject during the course of a study. A serious AE is any AE that results in death; is life-threatening; requires inpatient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; or constitutes an important medical event. For both AEs and SAEs the investigator assessed the severity of the event according to the grading scale: Mild: asymptomatic or with mild symptoms, Moderate: symptoms causing moderate discomfort or Severe: symptoms causing severe discomfort or pain. (NCT01212770)
Timeframe: Week 0 to Week 16 for placebo participants who entered EE at Week 16 and up to Week 24 for all other participants (placebo participants who remained on placebo through week 24 and participants randomized to the APR 20 mg BID or APR 30 mg BID)

Number of Participants With Treatment Emergent Adverse Events During the Apremilast Exposure Period

A TEAE is an adverse event (AE) with a start date on or after the date of the first dose of investigational product (IP) and no later than 28 days after the last dose of IP. An adverse event (AE) is any noxious, unintended, or untoward medical occurrence that may appear or worsen in a subject during the course of a study. A serious AE is any AE that results in death; is life-threatening; requires inpatient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; or constitutes an important medical event. For both AEs and SAEs the investigator assessed the severity of the event according to the grading scale: Mild: asymptomatic or with mild symptoms, Moderate: symptoms causing moderate discomfort or Severe: symptoms causing severe discomfort or pain. (NCT01212770)
Timeframe: Week 0 to Week 260; median duration of exposure to apremilast 20 mg BID was 121.71 weeks and 232.50 weeks for apremilast 30 mg BID

Change From Baseline in 36-item Short Form Health Survey (SF-36) V 2 Physical Functioning Domain at Week 16

The SF-36 (v 2.0) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from Baseline score indicates an improvement. (NCT01925768)
Timeframe: Baseline and Week 16

Change From Baseline in Health Assessment Questionnaire-Disability Index (HAQ-DI) at Week 16

HAQ-DI is a patient-reported questionnaire consisting of 20 questions referring to eight domains: dressing/grooming, arising, eating, walking, hygiene, reach, grip, and usual activities. Participants assessed their ability to do each task over the past week using the following response categories: without any difficulty (0); with some difficulty (1); with much difficulty (2); and unable to do (3). Scores on each task are summed and averaged to provide an overall score ranging from 0 to 3, where zero represents no disability and three very severe, high-dependency disability. A higher score indicates worse physical functioning, and a negative change from baseline indicates improvement. (NCT01925768)
Timeframe: Baseline and Week 16

Change From Baseline in Health Assessment Questionnaire-Disability Index (HAQ-DI) at Week 24

Change From Baseline in the 28-Joint Disease Activity Score Using C-reactive Protein as the Acute-Phase Reactant (DAS28 [CRP]) at Week 24

"The DAS28 measures the severity of disease at a specific time and is derived from the following variables:~28 tender joint count~28 swollen joint count, which do not include the DIP joints, the hip joint, or the joints below the knee;~C-reactive protein (CRP)~Patient's global assessment of disease activity. DAS28 (CRP) scores range from 0 to 9.4. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. A higher value indicates higher disease activity, and a negative change from baseline indicates improvement." (NCT01925768)
Timeframe: Baseline and Week 24

Change From Baseline in the 36-item SF-36 Physical Component Summary Score at Week 24

The SF-36 (v 2.0) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). The physical component summary (PCS) score includes the physical functioning, role physical, bodily pain, and general health domains. Minimum clinically important difference (MCID) for the scale scores, as well as the PCS and MCS, is defined as a 2.5-point improvement (increase) from baseline. The summary scores range from 0 to 100, with lower scores reflecting more disability, and higher scores reflecting less disability and better health. The 8 domains are regrouped into the PCS and MCS scores. (NCT01925768)
Timeframe: Baseline and Week 24

Change From Baseline in the Disease Activity Score DAS28 (CRP) at Week 16

"The DAS28 measures the severity of disease at a specific time and is derived from the following variables:~28 tender joint count~28 swollen joint count, which do not include the DIP joints, the hip joint, or the joints below the knee;~C-reactive protein (CRP)~Patient's global assessment of disease activity. DAS28 (CRP) scores range from 0 to 9.4. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. A negative change from baseline indicates improvement." (NCT01925768)
Timeframe: Baseline and Week 16

Change From Baseline in the Duration of Morning Stiffness at Week 24

Morning stiffness was the participant's assessment of how long their morning stiffness lasted after first waking up in the morning, on average, during the previous week. A higher value indicates longer duration, and a negative change from baseline indicates improvement. (NCT01925768)
Timeframe: Baseline and Week 24

Change From Baseline in the Medical Outcomes Short Form Health Survey (SF-36) V2 Physical Function Domain Score at Week 24

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10. Higher scores indicate a higher level of functioning. The physical functioning domain assesses limitations in physical activities because of health problems. A positive change from baseline score indicates an improvement. (NCT01925768)
Timeframe: Baseline and Week 24

Mean Change From Baseline in the Duration of Morning Stiffness at Week 16

Percentage of Participants Who Achieved an American College of Rheumatology 20% (ACR20) at Week 24

"Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met:~≥ 20% improvement in 78 tender joint count;~≥ 20% improvement in 76 swollen joint count; and~≥ 20% improvement in at least 3 of the 5 following parameters:~Patient's self-assessment of pain (measured on a 0 to 10 unit numeric rating scale [NRS]);~Patient's global self-assessment of disease activity (measured on a 0 to 10 unit NRS);~Physician's global assessment of disease activity (measured on a 0 to 10 unit NRS);~Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]);~C-Reactive Protein (CRP) Those who withdrew early or who did not have sufficient data at Week 16 were counted as non-responders." (NCT01925768)
Timeframe: Baseline and Week 24

