diclofenac and Osteoarthritis of Knee studies

Diclofenac: A non-steroidal anti-inflammatory agent (NSAID) with antipyretic and analgesic actions. It is primarily available as the sodium salt.
diclofenac : A monocarboxylic acid consisting of phenylacetic acid having a (2,6-dichlorophenyl)amino group at the 2-position.

Research Excerpts

Excerpt	Relevance	Reference
"To evaluate the efficacy and safety of intra-articular injection of diclofenac etalhyaluronate (DF-HA) in patients with osteoarthritis (OA) of the hip, ankle, shoulder, or elbow."	9.51	Diclofenac-hyaluronate conjugate (diclofenac etalhyaluronate) intra-articular injection for hip, ankle, shoulder, and elbow osteoarthritis: a randomized controlled trial. ( Ikegami, H; Kano, K; Kubo, T; Kumai, T; Nishii, M; Seo, T, 2022)
"To compare the efficacy and safety of ketoprofen plasters and diclofenac plasters after 3 weeks of administration in patients with osteoarthritis-related knee pain."	9.41	Comparison of the Efficacy and Safety of Ketoprofen Plaster and Diclofenac Plaster for Osteoarthritis-Related Knee Pain: A Multicenter, Randomized, Active-Controlled, Open-Label, Parallel-Group, Phase III Clinical Trial. ( Cha, JE; Ershova, O; Hyun, BJ; Kastanayan, A; Krechikova, D; Nikulenkova, N; Polyakova, S; Shvarts, Y; Vinogradova, I; Yakushin, S, 2021)
"Joint pain decreased after 2 weeks of therapy in all patients during treatment with Voltaren Emulgel 2% (diclofenac diethylamine 2%) in both groups."	8.02	[Evaluation of topical therapy of patients with osteoarthritis of small joints of the hands with Voltaren® Emulgel® 2% (diclofenac diethylamine 2%)]. ( Gromova, MA; Tsurko, VV, 2021)
"To evaluate the safety of topical diclofenac sodium 1% gel (DSG) for knee and hand osteoarthritis (OA) in older and younger patients and in patients with versus without comorbid hypertension, type 2 diabetes, or cerebrovascular or cardiovascular disease."	7.78	Tolerability of topical diclofenac sodium 1% gel for osteoarthritis in seniors and patients with comorbidities. ( Baraf, HS; Gold, MS; Petruschke, RA; Wieman, MS, 2012)
"5% dimethyl sulfoxide (TDiclo) for the treatment of knee or hand osteoarthritis in persons aged 75 years or older."	7.78	Pooled safety analysis of diclofenac sodium topical solution 1.5% (w/w) in the treatment of osteoarthritis in patients aged 75 years or older. ( Fuller, P; Roth, SH, 2012)
" The chronic use of diclofenac sodium can lead to adverse gastrointestinal problems."	6.43	The use of topical diclofenac for pain in osteoarthritis of the knee: a review. ( Banning, M, 2006)
"Dry needling on latent and active MTrPs combined with stretching and oral diclofenac combined with stretching can effectively relieve pain, improve function, and restore knee ROM affected by KOA."	5.69	Dry needling on latent and active myofascial trigger points versus oral diclofenac in patients with knee osteoarthritis: a randomized controlled trial. ( Dong, YL; Huang, QM; Ma, YT; Wang, B; Xie, WP; Zheng, YJ, 2023)
"Non-inferiority of SFPP to diclofenac gel was demonstrated in the efficacy for pain on rising from a chair."	5.51	Efficacy and safety of S-flurbiprofen plaster in knee osteoarthritis patients: A 2-week randomized controlled Phase III clinical trial compared to diclofenac gel. ( Fuady, A; Matsumoto, H; Tomatsu, K; Yasuda, S, 2022)
"To evaluate the efficacy and safety of intra-articular injection of diclofenac etalhyaluronate (DF-HA) in patients with osteoarthritis (OA) of the hip, ankle, shoulder, or elbow."	5.51	Diclofenac-hyaluronate conjugate (diclofenac etalhyaluronate) intra-articular injection for hip, ankle, shoulder, and elbow osteoarthritis: a randomized controlled trial. ( Ikegami, H; Kano, K; Kubo, T; Kumai, T; Nishii, M; Seo, T, 2022)
"To compare the efficacy and safety of ketoprofen plasters and diclofenac plasters after 3 weeks of administration in patients with osteoarthritis-related knee pain."	5.41	Comparison of the Efficacy and Safety of Ketoprofen Plaster and Diclofenac Plaster for Osteoarthritis-Related Knee Pain: A Multicenter, Randomized, Active-Controlled, Open-Label, Parallel-Group, Phase III Clinical Trial. ( Cha, JE; Ershova, O; Hyun, BJ; Kastanayan, A; Krechikova, D; Nikulenkova, N; Polyakova, S; Shvarts, Y; Vinogradova, I; Yakushin, S, 2021)
"osteoarthritis of knee compared to 1% diclofenac gel as an active control."	5.24	A Comparative of Ginger Extract in Nanostructure Lipid Carrier (NLC) and 1% Diclofenac Gel for Treatment of Knee Osteoarthritis (OA). ( Amorndoljai, P; Niempoog, S; Nimmannit, U; Taneepanichskul, S, 2017)
"A phase II, 4 week, randomized, double-blind, parallel-group, two-arm, vehicle-controlled study compared pain relief with diclofenac sodium 2% topical solution versus control (vehicle only) in patients aged 40 to 85 years with radiographically confirmed primary OA of the knee."	5.22	Efficacy and safety of diclofenac sodium 2% topical solution for osteoarthritis of the knee: a randomized, double-blind, vehicle-controlled, 4 week study. ( Holt, RJ; Kent, JD; Wadsworth, LT, 2016)
"Patients with knee OA (n = 35) were compared on QST responses to a demographically-matched pain-free control group (n = 39), after which patients completed a month-long treatment study of diclofenac sodium topical gel (1 %), applied up to 4 times daily."	5.22	Variability in conditioned pain modulation predicts response to NSAID treatment in patients with knee osteoarthritis. ( Cornelius, M; Dolman, AJ; Edwards, RR; Finan, PH; Lazaridou, A; Martel, MO; Wasan, AD, 2016)
"To evaluate the effects of mesotherapy with diclofenac for anserine bursitis associated with knee osteoarthritis."	5.20	Pes Anserine Bursitis in Symptomatic Osteoarthritis Patients: A Mesotherapy Treatment Study. ( Bellomo, RG; Di Stefano, A; Dodaj, I; Saggini, R; Scarcello, L, 2015)
"Hyaluronic acid alone and in combination with sodium clodronate or diclofenac sodium produced a significant improvement in mean VAS pain score at 3 and 6-month follow-up."	5.17	Preliminary study of highly cross-linked hyaluronic acid-based combination therapy for management of knee osteoarthritis-related pain. ( Iannitti, T; Palmieri, B; Rottigni, V, 2013)
" The meta-analysis indicated that celecoxib reduced pain more effectively than diclofenac sodium in patients with KOA, as evaluated by the VAS score."	5.12	Meta-analysis Comparing Celecoxib with Diclofenac Sodium in Patients with Knee Osteoarthritis. ( Hou, S; Huang, H; Liang, G; Liang, H; Liu, J; Luo, M; Pan, J; Yang, W; Zeng, L; Zhao, J, 2021)
"Topical diclofenac and ketoprofen are the most rigorously studied topical NSAIDs in the treatment of knee OA and have demonstrated the most significant reduction in pain and improvement of function."	5.12	Topical nonsteroidal anti-inflammatory drugs in the treatment of knee osteoarthritis: a systematic review and meta-analysis. ( Brown, SM; Christophersen, C; Mulcahey, MK; Wolff, DG, 2021)
" In the first few weeks of treatment, the mean changes in some variables (VAS, which assessed walking pain, standing pain and stiffness, as well as Lequesne's functional index) of the DJW group were significantly lower than those of the diclofenac group."	5.11	Chinese herbal recipe versus diclofenac in symptomatic treatment of osteoarthritis of the knee: a randomized controlled trial [ISRCTN70292892]. ( Kunanusorn, P; Lhieochaiphunt, S; Pojchamarnwiputh, S; Pruksakorn, S; Rojanasthien, N; Sananpanich, K; Teekachunhatean, S, 2004)
"The topical diclofenac group had a significantly greater mean change in score (final minus baseline) compared to the vehicle control group for pain (-5."	5.11	Treatment of osteoarthritis of the knee with a topical diclofenac solution: a randomised controlled, 6-week trial [ISRCTN53366886]. ( Baer, PA; Shainhouse, Z; Thomas, LM, 2005)
"To analyse the efficacy of acupuncture as a complementary therapy to the pharmacological treatment of osteoarthritis of the knee, with respect to pain relief, reduction of stiffness, and increased physical function during treatment; modifications in the consumption of diclofenac during treatment; and changes in the patient's quality of life."	5.11	Acupuncture as a complementary therapy to the pharmacological treatment of osteoarthritis of the knee: randomised controlled trial. ( Aguilar, I; Borge, MA; Gaspar, O; Jurado, R; León, JM; Méndez, C; Panadero, MD; Perea-Milla, E; Sánchez-Rodríguez, F; Vas, J; Vega, E, 2004)
"The nonsteroidal anti-inflammatory drug (NSAID) diclofenac epolamine (DHEP) formulated as a topical patch has demonstrated efficacy and safety in the localized treatment of acute pain from minor strains, sprains and contusions, and for epicondylitis and knee osteoarthritis."	5.01	Rationale and evidence for the incorporation of heparin into the diclofenac epolamine medicated plaster. ( Jones, C; Nencioni, A; Rainsford, KD; Roberts, MS, 2019)
" All treatments except acetaminophen showed clinically significant improvement from baseline pain."	4.91	Comparative effectiveness of pharmacologic interventions for knee osteoarthritis: a systematic review and network meta-analysis. ( Bannuru, RR; Kent, DM; McAlindon, TE; Schmid, CH; Vaysbrot, EE; Wong, JB, 2015)
" In patients with neuropathic pain, topical forms of both capsaicin and lidocaine have been shown to be useful in the treatment of postherpetic neuralgia and diabetic peripheral neuropathic pain."	4.89	Topical therapies in the management of chronic pain. ( Galluzzi, KE; Stanos, SP, 2013)
"Joint pain decreased after 2 weeks of therapy in all patients during treatment with Voltaren Emulgel 2% (diclofenac diethylamine 2%) in both groups."	4.02	[Evaluation of topical therapy of patients with osteoarthritis of small joints of the hands with Voltaren® Emulgel® 2% (diclofenac diethylamine 2%)]. ( Gromova, MA; Tsurko, VV, 2021)
"5% dimethyl sulfoxide (TDiclo) for the treatment of knee or hand osteoarthritis in persons aged 75 years or older."	3.78	Pooled safety analysis of diclofenac sodium topical solution 1.5% (w/w) in the treatment of osteoarthritis in patients aged 75 years or older. ( Fuller, P; Roth, SH, 2012)
"To evaluate the safety of topical diclofenac sodium 1% gel (DSG) for knee and hand osteoarthritis (OA) in older and younger patients and in patients with versus without comorbid hypertension, type 2 diabetes, or cerebrovascular or cardiovascular disease."	3.78	Tolerability of topical diclofenac sodium 1% gel for osteoarthritis in seniors and patients with comorbidities. ( Baraf, HS; Gold, MS; Petruschke, RA; Wieman, MS, 2012)
" Adverse events (AEs) were similar between patients treated with tanezumab 2."	3.01	Long-Term Safety and Efficacy of Subcutaneous Tanezumab Versus Nonsteroidal Antiinflammatory Drugs for Hip or Knee Osteoarthritis: A Randomized Trial. ( Brown, MT; Carrino, JA; Fountaine, RJ; Guermazi, A; Hickman, A; Hochberg, MC; Nakajo, S; Pixton, G; Schnitzer, TJ; Verburg, KM; Viktrup, L; Walsh, DA; West, CR; White, A, 2021)
" Safety was evaluated by adverse event monitoring."	3.01	Efficacy and Safety of Diclofenac-Hyaluronate Conjugate (Diclofenac Etalhyaluronate) for Knee Osteoarthritis: A Randomized Phase III Trial in Japan. ( Kano, K; Nishida, Y; Nobuoka, Y; Seo, T, 2021)
" Observation indicators included: the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC), Hospital for Special Surgery Knee Score (HSS), liver and kidney function, adverse reactions, and so on."	3.01	Efficacy and safety of Biqi capsule in the treatment of knee osteoarthritis: A protocol of a randomized controlled trial. ( Huang, H; Jia, M; Tian, K; Wang, W; Zhou, Y, 2021)
" Safety after treatment was evaluated by recording adverse events and laboratory investigations."	2.94	Efficacy and safety of combination of curcuminoid complex and diclofenac versus diclofenac in knee osteoarthritis: A randomized trial. ( Gade, P; Karad, S; Khanwelkar, C; Shep, D, 2020)
"Pelubiprofen was considered non-inferior to aceclofenac if the upper limit of the one-sided 97."	2.94	Efficacy and safety of short-term use of a pelubiprofen CR and aceclofenac in patients with symptomatic knee osteoarthritis: A double-blinded, randomized, multicenter, active drug comparative, parallel-group, phase IV, non-inferiority clinical trial. ( Chang, MJ; Han, SB; Kang, SB; Kim, KI; Kim, MK; Kim, SH; Lee, HJ; Lee, S; Moon, YW; Park, HG; Shin, JY; Yoo, JD, 2020)
"Curcumin has similar efficacy to diclofenac but demonstrated better tolerance among patients with knee OA."	2.90	Safety and efficacy of curcumin versus diclofenac in knee osteoarthritis: a randomized open-label parallel-arm study. ( Gade, P; Karad, S; Khanwelkar, C; Shep, D, 2019)