Percentage of Participants Who Achieved an American College of Rheumatology 20% (ACR20) Response at Week 16

Percentage of Participants Whose Severity of Morning Stiffness at Week 16 Improved From Baseline

Morning stiffness severity was the participant's assessment of how severe their morning stiffness was after first waking up in the morning, on average, during the previous week. The severity was recorded as none, mild, moderate, moderately severe, or very severe. Improvement is defined as the change from baseline of a more severe assessment to less severe assessment. Full Analysis Set; Participants who discontinued early prior to Week 16 and those who did not have sufficient data for a definitive determination of response status at Week 16 were counted as non-responders. (NCT01925768)
Timeframe: Baseline and Week 16

Percentage of Participants With Improved Change in Severity of Morning Stiffness at Week 24

Morning stiffness severity was the participant's assessment of how severe their morning stiffness was after first waking up in the morning, on average, during the previous week. The severity was recorded as none, mild, moderate, moderately severe, or very severe. The response of no improvement includes subjects who had no change or worsened. Improvement is defined as the change from baseline of a more severe assessment to less severe assessment. (NCT01925768)
Timeframe: Baseline and Week 24

Change From Baseline in 36-item SF-36 (V2.0) Physical Functioning Domain Score at Weeks 52 and 104

Change From Baseline in Health Assessment Questionnaire-Disability Index (HAQ-DI) at Weeks 52 and 104

Change From Baseline in the Disease Activity Score (DAS28) at Week 52 and 104

"The DAS28 measures the severity of disease at a specific time and is derived from the following variables:~28 tender joint count~28 swollen joint count, which do not include the DIP joints, the hip joint, or the joints below the knee;~C-reactive protein (CRP)~Patient's global assessment of disease activity. DAS28 (CRP) scores range from 0 to 9.4. A DAS28 score higher than 5.1 indicates high disease activity, a DAS28 score less than 3.2 indicates low disease activity, and a DAS28 score less than 2.6 indicates clinical remission. A negative change from baseline indicates improvement." (NCT01925768)
Timeframe: Baseline and Weeks 52 and 104

Change From Baseline in the Duration of Morning Stiffness at Weeks 52 and 104

Number of Participants With Treatment Emergent Adverse Events (TEAE) During the 24 Week Placebo Controlled Phase

A TEAE is an AE with a start date on or after the date of the first dose of Investigational Product (IP). An AE is any noxious, unintended, or untoward medical occurrence, that may appear or worsen in a participant during the course of study. It may be a new intercurrent illness, a worsening concomitant illness, an injury, or any concomitant impairment of the participant's health, including laboratory test values regardless of etiology. Any worsening (ie, any clinically significant adverse change in the frequency or intensity of a preexisting condition) was considered an AE. A serious AE (SAE) is any untoward adverse event that is fatal, life-threatening, results in persistent or significant disability or incapacity, requires or prolongs existing in-patient hospitalization, is a congenital anomaly or birth defect, or a condition that may jeopardize the patient or may require intervention to prevent one of the outcomes listed above. (NCT01925768)
Timeframe: Date of first dose of study drug to Week 24; median duration of exposure during placebo controlled phase was 24.14 weeks

Number of Participants With Treatment Emergent Adverse Events (TEAE) During the Apremilast-Exposure Period

A TEAE is an AE with a start date on or after the date of the first dose of Investigational Product (IP). An AE is any noxious, unintended, or untoward medical occurrence, that may appear or worsen in a participant during the course of study. It may be a new intercurrent illness, a worsening concomitant illness, an injury, or any concomitant impairment of the participant's health, including laboratory test values regardless of etiology. Any worsening (ie, any clinically significant adverse change in the frequency or intensity of a preexisting condition) was considered an AE. A serious AE (SAE) is any untoward adverse event that is fatal, life-threatening, results in persistent or significant disability or incapacity, requires or prolongs existing in-patient hospitalization, is a congenital anomaly or birth defect, or a condition that may jeopardize the patient or may require intervention to prevent one of the outcomes listed above. (NCT01925768)
Timeframe: Start of lst dose of IP up to week 104: Weeks 0 to104 for those initially randomized to APR 30 mg BID, Weeks 16 -104 for PBO-treated patients who EE to APR at Week 16 and from Weeks 24-104 for PBO-treated patients who transitioned to APR at Week 24

Percentage of Participants Who Achieved an American College of Rheumatology 20% (ACR20) Response at Weeks 2, 4, 6, 8, 12 and 20

"Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met:~≥ 20% improvement in 78 tender joint count;~≥ 20% improvement in 76 swollen joint count; and~≥ 20% improvement in at least 3 of the 5 following parameters:~Patient's self-assessment of pain (measured on a 0 to 10 unit numeric rating scale [NRS]);~Patient's global self-assessment of disease activity (measured on a 0 to 10 unit NRS);~Physician's global assessment of disease activity (measured on a 0 to 10 unit NRS);~Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]);~C-Reactive Protein (CRP)" (NCT01925768)
Timeframe: Baseline and at Weeks 2, 4, 6, 8, 12 and 20

Percentage of Participants Who Achieved an American College of Rheumatology 20% (ACR20) Response at Weeks 52 and 104

"Percentage of participants with an American College of Rheumatology 20% (ACR20) response. A participant was a responder if the following 3 criteria for improvement from Baseline were met:~≥ 20% improvement in 78 tender joint count;~≥ 20% improvement in 76 swollen joint count; and~≥ 20% improvement in at least 3 of the 5 following parameters:~Patient's self-assessment of pain (measured on a 0 to 10 unit numeric rating scale [NRS]);~Patient's global self-assessment of disease activity (measured on a 0 to 10 unit NRS);~Physician's global assessment of disease activity (measured on a 0 to 10 unit NRS);~Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]);~C-Reactive Protein (CRP)" (NCT01925768)
Timeframe: Baseline and Weeks 52 and 104