" No difference in adverse events was observed between the two groups."	2.87	Efficacy and safety of adalimumab by intra-articular injection for moderate to severe knee osteoarthritis: An open-label randomized controlled trial. ( Wang, J, 2018)
" In addition, the rate of adverse reaction of research group was also lower than that of control group, P<0."	2.87	Clinical therapeutic effect and safety of celecoxib in treating knee osteoarthritis. ( Bi, J; Yu, C; Yu, X; Yu, Z; Zhao, L, 2018)
"Knee osteoarthritis is a common form of arthritis in elderly patients that is characterised by pain and functional limitation."	2.84	Moxibustion versus diclofenac sodium gel for the treatment of knee osteoarthritis: a study protocol for a double-blinded, double-placebo, randomised controlled trial. ( Luo, L; Lv, P; Peng, JX; Tang, Y; Wu, Q; Yin, HY; Yu, SG; Zhang, CS; Zhou, JY; Zhu, LL, 2017)
" The recommended dosing regimens have generally ranged from 3 to 5 injections."	2.82	Efficacy of a Single Intra-Articular Injection of 2% Sodium Hyaluronate Plus 0.5% Mannitol in Patients with Symptomatic Osteoarthritis of the Knee: A Preliminary Report. ( Lamsam, C; Lertwanich, P, 2016)
" Any observed adverse effects were also scrutinized."	2.82	Efficacy and short-term safety of topical Dwarf Elder (Sambucus ebulus L.) versus diclofenac for knee osteoarthritis: A randomized, double-blind, active-controlled trial. ( Emtiazy, M; Hashempur, MH; Jabbari, M; Kamalinejad, M; Razavi, SZ; Shahraki, HR, 2016)
" The test group (n = 41) was given Compound DCR with the dosage of 1."	2.80	[Controlled clinical study on compound Decumbent Corydalis Rhizome and diclofenac in treatment of knee osteoarthritis]. ( Cen, XM; Xie, QB; Yin, G; Zuo, C, 2015)
"Diclofenac is used for the treatment of osteoarthritis (OA); however, like other nonsteroidal anti-inflammatory drugs (NSAIDs) it can be associated with serious dose-related adverse events (AEs)."	2.80	Low-dose SoluMatrix diclofenac in the treatment of osteoarthritis: A 1-year, open-label, Phase III safety study. ( Altman, RD; Cryer, B; Gibofsky, A; Hochberg, MC; Hopkins, WE; Imasogie, O; Kivitz, A; Markenson, JA; Nezzer, J; Strand, V; Young, CL, 2015)
"Knee osteoarthritis is one of the most prevalent chronic disorders."	2.80	Comparative effectiveness of B and e vitamins with diclofenac in reducing pain due to osteoarthritis of the knee. ( Dehghan, M, 2015)
"NSAIDs, such as diclofenac, are the most commonly used medications to treat osteoarthritis (OA), but they are associated with dose-related adverse events (AEs)."	2.79	Efficacy and safety of low-dose submicron diclofenac for the treatment of osteoarthritis pain: a 12 week, phase 3 study. ( Gibofsky, A; Hochberg, MC; Jaros, MJ; Young, CL, 2014)
" The incidence of adverse events of abnormal peripheral sensation was lower than in previous tanezumab trials."	2.79	Efficacy and safety of tanezumab added on to diclofenac sustained release in patients with knee or hip osteoarthritis: a double-blind, placebo-controlled, parallel-group, multicentre phase III randomised clinical trial. ( Balanescu, AR; Brown, MT; Davignon, I; Feist, E; Smith, MD; West, CR; Wolfram, G, 2014)
"Aceclofenac was better tolerated in terms of incidence and severity of GI AEs and GPA requirement and was as efficacious as diclofenac."	2.78	Comparison of gastrointestinal safety and tolerability of aceclofenac with diclofenac: a multicenter, randomized, double-blind study in patients with knee osteoarthritis. ( Chandurkar, N; Pareek, A, 2013)
"Osteoarthritis of the knee is one of the most common public health problems in Thailand and throughout the world."	2.77	Phase II clinical trial of Ayurved Siriraj Wattana Recipe for symptomatic relief in patients with osteoarthritis of the knee. ( Akarasereenont, P; Charoencholvanich, K; Chatsiricharoenkul, S; Pengkhum, T, 2012)
"Aceclofenac-CR treated patients took fewer acetaminophen and ranitidine tablets during the treatment period as compared to conventional aceclofenac treated patients."	2.76	Efficacy and safety of aceclofenac-cr and aceclofenac in the treatment of knee osteoarthritis: a 6-week, comparative, randomized, multicentric, double-blind study. ( Chandurkar, N; Dalal, B; Gupta, A; Jesalpura, B; Mehrotra, A; Mukherjee, A; Pareek, A; Sirsikar, A, 2011)
" Both the study medications were well tolerated with no incidence of serious adverse events."	2.76	Zaltoprofen, a noninferior alternative to diclofenac for the treatment of primary knee osteoarthritis -- a comparative evaluation of efficacy and safety in a 4-week, multicentric, randomized, double-blind, double-dummy trial. ( Ambade, RE; Chandurkar, NB; Gupta, AK; Jesalpura, BH; Pareek, A; Sirsikar, AD; Swamy, AP, 2011)
" Safety was evaluated through adverse event (AE) reporting, physical examination, and laboratory investigations."	2.76	An open-label, long-term safety and tolerability trial of diclofenac sodium 1% gel in patients with knee osteoarthritis. ( Alwine, LK; Gold, MS; Peniston, JH, 2011)
" Treatment-related adverse events (AEs) were infrequent (DSG, 7."	2.75	Safety and efficacy of topical diclofenac sodium 1% gel in knee osteoarthritis: a randomized controlled trial. ( Altman, RD; Baraf, HS; Clark, MB; Gold, MS, 2010)
"To observe the curative effect of Chinese drugs-paste separated moxibustion combined with electroacupuncture (EA) for knee osteoarthritis (KOA)."	2.75	[Clinical observation on the therapeutic effect of drugs-paste separated moxibustion combined with electroacupunture for knee osteoarthritis patients of cold-damp type]. ( Chen, RL; Ji, L; Miao, FR; Zhu, Y, 2010)
" The commonest adverse event associated with TDiclo was dry skin (18."	2.74	Efficacy and safety of topical diclofenac containing dimethyl sulfoxide (DMSO) compared with those of topical placebo, DMSO vehicle and oral diclofenac for knee osteoarthritis. ( Bookman, AAM; Grierson, LM; Naseer, Z; Shainhouse, ZJ; Simon, LS, 2009)
"The incidence of gastrointestinal disorders was 5."	2.74	Randomized controlled trial of diclofenac sodium gel in knee osteoarthritis. ( Altman, RD; Barthel, HR; Gold, MS; Haselwood, D; Longley, S, 2009)
" Moreover, erythrocyte sedimentation rate (ESR), blood C-reactive protein (CRP), blood and urinary routine tests, liver and kidney function examination, and the adverse reaction that occurred during the treatment period were observed."	2.74	Clinical efficacy and safety of Gubitong Recipe () in treating osteoarthritis of knee joint. ( Jin, DE; Tao, QW; Xu, Y; Yan, XP, 2009)
"Celecoxib was not significantly different from placebo in this analysis (P = 0."	2.72	First-dose analgesic effect of the cyclo-oxygenase-2 selective inhibitor lumiracoxib in osteoarthritis of the knee: a randomized, double-blind, placebo-controlled comparison with celecoxib [NCT00267215]. ( Burger, KJ; Fashola, TO; Krehan, G; Maeumbaed, R; Runge, H; Schell, E; Schlüter, P; Thurston, HJ; Trechsel, U; Wittenberg, RH, 2006)
" The incidences of related adverse events were 35."	2.72	Evaluation of efficacy and safety of diacerein in knee osteoarthritis in Chinese patients. ( Huang, F; Li, J; Li, ZG; Liang, DF; Ma, L; Su, Y; Tang, FL; Wu, DH; Xu, H; Zhang, FC; Zhang, JL; Zheng, WJ; Zhou, HQ; Zhou, YX, 2006)
" Efficacy assessments included overall joint pain intensity and Western Ontario and McMaster Universities Osteoarthritis Index subscales; tolerability was evaluated by adverse event and physician reporting."	2.71	Efficacy and safety of four doses of lumiracoxib versus diclofenac in patients with knee or hip primary osteoarthritis: a phase II, four-week, multicenter, randomized, double-blind, placebo-controlled trial. ( Beier, J; Geusens, P; Gitton, X; Hasler, P; Moore, A; Patel, SK; Poór, G; Schnitzer, TJ; Senftleber, I; Sloan, VS, 2004)
" A topical NSAID formulation may provide symptom relief with fewer adverse effects."	2.71	Efficacy and safety of a topical diclofenac solution (pennsaid) in the treatment of primary osteoarthritis of the knee: a randomized, double-blind, vehicle-controlled clinical trial. ( Roth, SH; Shainhouse, JZ, 2004)
"Diclofenac gel was effective and safe for relief of symptoms of OA of the knee over 3 weeks of dosing."	2.71	Efficacy of topical diclofenac diethylamine gel in osteoarthritis of the knee. ( Albrecht, HH; Elkik, F; Gold, MS; Liu, JM; Niethard, FU; Solomon, GS; Unkauf, M, 2005)
"Diclofenac-treated patients experienced statistically significant elevations in mean hepatic transaminases and serum creatinine and reductions in haemoglobin concentration when compared to placebo, events not observed with celecoxib."	2.70	Celecoxib versus diclofenac in the management of osteoarthritis of the knee. ( Borenstein, D; Geis, GS; Lefkowith, JB; McKenna, F; Wallemark, C; Wendt, H, 2001)
"Acetaminophen was associated with fewer adverse events."	2.70	A randomized, double-blind, crossover clinical trial of diclofenac plus misoprostol versus acetaminophen in patients with osteoarthritis of the hip or knee. ( Abramson, SB; Caldwell, JR; Callahan, LF; Cummins, P; Fort, J; Harrell, RA; Jordan, JM; Koch, GG; Kremer, JM; Lautzenheiser, RL; Lefkowith, J; Luta, G; Markenson, JA; Morant, S; Pincus, T; Schnitzer, TJ; Schwartz, T; Sokka, T; Wang, X; Weaver, A; Wilson, A; Wolfe, F, 2001)
" However, compliance is limited by the different dosing regimens of misoprostol and NSAID and GI symptoms associated with misoprostol at its recommended q."	2.69	Diclofenac/misoprostol compared with diclofenac in the treatment of osteoarthritis of the knee or hip: a randomized, placebo controlled trial. Arthrotec Osteoarthritis Study Group. ( Ball, JA; Bocanegra, TS; Fort, JG; Geis, GS; Sikes, DH; Tindall, EA; Wallemark, CB; Weaver, AL, 1998)
"diclofenac (n = 131) were assessed in a multicentre, randomised, double-blind study of a mixed population of patients with osteoarthritis of the knee and/or hip."	2.69	Oxaceprol is a well-tolerated therapy for osteoarthritis with efficacy equivalent to diclofenac. ( Dirschedl, H; Fürst, M; Gimbel, W; Herrmann, G; Hildebrandt, HD; Jungmichel, D; Klasser, M; Parnham, MJ; Rohde, H; Steeger, D; Venbrocks, R; Wirbitzky, J, 2000)
"Rofecoxib was well tolerated and provided efficacy that was clinically comparable, according to predefined statistical criteria, to that of 150 mg of diclofenac per day in this 1-year study."	2.69	Rofecoxib, a specific inhibitor of cyclooxygenase 2, with clinical efficacy comparable with that of diclofenac sodium: results of a one-year, randomized, clinical trial in patients with osteoarthritis of the knee and hip. Rofecoxib Phase III Protocol 035 ( Bolognese, J; Caldwell, JR; Cannon, GW; Daniels, B; Ehrich, E; Holt, P; McLean, B; Mukhopadhyay, S; Seidenberg, B, 2000)
"Celecoxib is a selective non-steroidal anti-inflammatory drug (NSAID)."	2.55	Celecoxib for osteoarthritis. ( Marin, A; Markotic, F; Puljak, L; Tugwell, P; Utrobicic, A; Vrdoljak, D, 2017)
"Diclofenac is a commonly used non-steroidal anti-inflammatory drug (NSAID) for symptom control in osteoarthritis (OA) of the knee and soft tissue injuries."	2.44	Topical diclofenac: clinical effectiveness and current uses in osteoarthritis of the knee and soft tissue injuries. ( Banning, M, 2008)
" The chronic use of diclofenac sodium can lead to adverse gastrointestinal problems."	2.43	The use of topical diclofenac for pain in osteoarthritis of the knee: a review. ( Banning, M, 2006)
"To investigate the effects of different nonsteroidal anti-inflammatory drugs combined with platelet-rich plasma on inflammatory factor levels in patients with osteoarthritis."	1.72	Effects of Different Nonsteroidal Anti-Inflammatory Drugs Combined with Platelet-Rich Plasma on Inflammatory Factor Levels in Patients with Osteoarthritis. ( Cheng, Y; Huang, Y; Jiang, W; Zhang, Y, 2022)
"NSAIDs used for the treatment of osteoarthritis (OA) have dose-related risks for gastrointestinal, cardiovascular and renal adverse events (AEs), particularly in elderly patients."	1.37	Safety and efficacy of topical diclofenac sodium gel for knee osteoarthritis in elderly and younger patients: pooled data from three randomized, double-blind, parallel-group, placebo-controlled, multicentre trials. ( Altman, RD; Baraf, HS; Barthel, HR; Gloth, FM; Gold, MS, 2011)
"The diclofenac therapy was discontinued."	1.32	[Pulmonary infiltrates with blood eosinophilia in a 62-year-old patient]. ( Geiger, D; Häussinger, K; Kohlhäufl, M; Morresi-Hauf, A; Raith, H; Weber, N, 2003)

Research

Studies (163)

Authors

Clinical Trials (33)

Trial Overview

Trial Outcomes

Change From Baseline in Patient's Global Assessment (PGA) of Osteoarthritis at Week 16

Timeframe	Studies, this research(%)	All Research%
pre-1990	0 (0.00)	18.7374
1990's	6 (3.68)	18.2507
2000's	63 (38.65)	29.6817
2010's	63 (38.65)	24.3611
2020's	31 (19.02)	2.80

Authors	Studies
Yakushin, S	1
Polyakova, S	1
Shvarts, Y	1
Kastanayan, A	1
Krechikova, D	1
Ershova, O	1
Nikulenkova, N	1
Vinogradova, I	1
Hyun, BJ	1
Cha, JE	1
Azadbakht, Z	1
Sajedi, F	1
Mahboobian, MM	1
Mohammadi, M	1
Ataei, S	1
Tomatsu, K	1
Yasuda, S	1
Fuady, A	1
Matsumoto, H	1
Jiang, W	1
Zhang, Y	2
Huang, Y	1
Cheng, Y	1
Wang, W	2
Yu, S	3
Long, Z	1
Liu, Y	1
Yan, Y	1
Sun, T	1
Liu, Z	1
Kubo, T	1
Kumai, T	1
Ikegami, H	1
Kano, K	4
Nishii, M	1
Seo, T	4
Chobpenthai, T	1
Arunwatthanangkul, P	1
Mahikul, W	1
Wen-Yue, W	1
Ying-Peng, X	1
Quan-Mao, D	1
Li-Min, X	1
De-Zhi, W	1
Yang, B	1
Li-Su, W	1
Yu-Bin, L	1
Zhi-Jun, N	1
Yan-Xu, M	1
Wu-Zhong, C	1
Li-Qun, B	1
Yang, L	2
Li-Kun, J	1
Li, T	1
Guo, M	1
Zhang, W	1
Zhang, D	2
Song, S	1
Bian, Z	1
Huang, Z	1
Tsurko, VV	1
Gromova, MA	1
Arai, T	1
Suzuki-Narita, M	1
Takeuchi, J	1
Tajiri, I	1
Inage, K	1
Kawarai, Y	1
Eguchi, Y	1
Shiga, Y	1
Hozumi, T	1
Kim, G	1
Tsuchiya, R	1
Otagiri, T	1
Mukaihata, T	1
Hishiya, T	1
Toshi, N	1
Okuyama, K	1
Tokeshi, S	1
Furuya, T	1
Maki, S	1
Matsuura, Y	1
Suzuki, T	1
Nakamura, J	1
Hagiwara, S	1
Ohtori, S	1
Orita, S	1
Ma, YT	1
Dong, YL	1
Wang, B	2
Xie, WP	1
Huang, QM	1
Zheng, YJ	1
Yao, Y	1
Wei, G	1
Ding, J	1
Cui, W	1
Yin, S	1
Chang, Y	1
Yan, X	1
Feng, X	1
Wu, N	1
Osnovina, IP	1
Alekseeva, NV	1
Ivanov, AV	1
Sekirin, AB	1
Askari, A	1
Ravansalar, SA	1
Naghizadeh, MM	1
Mosavat, SH	1
Khodadoost, M	1
Jazani, AM	1
Hashempur, MH	2
Huang, H	3
Pan, J	2
Yang, W	2
Chen, H	1
Liang, G	2
Zeng, L	2
Liu, J	2
Pan, B	1
Shep, D	2
Khanwelkar, C	2
Gade, P	2
Karad, S	2
Luo, M	1
Liang, H	1
Hou, S	1
Zhao, J	2
Shin, JY	1
Chang, MJ	1
Kim, MK	1
Kang, SB	1
Kim, KI	1
Park, HG	1
Lee, S	1
Kim, SH	1
Han, SB	1
Lee, HJ	1
Moon, YW	1
Yoo, JD	1
Nishida, Y	3
Nobuoka, Y	2
Bihlet, AR	1
Byrjalsen, I	1
Simon, LS	2
Carrara, D	1
Delpy, L	1
Derne, C	1
Ling, T	1
Li, JJ	1
Xu, RJ	1
Ge, WH	1
Hochberg, MC	3
Carrino, JA	1
Schnitzer, TJ	3
Guermazi, A	1
Walsh, DA	1
White, A	1
Nakajo, S	1
Fountaine, RJ	1
Hickman, A	1
Pixton, G	1
Viktrup, L	1
Brown, MT	2
West, CR	2
Verburg, KM	1
Wolff, DG	1
Christophersen, C	1
Brown, SM	1
Mulcahey, MK	1
Osato, T	1
Moman, RN	1
Hooten, WM	1
Zhou, Y	1
Tian, K	1
Jia, M	1
Tolu, S	1
Köse, MM	1
Korkmaz, MC	1
Üşen, A	1
Rezvani, A	1
Riddle, DL	1
van Herwaarden, N	1
van den Elsen, GAH	1
de Jong, ICA	1
Kramers, CK	1
Kloppenburg, M	1
van den Bemt, BJF	1
Zhou, JY	1
Luo, L	1
Zhu, LL	1
Yin, HY	1
Wu, Q	1
Peng, JX	1
Zhang, CS	1
Lv, P	1
Tang, Y	2
Yu, SG	1
Sivordova, LE	1
Zavodovsky, BV	1
Polyakova, JV	1
Akhverdyan, YR	1
Puljak, L	1
Marin, A	1
Vrdoljak, D	1
Markotic, F	1
Utrobicic, A	1
Tugwell, P	1
Wang, J	1
Adeyemi, WJ	1
Olayaki, LA	1
Gu, LJ	2
Zhang, B	1
Li, WH	1
Dong, FH	2
Amorndoljai, P	1
Taneepanichskul, S	1
Niempoog, S	3
Nimmannit, U	1
Wang, Q	1
Wu, J	1
Shi, X	1
Qi, Q	1
Zheng, H	1
Lang, S	1
Lertwanich, P	1
Lamsam, C	1
Ogawa, S	1
Natsume, T	1
Takamatsu, H	1
Yu, Z	1
Zhao, L	1
Yu, C	1
Bi, J	1
Yu, X	1
Rainsford, KD	1
Roberts, MS	1
Nencioni, A	1
Jones, C	1
Ter Heegde, F	1
Luiz, AP	1
Santana-Varela, S	1
Chessell, IP	1
Welsh, F	1
Wood, JN	1
Chenu, C	1
Jensen, MP	1
Molton, IR	1
Siriarchavatana, P	1
Kajsongkram, T	1
Pareek, A	3
Chandurkar, N	2
Qiu, XD	1
Zhao, Y	1
Qin, WK	1
Balanescu, AR	1
Feist, E	1
Wolfram, G	1
Davignon, I	1
Smith, MD	1
Pinsornsak, P	1
Gallelli, L	1
Galasso, O	1
Falcone, D	1
Southworth, S	1
Greco, M	1
Ventura, V	1
Romualdi, P	1
Corigliano, A	1
Terracciano, R	1
Savino, R	1
Gulletta, E	1
Gasparini, G	1
De Sarro, G	1
Stanos, SP	1
Galluzzi, KE	1
Uesugi, K	1
Kitano, N	1
Kikuchi, T	1
Sekiguchi, M	1
Konno, S	1
Gibofsky, A	3
Jaros, MJ	1
Young, CL	2
Bannuru, RR	1
Schmid, CH	1
Kent, DM	1
Vaysbrot, EE	1
Wong, JB	1
McAlindon, TE	1
Altman, RD	5
Strand, V	2
Markenson, JA	2
Hopkins, WE	1
Cryer, B	1
Kivitz, A	2
Nezzer, J	1
Imasogie, O	1
Zuo, C	1
Yin, G	1
Cen, XM	1
Xie, QB	1
Dehghan, M	1
Saggini, R	1
Di Stefano, A	1
Dodaj, I	1
Scarcello, L	1
Bellomo, RG	1
Voronina, NV	1
Slutskaya, NP	1
Markina, OI	1
Kovalskaya, LP	1
Agievich, TB	1
Gelmutdinov, DD	1
Bushina, AV	1
Verkleij, SP	2
Luijsterburg, PA	2
Willemsen, SP	1
Koes, BW	3
Bohnen, AM	2
Bierma-Zeinstra, SM	4
Orak, MM	1
Ak, D	1
Midi, A	1
Laçin, B	1
Purisa, S	1
Bulut, G	1
Wadsworth, LT	1
Kent, JD	1
Holt, RJ	1
Lauche, R	1
Gräf, N	1
Cramer, H	1
Al-Abtah, J	1
Dobos, G	1
Saha, FJ	1
Lee, T	1
Lu, N	1
Felson, DT	1
Choi, HK	1
Dalal, DS	1
Dubreuil, M	1
Jabbari, M	1
Razavi, SZ	1
Shahraki, HR	1
Kamalinejad, M	1
Emtiazy, M	1
Edwards, RR	1
Dolman, AJ	1
Martel, MO	1
Finan, PH	1
Lazaridou, A	1
Cornelius, M	1
Wasan, AD	1
Schattner, A	1
Kasemsuk, T	1
Saengpetch, N	1
Sibmooh, N	1
Unchern, S	1
Modak, MD	1
Barde, MP	1
Bergman, M	1
Singh, JA	1
Young, C	1
Alvarez-Soria, MA	2
Herrero-Beaumont, G	2
Moreno-Rubio, J	1
Calvo, E	2
Santillana, J	2
Egido, J	2
Largo, R	2
Ozgüney, I	1
Lüdtke, R	2
Banning, M	2
Deng, W	1
Medhi, B	1
Kishore, K	1
Singh, U	1
Seth, SD	1
Altman, R	1
Barkin, RL	1
Grierson, LM	1
Naseer, Z	1
Bookman, AAM	1
Shainhouse, ZJ	1
Elron-Gross, I	1
Glucksam, Y	1
Margalit, R	1
Maĭko, OIu	1
Bagirova, GG	1
Schuelert, N	1
McDougall, JJ	1
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Haselwood, D	1
Longley, S	1
Gold, MS	6
Moen, MD	1
Tao, QW	1
Xu, Y	1
Jin, DE	1
Yan, XP	1
Baraf, HS	3
Clark, MB	1
Zhu, Y	1
Chen, RL	1
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Ji, L	1
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Sirsikar, AD	1
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Trial	Phase	Enrollment	Study Type	Start Date	Status
Electroacupuncture vs Topical Diclofenac Sodium Gel for Patients With Hand Osteoarthritis: Study Protocol for a Randomized Controlled Trial[NCT04402047]		108 participants (Anticipated)	Interventional	2020-09-01	Recruiting
A PHASE 3 RANDOMIZED, DOUBLE-BLIND, ACTIVE-CONTROLLED, MULTICENTER STUDY OF THE LONG-TERM SAFETY AND EFFICACY OF SUBCUTANEOUS ADMINISTRATION OF TANEZUMAB IN SUBJECTS WITH OSTEOARTHRITIS OF THE HIP OR KNEE[NCT02528188]	Phase 3	3,021 participants (Actual)	Interventional	2015-07-21	Completed
The Effectiveness of Moxibustion Treatment for Osteoarthritis of the Knee : a Double-blinded, Double-dummy, Randomized Controlled Trial[NCT02769572]	Phase 3	144 participants (Actual)	Interventional	2016-05-31	Completed
EN20-01: A 24 Week Study to Evaluate the Safety and Efficacy of CNTX-6970 in Subjects With Moderate to Severe Knee Osteoarthritis Pain.[NCT05025787]	Phase 2	77 participants (Anticipated)	Interventional	2021-10-25	Recruiting