Percentage of Participants Whose Severity of Morning Stiffness at Week 52 and 104 Improved From Baseline

Change From Baseline in Bath Ankylosing Spondylitis Disease Activity Index (BASDAI) at Week 24

The BASDAI is a composite score based on a participant self-administered survey of six questions measured using a 0 to 10 unit numerical rating scale (NRS) that assessed the participants' five major symptoms of AS: 1) fatigue; 2) spinal pain; 3) peripheral joint pain/swelling; 4) areas of localized tenderness; 5a) morning stiffness severity upon wakening; 5b) morning stiffness duration upon wakening. The participant was asked to mark the box with an X on a 0 to 10 unit NRS for each of the 6 questions. To give each of the five symptoms equal weighting, the mean of the two scores relating to morning stiffness was taken. The resulting 0 to 50 score was divided by 5 to give a final 0 to 10 BASDAI score. A BASDAI score of 4 or greater was considered to be indicative of active AS disease. (NCT01583374)
Timeframe: Baseline and Week 24

Change From Baseline in Bath Ankylosing Spondylitis Functional Index (BASFI) at Week 24

The BASFI is a composite score based on a self-administered survey of 10 questions using a 0 to 10 unit numerical rating scale (NRS) that assesses the degree of mobility and functional ability. The survey consists of 8 questions regarding function in AS and the last 2 reflect the ability to manage everyday life. The patient marks a box with an X on a 0 to 10 unit NRS for 10 questions; the left-hand box of 0 = easy; the right-hand box = impossible. The resulting 0 to 100 score is divided by 10 to give a final 0 to 10 BASFI score. The overall score is the mean of the 10 items and ranges from 0 to 10. A higher score correlates to reduced functional ability. (NCT01583374)
Timeframe: Baseline and Week 24

Change From Baseline in Bath Ankylosing Spondylitis Metrology Index-Linear (BASMI-Linear) at Week 24

The BASMI-Linear was designed to assess axial status (ie, cervical, dorsal and lumbar spine, hips, and pelvic soft tissue) and to define clinically significant changes in spinal movement. Five dimensions of movement (lateral lumbar flexion, tragus to wall, forward lumbar flexion, maximal intermalleolar distance, and cervical rotation) were measured and normalized on 0 to 10 unit NRS. The average of these scores was the total BASMI score, ranging from 0-10 with higher values indicating more severe limitation in spinal mobility. (NCT01583374)
Timeframe: Baseline and Week 24

Change From Baseline in the Ankylosing Spondylitis Quality of Life (ASQoL) Summary Score at Week 24

The ASQoL is a validated disease specific patient reported outcomes instrument to assess the impact of ankylosing spondylitis on the quality of life of individuals with emphasis on the ability of the person to fulfill his or her needs. It consisted of 18 items requesting a yes (score=1) or no (score=0) response to questions related to the impact of pain on sleep, mood, motivation, ability to cope, activities of daily living, independence, relationships, and social life. The summary score ranges 0-18 with higher scores indicating worse quality of life. (NCT01583374)
Timeframe: Baseline and Week 24

Change From Baseline in the Physical Component Summary Score (PCS) of Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) at Week 24

The Medical Outcome Study Short Form 36-Item Health Survey, Version 2 (SF-36) was a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). Norm-based scores (based on US general population with mean of 50 and standard deviation of 10) were used in analyses. Higher scores indicate a higher level of functioning. The PCS encompasses physical functioning, role-physical, and bodily pain, as well as general health and vitality. A positive change from baseline score indicates an improvement (NCT01583374)
Timeframe: Baseline and Week 24

Percentage of Participants Who Achieved an Assessment of SpondyloArthritis International Society 20 (ASAS 20) Response at Week 16

"ASAS 20 was defined as achieving an improvement from baseline of ≥ 20% and ≥ 1 unit in at least 3 of 4 ASAS domains on a scale of 0 to 10 units and no worsening from baseline of ≥ 20% and ≥ 1 unit in the remaining ASAS domain on a scale of 0 to 10 units. The 4 ASAS domains are:~Patient Global Assessment of Disease (0 - 10 unit Numerical Rating Scale [NRS]); participant marks a box with an X on a 0 - 10 unit NRS; the left-hand box of 0 = not active and the right-hand box = very active~Total Back Pain (0 to 10 unit NRS); participant marks a box with an X on a 0 - 10 unit NRS; the left-hand box of 0 = no pain and the right-hand box = most severe pain~Function (Bath AS Functional Index [BASFI] NRS 0 - 10 unit); participant provides a self-administered survey of 10 questions assessing for degree of mobility and functional ability~Inflammation domain is determined by the mean of 2 Bath AS Disease Activity Index NRS Questions #5 and #6 for morning stiffness) (0 - 10 unit)" (NCT01583374)
Timeframe: Baseline and Week 16

Percentage of Participants Who Achieved an Assessment of SpondyloArthritis International Society 20 (ASAS) Response at Week 24

Change From Baseline in the Radiographic Score Using the Modified Stoke Ankylosing Spondylitis Spine Score (m-SASSS) at Week 104 and Week 260