A PHASE 3, RANDOMIZED, DOUBLE BLIND, CONTROLLED, MULTI CENTER STUDY OF THE ANALGESIC EFFICACY AND SAFETY OF TANEZUMAB ADDED ON TO DICLOFENAC SR IN PATIENTS WITH OSTEOARTHRITIS OF THE KNEE OR HIP[NCT00864097]	Phase 3	607 participants (Actual)	Interventional	2009-08-11	Terminated (stopped due to See termination reason in detailed description.)
Effect of Combination of Curcuminoid Standardized Turmeric Extract With Acupressure on Inflammatory Markers, Endorphins and Quality of Life in Elderly People With Osteoarthritis Genu[NCT06105840]	Phase 1/Phase 2	70 participants (Anticipated)	Interventional	2023-08-27	Enrolling by invitation
EFFECTS OF NSAIDs ON CLINICAL OUTCOMES, SYNOVIAL FLUID CYTOKINE CONCENTRATION AND SIGNAL TRANSDUCTION PATHWAYS IN KNEE OSTEOARTHRITIS[NCT01860833]	Phase 4	90 participants (Actual)	Interventional	2010-04-30	Completed
Trial Evaluating multimOdal toPical Cream In CompArison to pLacebo (TOPICAL)[NCT03199417]	Phase 2/Phase 3	50 participants (Actual)	Interventional	2017-05-01	Terminated (stopped due to Terminated prematurely due to feasibility issues with rate of recruitment)
A Phase 3, Multicenter, Randomized, Double-Blind, Placebo-Controlled, Fixed-Dose, Parallel-Group, Efficacy and Safety Study of Diclofenac [Test] Capsules in Subjects With Osteoarthritis of the Knee or Hip[NCT01461369]	Phase 3	305 participants (Actual)	Interventional	2011-10-31	Completed
Pilot, Open Non-controled Trial to Assess the Feasibility of Implementing Objective Parameters as Primary Endpoints in a Clinical Trial With Patients Affected by Knee Osteoarthritis[NCT03421054]		8 participants (Actual)	Interventional	2018-03-19	Completed
Double Blind, Placebo Controlled Trial to Evaluate the Effects of a Nutraceutical Containing High-Molecular-Weight Hyaluronic Acid (HA) and Acetyl-11-Keto-Beta-Boswellic Acid (AKBA) in Patients Affected by Knee Osteoarthritis[NCT03612986]		72 participants (Actual)	Interventional	2018-08-22	Completed
A Multicenter, Open-Label, Safety Study of Diclofenac [Test] Capsules in Subjects With Osteoarthritis of the Knee or Hip[NCT01510912]	Phase 3	602 participants (Actual)	Interventional	2012-01-31	Completed
A Phase 2, Randomized, Double-Blind, Vehicle-Controlled, Parallel Group Clinical Study to Evaluate the Safety and Efficacy of PENNSAID Gel in the Symptomatic Treatment of Osteoarthritis of the Knee[NCT01119898]	Phase 2	260 participants (Actual)	Interventional	2010-08-02	Completed
Randomised Controlled Trial on the Efficacy of Cabbage Leaf Wraps in Symptomatic Primary Osteoarthritis of the Knee[NCT02027792]		81 participants (Actual)	Interventional	2014-01-31	Completed
Investigating Brain Abnormalities in People With Knee Osteoarthritis Using MRI: a Nociplastic Pain Mechanism Based Assessment[NCT05986513]		66 participants (Anticipated)	Interventional	2023-09-01	Not yet recruiting
The Efficacy of Diclofenac Gel for Breakthrough Pain and the Neuropathic Components of Pain in Knee Osteoarthritis[NCT01383954]	Phase 4	52 participants (Actual)	Interventional	2011-06-30	Completed
The Effect of St. John's Wort Oil on Pain Intensity and Physical Functions in People With Knee Osteoarthritis: a Qualitative and Randomized Placebo-controlled Trial[NCT05663996]		60 participants (Actual)	Interventional	2017-12-25	Completed
Efficacy of PENNSAID® for Pain Management in the Emergency Department[NCT01350622]		0 participants (Actual)	Interventional	2011-12-31	Withdrawn (stopped due to Study never initiated)
Efficacy and Safety of Diclofenac Sodium Gel in Knee Osteoarthritis[NCT00171678]	Phase 3	480 participants	Interventional	2004-10-31	Completed
Efficacy and Safety of Diclofenac Sodium Gel in Knee Osteoarthritis[NCT00171626]	Phase 3	480 participants	Interventional	2004-08-31	Completed
A 12-Week, Randomized, Double-Blind, Multi-Center, Vehicle-Controlled, Parallel Group Study to Assess the Efficacy and Safety of the Diclofenac Sodium Gel 1% for the Relief of Signs and Symptoms in Patients With Osteoarthritis of the Knee.[NCT00426621]	Phase 3	420 participants (Actual)	Interventional	2006-11-30	Completed
Safety of Diclofenac Sodium Gel in Knee Osteoarthritis[NCT00171691]	Phase 3	450 participants	Interventional	2004-10-31	Completed
A Placebo-Controlled, Parallel-Group, Double-Blind Study to Assess Safety and to Define the Clinically Effective Dose Range of MK0663 in Patients With Osteoarthritis of the Knee, Followed by a Double-Blind, Active-Comparator-Controlled Extension.[NCT00242489]	Phase 2	1,167 participants (Actual)	Interventional	1998-06-30	Completed
Aminotransferase Trends During Prolonged Therapeutic Acetaminophen Dosing[NCT00743093]	Phase 4	398 participants (Actual)	Interventional	2008-08-31	Completed
Single and Repeated Leech Therapy for the Treatment of Late Stage Knee Osteoarthritis. A Randomized, Placebo Controlled Comparative Trial[NCT00435773]	Phase 2	118 participants	Interventional	2004-02-29	Completed
A Randomized, Double-Blind Study to Evaluate the Safety and Efficacy of Etoricoxib 60 mg and Diclofenac Sodium 150 mg in Patient With Osteoarthritis of the Knee or Hip[NCT00542087]	Phase 3	516 participants (Actual)	Interventional	2002-03-22	Completed
Effect of a Menthol Gel (Biofreeze) on the Symptoms Associated With Knee Osteoarthritis: a Double-blind Randomized Control Trial.[NCT04351594]	Phase 2/Phase 3	100 participants (Anticipated)	Interventional	2020-11-01	Recruiting
Double-blind Randomized Clinical Study on Topical Diclofenac Efficacy in Symptomatic Relief of Temporomandibular Degenerative Joint Disease in Women.[NCT00471393]		28 participants (Actual)	Interventional	2006-05-31	Completed
Randomized, Double-Blind, Placebo-Controlled Trial, Parallel Design Used To Evaluate Pain, Endocrinologic Variations, Life Quality And Medication Use, After Electro-Acupuncture Treatment In Patients With Osteoarthritis Of The Knee[NCT02299713]		160 participants (Actual)	Interventional	2015-01-31	Completed
The Use of Cannabinoid Patch for Knee Osteoarthritis[NCT04412837]	Phase 2	0 participants (Actual)	Interventional	2022-10-31	Withdrawn (stopped due to Inadequate funding)
Comparison of Topical 1% Diclofenac and Topical 2.5% Hydrocortisone for TMJ Arthralgia[NCT05816226]	Phase 3	90 participants (Anticipated)	Interventional	2023-06-01	Recruiting
A One-week Multicenter, Multiple-dose, Randomized, Double-blind, Double-dummy, Parallel-group Comparison of the Analgesic Efficacy and Safety of Lumiracoxib (COX189), Celecoxib, and Placebo in the Treatment of Osteoarthritis of the Knee[NCT00267215]	Phase 3	330 participants	Interventional	2000-11-30	Completed
Hypoalgesic Effect of Median Nerve Neural Mobilization Versus Ibuprofen Pharmacologic Treatment in Patients With Cervicobrachial Pain[NCT02593721]	Phase 2/Phase 3	50 participants (Actual)	Interventional	2015-07-31	Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

"PGA of OA was assessed by asking a question from participants: Considering all the ways your OA in your knee or hip (index joint) affects you, how are you doing today? Participants responded on a scale ranging from 1-5, using Interactive Response Technology (IRT), where 1=very good (no symptom and no limitation of normal activities), 2= good (mild symptoms and no limitation of normal activities), 3= fair (moderate symptoms and limitation of some normal activities), 4= poor (severe symptoms and inability to carry out most normal activities), and 5= very poor (very severe symptoms and inability to carry out all normal activities). Higher scores indicated worsening of condition." (NCT02528188)
Timeframe: Baseline, Week 16

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale at Week 16

Intervention	units on a scale (Least Squares Mean)
Tanezumab 2.5 mg	-0.96
Tanezumab 5 mg	-0.97
NSAID	-0.94

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Physical Function Subscale at Week 16

Intervention	units on a scale (Least Squares Mean)
Tanezumab 2.5 mg	-3.22
Tanezumab 5 mg	-3.33
NSAID	-3.07

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. Physical function refers to participant's ability to move around and perform usual activities of daily living. The WOMAC physical function subscale is a 17-item questionnaire used to assess the degree of difficulty experienced due to OA in index joint (knee or hip) during past 48 hours. It was calculated as mean of the scores from 17 individual questions, which may not be a whole (integer) number, scored on a NRS. Scores for each question and WOMAC physical function subscale score on NRS ranged from 0 (no difficulty) to 10 (extreme difficulty), where higher scores indicated extreme difficulty/worse physical function. (NCT02528188)
Timeframe: Baseline, Week 16

Number of Days of Rescue Medication Used During Week 64

Intervention	units on a scale (Least Squares Mean)
Tanezumab 2.5 mg	-3.27
Tanezumab 5 mg	-3.39
NSAID	-3.08

In case of inadequate pain relief, after week 16, acetaminophen/paracetamol up to 3000 mg per day up to 7 days in a week could be taken as rescue medication and use was reported weekly via diary. Number of days the participants used the rescue medication during Week 64 were summarized. (NCT02528188)
Timeframe: Week 64

Number of Participants Who Took Rescue Medication During Week 64

Intervention	days (Mean)
Tanezumab 2.5 mg	2.0
Tanezumab 5 mg	2.3
NSAID	1.7

In case of inadequate pain relief, after Week 16, acetaminophen/paracetamol up to 3000 mg per day up to 7 days in a week could be taken as rescue medication and use was reported weekly via diary. Number of participants with any use of rescue medication during Week 64 were summarized. (NCT02528188)
Timeframe: Week 64

Number of Participants Who Withdrew Due to Lack of Efficacy

Intervention	Participants (Count of Participants)
Tanezumab 2.5 mg	251
Tanezumab 5 mg	268
NSAID	215

Number of participants who withdrew from treatment due to lack of efficacy have been reported here. (NCT02528188)
Timeframe: Baseline up to Week 56

Number of Participants With Laboratory Test Abnormalities With Regard to Abnormal Baseline

Intervention	Participants (Count of Participants)
Tanezumab 2.5 mg	60
Tanezumab 5 mg	63
NSAID	91

Primary Abnormality criteria: hemoglobin; hematocrit; RBC count < 0.8*LLN; Ery. mean corpuscular volume/ hemoglobin/ HGB concentration, erythrocytes distribution width <0.9*LLN, >1.1*ULN; platelets <0.5*LLN,>1.75*upper limit of normal (ULN); white blood cell count<0.6*LLN, >1.5*ULN; Lymphocytes, Lymphocytes/Leukocytes, Neutrophils, Neutrophils/Leukocytes <0.8*LLN, >1.2*ULN; Basophils, Eosinophils, Monocytes >1.2*ULN; total bilirubin>1.5*ULN; aspartate aminotransferase, alanine aminotransferase, gamma GT,LDH, alkaline phosphatase >3.0*ULN; total protein; albumin<0.8*LLN, >1.2*ULN; blood urea nitrogen, creatinine, Cholesterol, triglycerides >1.3*ULN; Urate >1.2*ULN; sodium <0.95*LLN,>1.05*ULN; potassium, chloride, calcium, magnesium, bicarbonate <0.9*LLN, >1.1*ULN; phosphate <0.8*LLN, >1.2*ULN; glucose <0.6*LLN, >1.5*ULN; Hemoglobin A1C >1.3*ULN; creatine kinase >2.0*ULN; specific gravity<1.003, >1.030; Urine erythrocytes,Leukocytes>=20; Hyaline Casts>=1. (NCT02528188)
Timeframe: Baseline up to Week 80

Number of Participants With Laboratory Test Abnormalities With Regard to Normal Baseline

Intervention	Participants (Count of Participants)
Tanezumab 2.5 mg	78
Tanezumab 5 mg	61
NSAID	84

Primary Abnormality criteria: HGB, hematocrit, RBC count <0.8* lower limit of normal(LLN); Ery. mean corpuscular volume/hemoglobin/ HGB concentration, RBCs distribution width <0.9*LLN, >1.1*upper limit of normal(ULN); platelets <0.5*LLN,>1.75*ULN; Leukocytes <0.6*LLN, >1.5*ULN; Lymphocytes, Neutrophils <0.8*LLN, >1.2*ULN; Basophils,Eosinophils,Monocytes>1.2*ULN; Prothrombin time/Intl. normalized ratio>1.1*ULN; total bilirubin>1.5*ULN; aspartate aminotransferase,alanine aminotransferase,gamma GT,LDH,alkaline phosphatase >3.0*ULN; total protein; albumin<0.8*LLN, >1.2*ULN; blood urea nitrogen,creatinine,Cholesterol,triglycerides >1.3*ULN; Urate>1.2*ULN; sodium<0.95*LLN,>1.05*ULN; potassium,chloride,calcium,magnesium,bicarbonate <0.9*LLN, >1.1*ULN; phosphate<0.8*LLN, >1.2*ULN; glucose<0.6*LLN, >1.5*ULN; HGB A1C >1.3*ULN; creatine kinase>2.0*ULN, specific gravity<1.003, >1.030; pH<4.5, >8;Urine erythrocytes,Leukocytes>=20. (NCT02528188)
Timeframe: Baseline up to Week 80

Observation Time-Adjusted Event Rate of Participants With Adjudicated Primary Composite Joint Safety Outcome

Intervention	Participants (Count of Participants)
Tanezumab 2.5 mg	109
Tanezumab 5 mg	102
NSAID	121

Observation time was defined as the start day of first SC study medication until either the (i) date of completion of or withdrawal from study, if a participant did not have the event, or (ii) date of the event (earliest event within each participant in the case of multiple events). Primary joint safety outcome included participants with adjudicated outcome of primary osteonecrosis, rapidly progressive OA type 1 or type 2, subchondral insufficiency fracture, or pathological fracture. Event rate was calculated as the number of events per 1000 participant-years at risk. (NCT02528188)
Timeframe: Baseline up to Week 80

Observation Time-Adjusted Event Rate of Participants With Adjudicated Secondary Composite Joint Safety Outcome

Intervention	events per 1000 participant-years (Number)
Tanezumab 2.5 mg	38.3
Tanezumab 5 mg	71.5
NSAID	14.8

Observation time was defined as the start day of first SC study medication until either the (i) date of completion of or withdrawal from study, if a participant did not have the event, or (ii) date of the event (earliest event within each participant in the case of multiple events). Secondary joint safety outcome included primary osteonecrosis, rapidly progressive OA (type-2), subchondral insufficiency fracture, or pathological fracture. Event rate was calculated as the number of events per 1000 participant-years at risk. (NCT02528188)
Timeframe: Baseline up to Week 80

Observation Time-Adjusted Event Rate of Participants With Total Joint Replacement or Adjudicated Primary Composite Joint Safety Outcome

Intervention	events per 1000 participant-years (Number)
Tanezumab 2.5 mg	9.7
Tanezumab 5 mg	21.8
NSAID	4.9

Observation time was defined as the start day of first SC study medication until either the (i) date of completion of or withdrawal from study, if a participant did not have the event, or (ii) date of the event (earliest event within each participant in the case of multiple events). Adjudicated primary composite joint safety outcomes included primary osteonecrosis, rapidly progressive OA type 1 or type 2, subchondral insufficiency fracture, or pathological fracture. Event rate was calculated as the number of events per 1000 participant-years at risk. (NCT02528188)
Timeframe: Baseline up to Week 80