"The Modified Stoke Ankylosing Spondylitis Spine Score is a scoring method used to determine the amount or degree of ankylosing spondylitis disease that is in the spine based on x-ray radiographs of the spine. The m-SASSS scores 0-3.~0 = No abnormality, 1 = Erosion, Sclerosis or Squaring, 2 = Syndesmophyte, 3 = Total bony Bridging at each Site. An increase in the m-SASSS indicated a worsening of AS disease." (NCT01583374)
Timeframe: Baseline to Week 104 and 260

Number of Participants With Treatment Emergent Adverse Events (TEAEs) During the Placebo Controlled Phase

A TEAE was an adverse event (AE) with a start date on or after the date of the first dose of IP and no later than 28 days after the last dose of IP for participants who discontinued early. A serious AE = results in death, is life-threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect; or constitutes an important medical event. The severity of AEs was assessed based on the following scale: Mild = asymptomatic or mild symptoms, clinical or diagnostic observations only; Moderate = symptoms cause moderate discomfort; Severe = symptoms causing severe pain discomfort. (NCT01583374)
Timeframe: From Week 0 to Week 24; the median duration of exposure was 23.57 weeks for the placebo arm, 23.71 weeks for the apremilast 20 mg arm and 24.00 weeks for the apremilast 30 mg arm.

Number of Participants With Treatment Emergent Adverse Events During the Apremilast Exposure Period

A TEAE was an adverse event (AE) with a start date on or after the date of the first dose of IP and no later than 28 days after the last dose of IP for participants who discontinued early. A serious AE = results in death, is life-threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect; or constitutes an important medical event. The severity of AEs was assessed based on the following scale: Mild = asymptomatic or mild symptoms, clinical or diagnostic observations only; Moderate = symptoms cause moderate discomfort; Severe = symptoms causing severe pain discomfort. (NCT01583374)
Timeframe: Week 0 to week 260; overall mean duration of exposure to apremilast 20 mg and 30 mg BID was 160.96 weeks

Change From Baseline in Dactylitis Severity Score at Week 12

Dactylitis is characterized by swelling of the entire finger or toe. Each digit on the hands and feet was rated on a scale from 0 (no dactylitis) to 3 (severe dactylitis). The dactylitis severity score is the sum of the individual scores for each digit and ranges from 0 to 60. (NCT00456092)
Timeframe: Baseline and Week 12

Change From Baseline in Dermatology Life Quality Index (DLQI) at Week 12

The DLQI is a validated, self-administered, 10-item questionnaire that measures the impact of skin disease on participants' quality of life, based on recall over the past week. Domains include symptoms, feelings, daily activities, leisure, work, personal relationships, and treatment. Each question is answered on a scale from 0 (not at all) to 3 (very much). The total score ranges from 0 to 30 where a higher score indicates that a participant's dermatological condition has a greater impact on their daily life. (NCT00456092)
Timeframe: Baseline and Week 12

Change From Baseline in the Functional Assessment of Chronic Illness Therapy for Fatigue (FACIT-F) at Week 12

"The FACIT-Fatigue is a 13 item self-administered questionnaire that assesses both the physical and functional consequences of fatigue based on recall during the past 7 days. Each question is answered on a 5-point scale, where 0 means not at all, and 4 means very much. The total score ranges from 0 to 52 with higher scores representing less fatigue." (NCT00456092)
Timeframe: Baseline and Week 12

Change From Baseline in the Health Assessment Questionnaire Disability Index (HAQ-DI) at Week 12

The HAQ-DI is a self-administered instrument consisting of 20 questions in eight categories of functioning which represent a comprehensive set of functional activities - dressing, rising, eating, walking, hygiene, reach, grip, and usual activities. Each item asks over the past week whether a particular task can be performed. For each item, there is a four-level difficulty scale that is scored from 0 to 3, representing normal (no difficulty) (0), some difficulty (1), much difficulty (2), and unable to do (3). The eight category scores are averaged into an overall HAQ-DI score on a scale from zero (no disability) to three (completely disabled). (NCT00456092)
Timeframe: Baseline and Week 12

Maximal ACR Response During the Extension Period

The ACR-N index score was calculated for each participant at each time point in the study according to the following definition: ACR-N = the lowest of the following 3 values: • percent improvement from Baseline in the 76 swollen joint count, • percent improvement from Baseline in the 78 tender joint count • median percent improvement from Baseline in the following 5 measures ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. The maximal ACR-N for each participant during the 12-week extension period was calculated, and represents the maximal ACR response achieved. (NCT00456092)
Timeframe: ACR was measured at Baseline and Weeks 16, 20 and 24

Maximal ACR Response During the Treatment Phase

The ACR-N index score was calculated for each participant at each time point in the study according to the following definition: ACR-N = the lowest of the following 3 values: - percent improvement from Baseline in the 76 swollen joint count, - percent improvement from Baseline in the 78 tender joint count - median percent improvement from Baseline in the following 5 measures ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. The maximal ACR-N for each participant during the 12-week treatment period was calculated, and represents the maximal ACR response achieved. (NCT00456092)
Timeframe: ACR was measured at Baseline and Weeks 2, 4, 6, 8, 10, and 12

Number of Participants Who Relapsed After the Extension Phase

Number of Participants Who Relapsed During the Observational Follow-up Phase

Relapse of psoriatic arthritis was defined as a 50% loss of the maximal ACR improvement during the Observation Phase in participants who received apremilast and achieved at least an ACR 20 at their Final Treatment Phase/Early Termination Visit. (NCT00456092)
Timeframe: 28-day observational follow-up period following Week 12

Number of Participants Who Withdrew Prematurely Due to Lack of Efficacy

The number of participants who withdrew prematurely from the treatment phase due to lack of efficacy, including flare of psoriasis, flare of psoriatic arthritis or worsening or not responding to study treatment. (NCT00456092)
Timeframe: Baseline to Week 12

Number of Participants With Adverse Events Leading to a Dose Reduction

The number of participants who were dose reduced during the treatment phase due to adverse events. (NCT00456092)
Timeframe: Baseline to Week 12

Percentage of Participants With a Modified ACR 50 Response at Week 12

A modified American College of Rheumatology 50% (ACR 50) response was defined as a participant who met the following 3 criteria for improvement from Baseline: • ≥ 50% improvement in 78 tender joint count (includes 10 additional joints often involved in psoriatic arthritis: the first carpometacarpal [CMC] and the distal interphalangeal [DIP] joints of the fingers); • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. Participants with no post-baseline ACR scores were considered non-responders. (NCT00456092)
Timeframe: Baseline and Week 12

Percentage of Participants With a Modified ACR 70 Response at Week 12

A modified American College of Rheumatology 70% (ACR 70) response was defined as a participant who met the following 3 criteria for improvement from Baseline: • ≥ 70% improvement in 78 tender joint count (includes 10 additional joints often involved in psoriatic arthritis: the first carpometacarpal [CMC] and the distal interphalangeal [DIP] joints of the fingers); • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index (HAQ-DI)); ◦ C-reactive protein. Participants with no post-baseline ACR scores were considered non-responders. (NCT00456092)
Timeframe: Baseline and Week 12

Percentage of Participants With a Modified ACR 70 Response at Week 24

A modified ACR 70 response was defined as a participant who met the following 3 criteria for improvement: • ≥ 70% improvement in 78 tender joint count (includes 10 additional joints often involved in psoriatic arthritis: the first carpometacarpal [CMC] and the distal interphalangeal [DIP] joints of the fingers); • ≥ 70% improvement in 76 swollen joint count; and • ≥ 70% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm VAS); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. Response at Week 24 was measured as improvement from Baseline (Day 1). Participants with no post-baseline ACR scores were considered non-responders. (NCT00456092)
Timeframe: Baseline (Day 1) and Week 24

Percentage of Participants With a Modified American College of Rheumatology 20% (ACR 20) Response at Week 12

A modified American College of Rheumatology 20% (ACR 20) response was defined as a participant who met the following 3 criteria for improvement from Baseline: • ≥ 20% improvement in 78 tender joint count (includes 10 additional joints often involved in psoriatic arthritis: the first carpometacarpal [CMC] and the distal interphalangeal [DIP] joints of the fingers); • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm visual analog scale [VAS]); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. Participants with no post-baseline ACR scores were considered non-responders. (NCT00456092)
Timeframe: Baseline and Week 12

Percentage of Participants With a Psoriatic Arthritis Response Criteria (PsARC) Response at Week 12

A PsARC response is defined as improvement from Baseline in at least 2 of the following 4 measures, at least 1 of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures, according to the following: • At least 30% improvement in the 78 tender joint count, • At least 30% improvement in the 76 swollen joint count, • At least 20% improvement in the patient global assessment of disease activity, measured on a 100 mm visual analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • At least 20% improvement in the physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Participants with no post-baseline PsARC scores were considered non-responders. (NCT00456092)
Timeframe: Baseline and Week 12

Percentage of Participants With a Psoriatic Arthritis Response Criteria (PsARC) Response at Week 24

A PsARC response is defined as improvement from Baseline in at least 2 of the following 4 measures, at least 1 of which must be tender joint count or swollen joint count, and no worsening in any of the 4 measures: • At least 30% improvement in the 78 tender joint count, • At least 30% improvement in the 76 swollen joint count, • At least 20% improvement in the patient global assessment of disease activity, measured on a 100 mm visual Analog scale (VAS), where 0 mm = lowest disease activity and 100 mm = highest; • At least 20% improvement in the physician global assessment of disease activity, measured on a 100 mm VAS, where 0 mm = lowest disease activity and 100 mm = highest. Participants with missing data were considered non-responders. (NCT00456092)
Timeframe: Baseline and Week 24

Percentage of Participants With DAS28-CRP(3) Score of Mild Disease Activity or In Remission at Week 12

The DAS28-CRP(3) measures the severity of disease derived from the following 3 variables: • 28 tender joint count (does not include the DIP joints, the hip joint, or the joints below the knee) • 28 swollen joint count • C-reactive protein (CRP) DAS28-CRP(3) scores range from 0 to 9.4, where higher scores indicate more disease activity. Mild disease severity is defined as a DAS28-CRP(3) score of ≤ 3.2. In remission is defined as a DAS28-CRP(3) score of ≤ 2.6. (NCT00456092)
Timeframe: Week 12

Percentage of Participants With DAS28-CRP(4) Score of Mild Disease Activity or In Remission at Week 12

The DAS28-CRP(4) measures the severity of disease derived from the following 4 variables: • 28 tender joint count, (does not include the DIP joints, the hip joint, or the joints below the knee) • 28 swollen joint count • C-reactive protein (CRP) • Patient's global assessment of disease activity. DAS28-CRP(4) scores range from 0 to 9.4, where higher scores indicate more disease activity. Mild disease severity is defined as a DAS28-CRP(4) score of ≤ 3.2. In remission is defined as a DAS28-CRP(4) score of ≤ 2.6. (NCT00456092)
Timeframe: Week 12

Percentage of Participants With Good or Moderate EULAR Response Based on DAS28-CRP(3) at Week 12