Percentage of Participants With Adjudicated Primary Composite Joint Safety Outcome

Intervention	events per 1000 participant-years (Number)
Tanezumab 2.5 mg	84.9
Tanezumab 5 mg	132.5
NSAID	36.7

Any participant with incidence of an adjudicated outcome of primary osteonecrosis, rapidly progressive osteoarthritis (OA) type 1 or type 2, subchondral insufficiency fracture, or pathological fracture. Rapidly progressive OA type 1 events were those that the Adjudication Committee considered to have significant loss of joint space width (JSW) (greater than or equal to [>=] 2 millimeters [mm]) within approximately 1 year without gross structural failure. Rapidly progressive OA type 2 events were those considered to have abnormal loss/destruction of bone including limited or total collapse of at least one subchondral surface (e.g., medial femoral condyle) that is not normally present in conventional end-stage OA. (NCT02528188)
Timeframe: Baseline up to Week 80

Percentage of Participants With Adjudicated Secondary Composite Joint Safety Outcome

Intervention	percentage of participants (Number)
Tanezumab 2.5 mg	3.9
Tanezumab 5 mg	7.1
NSAID	1.5

Any participant with incidence of an adjudicated outcome of primary osteonecrosis, rapidly progressive OA type 2, subchondral insufficiency fracture, or pathological fracture. Rapidly progressive OA type 2 events were those considered to have abnormal loss/destruction of bone including limited or total collapse of at least one subchondral surface (e.g., medial femoral condyle) that is not normally present in conventional end-stage OA. (NCT02528188)
Timeframe: Baseline up to Week 80

Percentage of Participants With Total Joint Replacement or Adjudicated Primary Composite Joint Safety Outcome

Intervention	percentage of participants (Number)
Tanezumab 2.5 mg	1.0
Tanezumab 5 mg	2.2
NSAID	0.5

Percentage of participants with total joint replacement (hip, knee or shoulder) or adjudicated primary composite joint safety outcomes were reported. Adjudicated primary composite joint safety outcomes included primary osteonecrosis, rapidly progressive OA type 1 or type 2, subchondral insufficiency fracture, or pathological fracture. (NCT02528188)
Timeframe: Baseline up to Week 80

Time to Discontinuation Due to Lack of Efficacy

Intervention	percentage of participants (Number)
Tanezumab 2.5 mg	8.6
Tanezumab 5 mg	13.1
NSAID	3.7

Time to discontinuation due to lack of efficacy was defined as the time interval from the date of first study drug administration up to the date of discontinuation of participant from treatment due to lack of efficacy. (NCT02528188)
Timeframe: Baseline up to Week 56

Amount of Rescue Medication Used During Weeks 2, 4, 8 and 16

Intervention	days (Median)
Tanezumab 2.5 mg	NA
Tanezumab 5 mg	NA
NSAID	NA

In case of inadequate pain relief, acetaminophen/paracetamol up to 3000 mg per day up to 3 days in a week could be taken as rescue medication. The total dosage of acetaminophen in milligrams used during the specified week were summarized. (NCT02528188)
Timeframe: Weeks 2, 4, 8 and 16

Change From Baseline in Average Daily Minutes of Bouted (Sustained) Moderate to Vigorous Physical Activity at Weeks 16 and 56

Intervention	milligrams (Least Squares Mean)
	Week 2	Week 4	Week 8	Week 16
NSAID	3310.5	2814.1	2839.7	2320.0
Tanezumab 2.5 mg	2880.3	2107.8	1995.6	1696.4
Tanezumab 5 mg	2898.7	1946.5	1628.8	1581.6

"An average daily physical activity count was measured using actigraphy which was then sorted into three intensity thresholds: light (100 - <1,500 counts) moderate (1,500 - <6,500 counts), and vigorous (>=6,500 counts). Participants continuously wore the accelerometer (apart for water activities) in the morning until going to bed at night for 7 or 14 consecutive days while going about their usual daily activities. Participants maintained a log (electronic or written) to record when the accelerometer was put on in the morning and removed at night (or if removed for any other purpose).A bout of moderate to vigorous activity was defined as 10 or more consecutive minutes above the moderate physical activity level threshold, with allowance for interruptions of 1 or 2 minutes below the threshold." (NCT02528188)
Timeframe: Baseline, Weeks 16 and 56

Change From Baseline in Average Daily Minutes of Moderate to Vigorous Physical Activity at Weeks 16 and 56

Intervention	minutes (Median)
	Baseline	Change at Week 16	Change at Week 56
NSAID	0.0	0.0	0.0
Tanezumab 2.5 mg	0.0	0.0	0.0
Tanezumab 5 mg	0.0	0.0	-1.4

An average daily physical activity count was measured using actigraphy which was then sorted into three intensity thresholds: light (100 - less than {<1500} counts moderate (1,500 - <6500 counts), and vigorous (>=6500 counts). Participants continuously wore the accelerometer (apart for water activities) in the morning until going to bed at night for 7 or 14 consecutive days while going about their usual daily activities. Participants maintained a log (electronic or written) to record when the accelerometer was put on in the morning and removed at night (or if removed for any other purpose). (NCT02528188)
Timeframe: Baseline, Weeks 16 and 56

Change From Baseline in Average Daily Minutes of Physical Activity at Weeks 16 and 56

Intervention	minutes (Median)
	Baseline	Change at Week 16	Change at Week 56
NSAID	41.9	-0.1	7.4
Tanezumab 2.5 mg	41.2	0.7	-3.8
Tanezumab 5 mg	53.1	-1.6	2.7

Participant activity level was assessed using actigraphy. Participants continuously wore the accelerometer (apart for water activities) in the morning until going to bed at night for 7 or 14 consecutive days while going about their usual daily activities. Participants maintained a log (electronic or written) to record when the accelerometer was put on in the morning and removed at night (or if removed for any other purpose). (NCT02528188)
Timeframe: Baseline, Weeks 16 and 56

Change From Baseline in Average Daily Physical Activity Counts at Weeks 16 and 56

Intervention	minutes (Median)
	Baseline	Change at Week 16	Change at Week 56
NSAID	99.2	-4.2	3.9
Tanezumab 2.5 mg	97.0	3.9	-8.9
Tanezumab 5 mg	107.1	2.9	-10.1

An average daily physical activity count was measured using actigraphy. Participants continuously wore the accelerometer (apart for water activities) in the morning until going to bed at night for 7 or 14 consecutive days while going about their usual daily activities. Participants maintained a log (electronic or written) to record when the accelerometer was put on in the morning and removed at night (or if removed for any other purpose). (NCT02528188)
Timeframe: Baseline, Weeks 16 and 56

Change From Baseline in Average Daily Step Count at Weeks 16 and 56

Intervention	physical activity counts (Median)
	Baseline	Change at Week 16	Change at Week 56
NSAID	74414	1202.9	4414.3
Tanezumab 2.5 mg	75244	-470.0	-14552
Tanezumab 5 mg	95911	-2261	-8313

Average daily step count was measured using actigraphy. Participants continuously wore the accelerometer (apart for water activities) in the morning until going to bed at night for 7 or 14 consecutive days while going about their usual daily activities. Participants maintained a log (electronic or written) to record when the accelerometer was put on in the morning and removed at night (or if removed for any other purpose). (NCT02528188)
Timeframe: Baseline, Weeks 16 and 56

Change From Baseline in Average Pain Score in the Index Joint at Week 64

Intervention	step count (Median)
	Baseline	Change at Week 16	Change at Week 56
NSAID	4779.0	-705.7	242.6
Tanezumab 2.5 mg	4851.0	350.9	-1938
Tanezumab 5 mg	5834.8	87.8	-543.2

Participants assessed their average pain in the index hip/knee in the past 24 hours using NRS, with a scale ranging from 0 (no pain) to 10 (worst possible pain). Higher scores indicated higher pain. Data represents averages of the values reported during the 4-week interval up to and including Week 64. Change from baseline was calculated using the difference between each post-baseline weekly mean and the baseline mean score. (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Average Pain Score in the Index Joint at Weeks 1, 2, 3, 4, 6, 8, 10, 12, 16, 20, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	6.76	-3.24
Tanezumab 2.5 mg	6.76	-3.01
Tanezumab 5 mg	6.77	-2.81

Participants assessed their average pain in the index hip/knee in the past 24 hours using NRS, with a scale ranging from 0 (no pain) to 10 (worst possible pain). Higher scores indicated higher pain. Data for Weeks 20 through 56 represents averages of the values reported during the 4-week interval up to and including the given week. Change from baseline was calculated using the difference between each post-baseline weekly mean and the baseline mean score. (NCT02528188)
Timeframe: Baseline, Weeks 1, 2, 3, 4, 6, 8, 10, 12, 16, 20, 24, 32, 40, 48 and 56

Change From Baseline in Blood Pressure (BP) at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Intervention	units on a scale (Least Squares Mean)
	Change at Week 1	Change at Week 2	Change at Week 3	Change at Week 4	Change at Week 6	Change at Week 8	Change at Week 10	Change at Week 12	Change at Week 16	Change at Week 20	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-0.56	-0.91	-1.23	-1.32	-1.49	-1.59	-1.98	-2.10	-2.17	-2.27	-2.11	-2.06	-2.07	-2.03	-2.04
Tanezumab 2.5 mg	-0.47	-1.02	-1.40	-1.62	-1.85	-1.83	-2.35	-2.48	-2.41	-2.56	-2.35	-2.27	-2.25	-2.20	-2.17
Tanezumab 5 mg	-0.56	-0.97	-1.30	-1.65	-1.97	-2.04	-2.46	-2.55	-2.52	-2.60	-2.41	-2.26	-2.20	-2.10	-2.03

Measurement of BP included sitting systolic blood pressure (SBP) and diastolic blood pressure (DBP). (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Change From Baseline in Electrocardiogram (ECG) Parameters at Weeks 56 and 80

Intervention	millimeters of mercury (mmHg) (Mean)
	SBP: Baseline	SBP: Change at Week 2	SBP: Change at Week 4	SBP: Change at Week 8	SBP: Change at Week 16	SBP: Change at Week 24	SBP: Change at Week 32	SBP: Change at Week 40	SBP: Change at Week 48	SBP: Change at Week 56	SBP: Change at Week 64	SBP: Change at Week 80	DBP: Baseline	DBP: Change at Week 2	DBP: Change at Week 4	DBP: Change at Week 8	DBP: Change at Week 16	DBP: Change at Week 24	DBP: Change at Week 32	DBP: Change at Week 40	DBP: Change at Week 48	DBP: Change at Week 56	DBP: Change at Week 64	DBP: Change at Week 80
NSAID	128.8	-1.2	-1.8	-1.8	-1.3	-1.7	-1.7	-2.3	-2.2	-2.2	-2.8	-2.3	79.3	-1.1	-1.4	-1.1	-1.1	-1.4	-1.2	-1.1	-1.5	-1.2	-1.7	-1.2
Tanezumab 2.5 mg	128.9	-2.7	-4.0	-2.9	-3.0	-3.0	-2.8	-2.5	-2.7	-3.1	-2.1	-1.0	79.3	-1.3	-2.2	-1.1	-1.3	-1.3	-1.3	-1.2	-0.9	-1.8	-0.8	-0.6
Tanezumab 5 mg	129.3	-4.2	-4.9	-3.8	-3.7	-3.1	-3.3	-3.8	-3.0	-3.4	-2.1	-1.3	79.1	-2.1	-2.5	-1.7	-1.8	-1.7	-1.4	-2.0	-1.8	-1.9	-0.8	-0.6