The DAS28 measures the severity of disease at a specific time. DAS28-CRP(3) is derived from the following 3 variables: • 28 tender joint count, (does not include the DIP joints, the hip joint, or the joints below the knee) • 28 swollen joint count • C-reactive protein (CRP) according to the formula: DAS28-CRP(3) = [0.56*√(TJC28) + 0.28*√(SJC28) + 0.36*ln(CRP+1)] * 1.10 + 1.15. DAS28 scores range from 0 to 9.4, where higher scores indicate more disease activity. A EULAR response reflects an improvement in disease activity based on the DAS-28 score. A Good Response is defined as an improvement (decrease) in the DAS28 > 1.2 from Baseline and attainment of a DAS28 score ≤ 3.2. A Moderate Response is defined as either: • an improvement (decrease) in the DAS28 > 0.6 and ≤ 1.2 and a DAS28 score ≤ to 5.1 or, • an improvement (decrease) in the DAS28 > 1.2 and a DAS28 score > 3.2 (NCT00456092)
Timeframe: Baseline and Week 12

Percentage of Participants With Good or Moderate EULAR Response Based on DAS28-CRP(3) at Week 24

Percentage of Participants With Good or Moderate EULAR Response Based on DAS28-CRP(4) at Week 24

The DAS28 measures the severity of disease at a specific time. DAS28-CRP(4) is derived from the following 4 variables: • 28 tender joint count, (does not include the DIP joints, the hip joint, or the joints below the knee) • 28 swollen joint count • C-reactive protein • Patient's global assessment of disease activity according to the formula: DAS28-CRP(4) = 0.56*√(TJC28) + 0.28*(SJC28) + 0.36*ln(CRP+1) + 0.014*GH + 0.96. DAS28 scores range from 0 to 9.4, where higher scores indicate more disease activity. A EULAR response reflects an improvement in disease activity based on the DAS-28 score. A Good Response is defined as an improvement (decrease) in the DAS28 > 1.2 from Baseline and attainment of a DAS28 score ≤ 3.2. A Moderate Response is defined as either: • an improvement (decrease) in the DAS28 > 0.6 and ≤ 1.2 and a DAS28 score ≤ to 5.1 or, • an improvement (decrease) in the DAS28 > 1.2 and a DAS28 score > 3.2 (NCT00456092)
Timeframe: Baseline and Week 24

Percentage of Participants With Good or Moderate European League Against Rheumatism (EULAR) Response Based on Disease Activity Score (DAS28)-CRP(4) at Week 12

The DAS28 measures the severity of disease at a specific time. DAS28-CRP(4) is derived from the following 4 variables: • 28 tender joint count, (TJC; does not include the DIP joints, the hip joint, or the joints below the knee) • 28 swollen joint count (SJC) • C-reactive protein (CRP) • Patient's global assessment of disease activity (GH) according to the formula: DAS28-CRP(4) = 0.56*√(TJC28) + 0.28*(SJC28) + 0.36*ln(CRP+1) + 0.014*GH + 0.96. DAS28 scores range from 0 to 9.4, where higher scores indicate more disease activity. A EULAR response reflects an improvement in disease activity based on the DAS-28 score. A Good Response is defined as an improvement (decrease) in the DAS28 > 1.2 from Baseline and a DAS28 score ≤ 3.2. A Moderate Response is defined as either: • an improvement (decrease) in the DAS28 > 0.6 and ≤ 1.2 and a DAS28 score ≤ to 5.1 or, • an improvement (decrease) in the DAS28 > 1.2 and a DAS28 score > 3.2 (NCT00456092)
Timeframe: Baseline and Week 12

Time to ACR 20 Response During the Study

Time to ACR 20 was measured from the first dose of apremilast to the first time a participant achieved an ACR 20 response in the treatment or extension phase. The Kaplan-Meier estimates of time to ACR 20 response were calculated for participants who had an ACR 20 response at any time during the study. (NCT00456092)
Timeframe: Baseline to Week 24

Time to ACR 20 Response During the Treatment Phase

The Kaplan-Meier estimates of time to ACR 20 response was calculated for participants who had an ACR 20 response at any time during the treatment phase. (NCT00456092)
Timeframe: Baseline to Week 12

Time to ACR 50 Response During the Treatment and Extension Phase

Time to ACR 50 response was measured from the first dose of apremilast to the first time a participant achieved an ACR 50 response in the treatment or extension phase. The Kaplan-Meier estimates of time to ACR 50 response were calculated for participants who had an ACR 50 response at any time during the study. (NCT00456092)
Timeframe: Baseline to Week 24

Time to ACR 50 Response During the Treatment Phase

The Kaplan-Meier estimates of time to ACR 50 response was calculated for participants who had an ACR 50 response at any time during the treatment phase. (NCT00456092)
Timeframe: Baseline to Week 12

Time to ACR 70 Response During the Treatment and Extension Phase

Time to ACR 70 response was measured from the first dose of apremilast to the first time a participant achieved an ACR 70 response in the treatment or extension phase. The Kaplan-Meier estimates of time to ACR 70 response were calculated for participants who had an ACR 70 response at any time during the study. (NCT00456092)
Timeframe: Baseline to Week 24

Time to ACR 70 Response During the Treatment Phase

The Kaplan-Meier estimates of time to ACR 70 response was calculated for participants who had an ACR 70 response at any time during the treatment phase. (NCT00456092)
Timeframe: Baseline to Week 12

Change From Baseline and Week 12 in Dactylitis Severity Score at Week 24

Change From Baseline and Week 12 in Dermatology Life Quality Index (DLQI) at Week 24