A 12-lead ECG was recorded after participants had rested for at least 5 minutes in the supine position in a quiet environment. All standard intervals (PR, QRS, QT, QTcF, QTcB, RR intervals) were collected. ECG abnormalities included: 1) QT interval, QT interval corrected using Bazett's formula (QTcB) and QT interval corrected using Fridericia's formula (QTcF): increase from baseline greater than (>) 30 millisecond (ms) or 60 ms; absolute value > 450 ms, >480 ms and > 500 ms; 2) heart rate (HR) : absolute value <=50 bpm and decrease from baseline >=20 bpm; absolute value >=120 beats per minute (bpm) and increase from baseline >=20 bpm; 3) PR interval: absolute value >=220 ms and increase from baseline >=20 ms; 4) QRS interval: absolute value >= 120 ms. (NCT02528188)
Timeframe: Baseline, Weeks 56 and 80

Change From Baseline in Heart Rate (as Assessed by ECG) at Weeks 56 and 80

Intervention	milliseconds (Mean)
	RR Interval: Baseline	RR Interval:Change at Week 56	RR Interval:Change at Week 80	PR Interval: Baseline	PR Interval:Change at Week 56	PR Interval:Change at Week 80	QRS Interval: Baseline	QRS Interval:Change at Week 56	QRS Interval:Change at Week 80	QT Interval: Baseline	QT Interval:Change at Week 56	QT Interval:Change at Week 80	QTCB Interval: Baseline	QTCB Interval:Change at Week 56	QTCB Interval:Change at Week 80	QTCF Interval: Baseline	QTCF Interval:Change at Week 56	QTCF Interval:Change at Week 80
NSAID	936.1	-14.9	-34.3	163.9	1.7	0.6	94.3	-0.4	-0.1	404.3	-2.9	-6.0	419.7	0.2	1.7	414.3	-0.8	-1.0
Tanezumab 2.5 mg	940.5	-26.3	-33.6	165.0	1.7	0.3	94.9	0.2	-0.2	405.0	-3.5	-6.2	419.3	2.3	1.5	414.2	0.3	-1.2
Tanezumab 5 mg	940.1	-22.6	-32.4	165.9	0.6	-0.8	94.6	0.4	1.0	403.8	-4.5	-6.8	418.5	0.5	0.2	413.3	-1.2	-2.1

Heart rate was measured at sitting position. (NCT02528188)
Timeframe: Baseline, Weeks 56 and 80

Change From Baseline in Heart Rate at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Intervention	beats per minute (Mean)
	Baseline	Change at Week 56	Change at Week 80
NSAID	65.6	1.0	2.5
Tanezumab 2.5 mg	65.2	2.0	2.7
Tanezumab 5 mg	65.4	1.7	2.3

Heart rate (pulse rate) was measured at sitting position. (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Change From Baseline in Joint Space Width of the Index Hip (Kellgren-Lawrence Grade 2 or 3) at Weeks 56 and 80

Intervention	beats per minute (Mean)
	Baseline	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 16	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56	Change at Week 64	Change at Week 80
NSAID	70.6	1.1	1.2	0.1	0.8	0.8	1.7	1.4	1.3	-0.0	0.5	0.9
Tanezumab 2.5 mg	70.8	1.8	1.6	0.7	0.5	0.4	1.2	1.2	0.6	0.2	1.5	0.9
Tanezumab 5 mg	70.5	2.0	2.0	0.8	0.5	0.7	1.6	1.6	1.0	0.1	1.5	0.6

Change from baseline in JSW was defined as narrowing in JSW compared to baseline in participants with Kellgren-Lawrence grade 2 or 3 over the course of the study. It was measured radiographically in the index hip in participants with OA. Kellgren-Lawrence grade system was a method of classifying the severity of hip OA using five grades i.e. 0 (no radiographic features of OA), 1 (doubtful JSN and possible osteophytic lipping), 2 (definite osteophytes and possible JSN on anteroposterior weight-bearing radiograph), 3 (multiple osteophytes, definite JSN, sclerosis, possible bony deformity), 4 (large osteophytes, marked JSN, severe sclerosis and definite bony deformity). Higher grade indicating worse hip function. (NCT02528188)
Timeframe: Baseline, Weeks 56 and 80

Change From Baseline in Medial or Lateral Joint Space Width of the Index Knee (Kellgren-Lawrence Grade 2 or 3) at Weeks 56 and 80

Intervention	millimeter (Least Squares Mean)
	Change at Week 56	Change at Week 80
NSAID	-0.21	-0.28
Tanezumab 2.5 mg	-0.35	-0.46
Tanezumab 5 mg	-0.40	-0.35

Change from baseline in JSW was defined as change in JSW compared to baseline in participants with Kellgren-Lawrence grade 2 or 3 over the course of the study. It was measured radiographically in the medial and lateral tibiofemoral of knee in participants with OA. Kellgren-Lawrence grade system was a method of classifying the severity of knee OA using five grades i.e. 0 [no radiographic features of OA], 1 [doubtful joint space narrowing (JSN) and possible osteophytic lipping], 2 [definite osteophytes and possible JSN on anteroposterior weight-bearing radiograph], 3 [multiple osteophytes, definite JSN, sclerosis, possible bony deformity], 4 [large osteophytes, marked JSN, severe sclerosis and definite bony deformity]. Higher grade indicating worse knee function. The number of participants with progression of OA in the index knee are summarized separately by the compartment of OA at baseline (medial or lateral). (NCT02528188)
Timeframe: Baseline, Weeks 56 and 80

Change From Baseline in Neuropathy Impairment Score (NIS) at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Intervention	millimeter (Least Squares Mean)
	Change in Medial JSW at Week 56	Change in Medial JSW at Week 80	Change in Lateral JSW at Week 56	Change in Lateral JSW at Week 80
NSAID	-0.19	-0.25	-0.27	-0.37
Tanezumab 2.5 mg	-0.25	-0.33	-0.26	-0.46
Tanezumab 5 mg	-0.34	-0.37	-0.32	-0.32

NIS is a standardized instrument used to evaluate participant for signs of peripheral neuropathy. NIS is the sum of scores of 37 items, from both the left and right side, where 24 items scored from 0 (normal) to 4 (paralysis), higher score indicated higher abnormality/impairment and 13 items scored from 0 (normal), 1 (decreased) and 2 (absent), higher score indicated higher impairment. NIS possible overall score ranged from 0 (no impairment) to 244 (maximum impairment), higher scores indicated increased impairment. (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Change From Baseline in Patient's Global Assessment (PGA) of Osteoarthritis at Week 64

Intervention	units on a scale (Mean)
	Baseline	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 16	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56	Change at Week 64	Change at Week 80
NSAID	1.87	-0.15	-0.19	-0.36	-0.47	-0.49	-0.53	-0.53	-0.55	-0.58	-0.57	-0.62
Tanezumab 2.5 mg	1.85	-0.22	-0.16	-0.27	-0.27	-0.32	-0.37	-0.35	-0.37	-0.35	-0.32	-0.35
Tanezumab 5 mg	1.70	-0.13	-0.17	-0.22	-0.31	-0.35	-0.40	-0.43	-0.49	-0.52	-0.47	-0.47

"PGA of OA was assessed by asking a question from participants: Considering all the ways your OA in your knee or hip (index joint) affects you, how are you doing today? Participants responded on a scale ranging from 1-5, using IRT, where 1=very good (no symptom and no limitation of normal activities), 2= good (mild symptoms and no limitation of normal activities), 3= fair (moderate symptoms and limitation of some normal activities), 4= poor (severe symptoms and inability to carry out most normal activities), and 5= very poor (very severe symptoms and inability to carry out all normal activities). Higher scores indicated worsening of condition." (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Patient's Global Assessment (PGA) of Osteoarthritis at Weeks 2, 4, 8, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	3.44	-0.95
Tanezumab 2.5 mg	3.49	-0.79
Tanezumab 5 mg	3.46	-0.64

"PGA of OA was assessed by asking a question from participants: Considering all the ways your OA in your knee or hip (index joint) affects you, how are you doing today? Participants responded on a scale ranging from 1-5, using IRT, where 1=very good (no symptom and no limitation of normal activities), 2= good (mild symptoms and no limitation of normal activities), 3= fair (moderate symptoms and limitation of some normal activities), 4= poor (severe symptoms and inability to carry out most normal activities), and 5= very poor (very severe symptoms and inability to carry out all normal activities). Higher scores indicated worsening of condition." (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 24, 32, 40, 48 and 56

Change From Baseline in Survey of Autonomic Symptom (SAS) Scores at Weeks 24, 56 and 80

Intervention	units on a scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-0.63	-0.69	-0.76	-0.74	-0.72	-0.69	-0.67	-0.66
Tanezumab 2.5 mg	-0.67	-0.81	-0.77	-0.74	-0.72	-0.70	-0.70	-0.65
Tanezumab 5 mg	-0.67	-0.84	-0.85	-0.79	-0.71	-0.69	-0.66	-0.60

The SAS is a 12 item (11 for females) questionnaire, from which the total number of symptoms (0-12 for males and 0-11 for females) is calculated. Each positive symptom is rated from 1 (not at all) to 5 (a lot). The total impact score was the sum of all symptom rating scores, with 0 assigned where the participant did not have the particular symptom. The range for the total impact score is 0-60 for males and 0-55 for females, higher scores indicating higher impact. (NCT02528188)
Timeframe: Baseline, Weeks 24, 56 and 80

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Average Score at Week 64

Intervention	units on a scale (Mean)
	Number of symptoms reported: Baseline	Number of symptoms reported: Change at Week 24	Number of symptoms reported: Change at Week 56	Number of symptoms reported: Change at Week 80	Total symptom impact score: Baseline	Total symptom impact score: Change at Week 24	Total symptom impact score: Change at Week 56	Total symptom impact score: Change at Week 80
NSAID	0.49	0.11	0.22	0.74	1.13	0.33	0.82	0.89
Tanezumab 2.5 mg	0.47	0.21	0.28	0.89	1.10	0.66	0.97	1.33
Tanezumab 5 mg	0.53	0.18	0.33	0.94	1.23	0.52	1.21	1.31