The DLQI is a validated, self-administered, 10-item questionnaire that measures the impact of skin disease on participants' quality of life, based on recall over the past week. Domains include symptoms, feelings, daily activities, leisure, work, personal relationships, and treatment. Each question is answered on a scale from 0 (not at all) to 3 (very much) The total score ranges from 0 to 30 where a higher score indicates that a participant's dermatological condition has a greater impact on their daily life. (NCT00456092)
Timeframe: Baseline (Day 1), Week 12 (Day 85) and Week 24

Change From Baseline and Week 12 in SF-36 at Week 24

The Medical Outcome SF 36-Item Health Survey, Version 2 is a self-administered instrument that measures the impact of disease on overall quality of life and consists of 36 questions in eight domains (physical function, pain, general and mental health, vitality, social function, physical and emotional health). The summary physical health score included the following subscales: physical functioning, role-physical, bodily pain, and general health. The summary mental health score included other subscales: vitality, social functioning, role-emotional, and mental health. Norm-based scores were used in analyses, calibrated so that 50 is the average score and the standard deviation equals 10, where higher scores are associated with better functioning/quality of life. Each domain is scored by summing the individual items and transforming the scores into a 0 to 100 scale. A higher change from baseline indicates an improvement in better health results or functioning. (NCT00456092)
Timeframe: Baseline (Day 1), Week 12 (Day 85) and Week 24

Change From Baseline and Week 12 in the Health Assessment Questionnaire Disability Index (HAQ-DI) at Week 24

Change From Baseline in Short Form 36 (SF-36) Summary Physical and Mental Component Scores at Week 12

Change From Baseline in the Functional Assessment of Chronic Illness Therapy for Fatigue (FACIT-F) at Week 24

Number of Participants With Adverse Events During the Extension Phase

The severity of each adverse event (AE) was graded based upon the participant's symptoms according to National Cancer Institute (NCI) Common Toxicity Criteria (CTCAE, Version 3.0), on a scale from 1 (Mild AE) to 5 (Death due to AE). Severe AEs are defined as NCI CTCAE grade 3 or higher. AEs related to study drug are those determined by the investigator as suspected to be related to study drug where a temporal relationship of the adverse event to study drug administration made a causal relationship possible, and other medications, therapeutic interventions, or underlying conditions did not provide a sufficient explanation for the observed event. A serious adverse event (SAE) is any AE which: - Resulted in death - Was life-threatening - Required inpatient hospitalization or prolongation of existing hospitalization - Resulted in persistent or significant disability/incapacity - Was a congenital anomaly/birth defect - Constituted an important medical event. (NCT00456092)
Timeframe: Weeks 12 to 24 (Extension Phase)

Number of Participants With Adverse Events During the Treatment Phase

Percentage of Participants With a Modified ACR 20 Response at Week 24

A modified ACR 20 response was defined as a participant who met the following 3 criteria for improvement: • ≥ 20% improvement in 78 tender joint count (includes 10 additional joints often involved in psoriatic arthritis: the first carpometacarpal [CMC] and the distal interphalangeal [DIP] joints of the fingers); • ≥ 20% improvement in 76 swollen joint count; and • ≥ 20% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm VAS); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. Response at Week 24 was measured as improvement from Baseline (Day 1) and from Week 12 (Day 85). Participants with no post-baseline ACR scores were considered non-responders. (NCT00456092)
Timeframe: Baseline (Day 1), Week 12 (Day 85) and Week 24

Percentage of Participants With a Modified ACR 50 Response at Week 24

A modified ACR 50 response was defined as a participant who met the following 3 criteria for improvement: • ≥ 50% improvement in 78 tender joint count (includes 10 additional joints often involved in psoriatic arthritis: the first carpometacarpal [CMC] and the distal interphalangeal [DIP] joints of the fingers); • ≥ 50% improvement in 76 swollen joint count; and • ≥ 50% improvement in at least 3 of the 5 following parameters: ◦ Patient's assessment of pain (measured on a 100 mm VAS); ◦ Patient's global assessment of disease activity (measured on a 100 mm VAS); ◦ Physician's global assessment of disease activity (measured on a 100 mm VAS); ◦ Patient's self-assessment of physical function (Health Assessment Questionnaire - Disability Index [HAQ-DI]); ◦ C-reactive protein. Response at Week 24 was measured as improvement from Baseline (Day 1) and from Week 12 (Day 85). Participants with no post-baseline ACR scores were considered non-responders. (NCT00456092)
Timeframe: Baseline (Day 1), Week 12 (Day 85) and Week 24

Percentage of Participants With Enthesitis

Enthesitis is inflammation of the entheses, the sites where tendons or ligaments insert into the bone. Enthesitis is characterized by swelling, pain, and tenderness around the calcaneous, and occasionally by effusion in the bursa associated with this joint. The enthesitis assessment is an evaluation of inflammation at the insertions of the Achilles tendon into the calcaneous and of the plantar fascia into the calcaneous. Inflammation at 1 or more insertions on either the right or left side constituted a positive assessment. (NCT00456092)
Timeframe: Baseline and Week 12

Percentage of Participants With Enthesitis in the Extension Phase

Time to Relapse of Psoriatic Arthritis After Extension Phase

Relapse of psoriatic arthritis was defined as a 50% loss of the maximal ACR improvement during the Follow-up Phase in participants who achieved at least an ACR 20 at their Final Extension Phase (Week 24)/Early Termination Visit. The time to relapse during the Follow-up Phase was calculated from the time of maximum ACR reduction and from the date of the Final Extension Phase visit. Participants classified as responders who did not relapse were censored at the day of the last follow-up. (NCT00456092)
Timeframe: From Week 24 to the end of the 28-day follow-up (1) and from the date of maximal ACR until the end of the 28-day follow-up phase (2).

Time to Relapse of Psoriatic Arthritis During the Observational Follow-up Phase

Relapse of psoriatic arthritis was defined as a 50% loss of the maximal ACR improvement during the Observation Phase in participants who received apremilast and achieved at least an ACR 20 at their Final Treatment Phase/Early Termination Visit. The time to relapse during the Observational Phase was calculated from the time of maximum ACR reduction and from the date of the Final Treatment Phase visit. Participants classified as responders who did not relapse were censored at the day of the last follow-up. (NCT00456092)
Timeframe: From Week 12 to end of 28-day observational follow-up (1) and from the date of maximal ACR during the 12-week Treatment Phase until the end of the 28-day observational follow-up phase (2).

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	93.8
Placebo / Apremilast 30 mg	94.7
Apremilast 20 mg	87.1
Apremilast 30 mg	85.9

Intervention	Percentage of Participants (Number)
Placebo / Apremilast 20 mg	75.0
Placebo / Apremilast 30 mg	78.9
Apremilast 20 mg	68.6
Apremilast 30 mg	68.8

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	39.0
Placebo / Apremilast 30 mg	61.9
Apremilast 20 mg	39.6
Apremilast 30 mg	45.9

Intervention	Participants (Count of Participants)
	Any TEAE	Any Drug-Related TEAE	Any Severe TEAE	Any Serious TEAE (SAE)	Drug-Related (SAE)	Any TEAE Leading to Drug Interruption	Any TEAE Leading to Drug Wirhdrawal	Any TEAE Leading to Death
Apremilast 20 mg (Pre-Switch)	188	89	24	35	6	41	22	0
Apremilast 20/30 mg (Post-Switch)	60	16	3	5	1	5	2	0
Apremilast 30 mg	204	113	23	36	6	36	26	0

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-0.208
Placebo / Apremilast 30 mg	-0.310
Apremilast 20 mg	-0.192
Apremilast 30 mg	-0.330

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-2.5
Placebo / Apremilast 30 mg	-2.5
Apremilast 20 mg	-1.7
Apremilast 30 mg	-2.1

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-13.66
Placebo / Apremilast 30 mg	-13.13
Apremilast 20 mg	-12.03
Apremilast 30 mg	-14.38

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-1.18
Placebo / Apremilast 30 mg	-1.18
Apremilast 20 mg	-1.11
Apremilast 30 mg	-1.30

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	1.97
Placebo / Apremilast 30 mg	4.95
Apremilast 20 mg	2.45
Apremilast 30 mg	4.38

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	4.13
Placebo / Apremilast 30 mg	5.97
Apremilast 20 mg	4.05
Apremilast 30 mg	4.97

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	78.3
Placebo / Apremilast 30 mg	77.8
Apremilast 20 mg	57.9
Apremilast 30 mg	65.0

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	42.5
Placebo / Apremilast 30 mg	41.0
Apremilast 20 mg	40.0
Apremilast 30 mg	37.2

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	70.0
Placebo / Apremilast 30 mg	64.5
Apremilast 20 mg	68.0
Apremilast 30 mg	67.5

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	53.3
Placebo / Apremilast 30 mg	47.5
Apremilast 20 mg	52.9
Apremilast 30 mg	52.6

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	30.5
Placebo / Apremilast 30 mg	27.4
Apremilast 20 mg	26.7
Apremilast 30 mg	18.6

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	16.9
Placebo / Apremilast 30 mg	14.3
Apremilast 20 mg	9.8
Apremilast 30 mg	6.8

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	95.7
Placebo / Apremilast 30 mg	88.9
Apremilast 20 mg	80.7
Apremilast 30 mg	85.0

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	72.5
Placebo / Apremilast 30 mg	79.5
Apremilast 20 mg	70.0
Apremilast 30 mg	69.2

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-0.27
Placebo / Apremilast 30 mg	-0.29
Apremilast 20 mg	-0.37
Apremilast 30 mg	-0.32

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-15.00
Placebo / Apremilast 30 mg	-14.03
Apremilast 20 mg	-15.41
Apremilast 30 mg	-14.54

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-0.8
Placebo / Apremilast 30 mg	-2.4
Apremilast 20 mg	-2.7
Apremilast 30 mg	-1.8

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	-1.47
Placebo / Apremilast 30 mg	-1.15
Apremilast 20 mg	-1.40
Apremilast 30 mg	-1.31

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	4.33
Placebo / Apremilast 30 mg	4.15
Apremilast 20 mg	4.27
Apremilast 30 mg	3.67

Intervention	mm (Mean)
Placebo / Apremilast 20 mg	-20.2
Placebo / Apremilast 30 mg	-21.0
Apremilast 20 mg	-17.8
Apremilast 30 mg	-20.3

Intervention	units on a scale (Mean)
Placebo / Apremilast 20 mg	4.46
Placebo / Apremilast 30 mg	4.62
Apremilast 20 mg	6.98
Apremilast 30 mg	5.69

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	52.2
Placebo / Apremilast 30 mg	53.8
Apremilast 20 mg	68.8
Apremilast 30 mg	63.3

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	33.3
Placebo / Apremilast 30 mg	27.8
Apremilast 20 mg	50.7
Apremilast 30 mg	38.2

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	82.8
Placebo / Apremilast 30 mg	70.0
Apremilast 20 mg	75.0
Apremilast 30 mg	74.4

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	53.1
Placebo / Apremilast 30 mg	50.0
Apremilast 20 mg	63.0
Apremilast 30 mg	54.6

Intervention	percentage of participants (Number)
Placebo / Apremilast 20 mg	4.8
Placebo / Apremilast 30 mg	14.8
Apremilast 20 mg	15.4
Apremilast 30 mg	13.8