WOMAC: self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA of index joint (knee or hip). WOMAC pain subscale assess amount of pain experienced (score: 0 [no pain] to 10 [extreme pain], higher score = more pain), WOMAC physical function subscale assess degree of difficulty experienced (score: 0 [no difficulty] to 10 [extreme difficulty], higher score = worse physical function) and WOMAC stiffness subscale assess the amount of stiffness experienced (score: 0 [no stiffness] to 10 [extreme stiffness], higher score = higher stiffness). WOMAC average score was the mean of WOMAC pain, physical function and stiffness subscale scores and ranges from 0 to 10, where higher scores indicated worse response. (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Average Score at Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	7.01	-3.77
Tanezumab 2.5 mg	7.09	-3.40
Tanezumab 5 mg	7.10	-3.09

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Item: Pain When Going Up or Down Stairs at Week 64

Intervention	units on a scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 16	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-1.52	-1.95	-2.23	-3.07	-2.64	-2.54	-2.49	-2.44	-2.40
Tanezumab 2.5 mg	-1.73	-2.28	-2.44	-3.26	-2.74	-2.65	-2.57	-2.56	-2.45
Tanezumab 5 mg	-1.61	-2.34	-2.71	-3.41	-2.88	-2.69	-2.58	-2.48	-2.38

"WOMAC: self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA in index joint (knee or hip). Participants answered a question: How much pain have you had when going up or down the stairs? Participants responded about the amount of pain they experienced when going up or down stairs by using a NRS of 0 (no pain) to 10 (extreme pain), where higher scores indicated higher pain." (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Item: Pain When Going Up or Down Stairs at Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	7.83	-3.70
Tanezumab 2.5 mg	7.89	-3.28
Tanezumab 5 mg	7.88	-2.97

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Item: Pain When Walking on a Flat Surface at Week 64

Intervention	units on a scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 16	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-1.66	-2.08	-2.40	-3.18	-2.83	-2.74	-2.70	-2.67	-2.55
Tanezumab 2.5 mg	-1.81	-2.34	-2.48	-3.34	-2.89	-2.76	-2.69	-2.70	-2.55
Tanezumab 5 mg	-1.66	-2.43	-2.81	-3.50	-3.03	-2.84	-2.74	-2.63	-2.47

"WOMAC: self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA in index joint (knee or hip). Participants answered a question: How much pain have you had when walking on a flat surface?. Participants responded about the amount of pain they experienced when walking on a flat surface by using a NRS of 0 (no pain) to 10 (extreme pain), where higher scores indicated higher pain." (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Item: Pain When Walking on a Flat Surface at Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	6.86	-3.67
Tanezumab 2.5 mg	6.86	-3.20
Tanezumab 5 mg	6.90	-2.69

"WOMAC: self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA in index joint (knee or hip). Participants answered a question: How much pain have you had when walking on a flat surface?. Participants responded about the amount of pain they experienced when walking on a flat surface by using a NRS of 0 (no pain) to 10 (extreme pain), where higher scores indicated higher pain." (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Stiffness Subscale at Week 64

Intervention	units on a scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 16	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-1.46	-1.91	-2.22	-2.95	-2.60	-2.52	-2.48	-2.42	-2.39
Tanezumab 2.5 mg	-1.54	-2.14	-2.26	-3.01	-2.64	-2.54	-2.48	-2.45	-2.37
Tanezumab 5 mg	-1.39	-2.15	-2.47	-3.13	-2.76	-2.54	-2.42	-2.34	-2.21

WOMAC: self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. Stiffness was defined as a sensation of decreased ease of movement in the index joint (knee or hip). The WOMAC stiffness subscale is a 2-item questionnaire used to assess the amount of stiffness experienced due to OA in the index joint (knee or hip) during the past 48 hours. It was calculated as the mean of scores from 2 individual questions scored on NRS. Scores for each question and WOMAC stiffness subscale score on NRS ranged from 0 (no stiffness) to 10 (extreme stiffness), where higher scores indicated higher stiffness. (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Stiffness Subscale at Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	7.09	-3.66
Tanezumab 2.5 mg	7.15	-3.31
Tanezumab 5 mg	7.20	-3.04

WOMAC: self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. Stiffness was defined as a sensation of decreased ease of movement in the index joint (knee or hip). The WOMAC stiffness subscale is a 2-item questionnaire used to assess the amount of stiffness experienced due to OA in the index joint (knee or hip) during the past 48 hours. It was calculated as the mean of scores from 2 individual questions scored on NRS. Scores for each question and WOMAC stiffness subscale score on NRS ranged from 0 (no stiffness) to 10 (extreme stiffness), where higher scores indicated higher stiffness. (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Change From Baseline in WOMAC Pain Subscale at Week 64

Intervention	units on a scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 16	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-1.48	-1.95	-2.16	-3.10	-2.63	-2.52	-2.46	-2.44	-2.42
Tanezumab 2.5 mg	-1.79	-2.32	-2.46	-3.32	-2.77	-2.68	-2.58	-2.60	-2.46
Tanezumab 5 mg	-1.70	-2.43	-2.79	-3.54	-2.95	-2.74	-2.64	-2.54	-2.46

Change From Baseline in WOMAC Pain Subscale at Weeks 2, 4, 8, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	6.96	-3.85
Tanezumab 2.5 mg	7.01	-3.47
Tanezumab 5 mg	7.02	-3.12

Change From Baseline in WOMAC Physical Function Subscale at Week 64

Intervention	units on scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-1.55	-1.98	-2.27	-2.67	-2.57	-2.52	-2.47	-2.42
Tanezumab 2.5 mg	-1.65	-2.25	-2.41	-2.73	-2.64	-2.56	-2.54	-2.44
Tanezumab 5 mg	-1.49	-2.29	-2.65	-2.86	-2.68	-2.57	-2.48	-2.37

Change From Baseline in WOMAC Physical Function Subscale at Weeks 2, 4, 8, 24, 32, 40, 48 and 56

Intervention	units on a scale (Mean)
	Baseline	Change at Week 64
NSAID	6.99	-3.81
Tanezumab 2.5 mg	7.09	-3.42
Tanezumab 5 mg	7.08	-3.12

Change From Baseline in Work Productivity and Activity Impairment Questionnaire for Osteoarthritis (WPAI:OA) Scores at Week 64

Intervention	units on a scale (Least Squares Mean)
	Change at Week 2	Change at Week 4	Change at Week 8	Change at Week 24	Change at Week 32	Change at Week 40	Change at Week 48	Change at Week 56
NSAID	-1.55	-1.96	-2.27	-2.66	-2.55	-2.50	-2.45	-2.41
Tanezumab 2.5 mg	-1.76	-2.29	-2.46	-2.78	-2.66	-2.56	-2.56	-2.45
Tanezumab 5 mg	-1.64	-2.31	-2.69	-2.88	-2.67	-2.57	-2.49	-2.36

WPAI is 6-question participant rated questionnaire to determine the impact of OA on absenteeism, presenteeism, work productivity, and daily activity impairment for a period of 7 days prior to a visit. It yields 4 sub-scores: work time missed (absenteeism), impairment while working (presenteeism), overall work impairment (work productivity) and activity impairment (daily activity impairment). These sub-scores are expressed as an impairment percentage (range from 0 to 100), with higher numbers indicating greater impairment and less productivity. (NCT02528188)
Timeframe: Baseline, Week 64

Change From Baseline in Work Productivity and Activity Impairment Questionnaire for Osteoarthritis (WPAI:OA) Scores at Weeks 16, 24 and 56

Intervention	units on a scale (Mean)
	Baseline: Percent Work Time Missed	Baseline: Percent Impairment While Working	Baseline: Percent Overall Work Impairment	Baseline: Percent Activity Impairment	Change at Week 64: Percent Work Time Missed	Change at Week 64:Percent Impairment While Working	Change at Week 64: Percent Overall Work Impairment	Change at Week 64: Percent Activity Impairment
NSAID	5.2	59.3	60.6	66.7	-2.1	-26.5	-27.0	-32.1
Tanezumab 2.5 mg	6.1	60.5	62.1	68.3	-1.8	-24.2	-24.5	-28.7
Tanezumab 5 mg	6.0	58.3	60.0	67.9	4.1	-20.7	-19.2	-24.1

European Quality of Life-5 Dimensions-5 Levels (EQ-5D-5L) Overall Health Utility Score/Index Value

EQ-5D-5L: standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional VAS. EQ-5D health state profile comprises of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1=no problems, 2=slight problems, 3=moderate problems, 4=severe problems, and 5=extreme problems. Responses from the five domains were used to calculate a single utility index (the Overall health utility score) where values are less than or equal to (<=) 1. The Overall health utility score for a participant with no problems in all 5 items is 1 for all countries (except for Zimbabwe where it is 0.9), and is reduced where a participant reports greater levels of problems across the five dimensions. (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 24, 40, 56 and 64

Health Care Resource Utilization (HCRU): Duration Since Quitting Job Due to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was duration since quitting job due to OA. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Health Care Resource Utilization (HCRU): Number of Nights Stayed in the Hospital Due to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was number of nights stayed in the hospital due to OA. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Health Care Resource Utilization (HCRU): Number of Nights Stayed in the Hospital Due to Osteoarthritis

Health Care Resource Utilization (HCRU): Number of Participants Hospitalized Due to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was number of participants who were hospitalized due to OA. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Health Care Resource Utilization (HCRU): Number of Participants Who Quit Job Due to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was number of participants who quit job due to OA. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Health Care Resource Utilization (HCRU): Number of Participants Who Visited the Emergency Room Due to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was number of participants who visited the emergency room due to OA. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Health Care Resource Utilization (HCRU): Number of Visits of Services Directly Related to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Visits of services directly related to OA evaluated were: visits to primary care physician, neurologist, rheumatologist, physician assistant or nurse practitioner, pain specialist, orthopedist, physical therapist, chiropractor, alternative medicine or therapy, podiatrist, nutritionist/dietitian, radiologist, home healthcare services and other practitioner. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Health Care Resource Utilization (HCRU): Number of Visits to the Emergency Room Due to Osteoarthritis

Osteoarthritis HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was number of visits to the emergency room due to OA. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Number of Days of Rescue Medication Used During Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

In case of inadequate pain relief during the treatment period, acetaminophen/paracetamol up to 3000 mg per day and up to 3 days in a week between baseline and Week 16, and 3000 mg per day and up to 7 days per week between Week 16 and 64 could be taken as rescue medication. Number of days the participants used the rescue medication during the particular study weeks were summarized. (NCT02528188)
Timeframe: Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Number of Participants Who Took Rescue Medication During Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

In case of inadequate pain relief, acetaminophen/paracetamol up to 3000 mg per day and up to 3 days in a week between baseline and Week 16, and 3000 mg per day and up to 7 days per week between Week 16 and 64 could be taken as rescue medication. Number of participants with any use of rescue medication during the particular study week were summarized. (NCT02528188)
Timeframe: Weeks 2, 4, 8, 16, 24, 32, 40, 48 and 56

Number of Participants With Anti-Tanezumab Antibodies

Human serum anti-drug antibody (ADA) samples were analyzed for the presence or absence of anti-tanezumab antibodies by using a semi quantitative enzyme linked immunosorbent assay (ELISA). (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 32, 48, 56, 64 and 80

Number of Participants With Confirmed Orthostatic Hypotension

Orthostatic hypotension was defined as postural change (supine to standing) that met the following criteria: For systolic BP <=150 mmHg (mean supine): Reduction in systolic BP>=20 mmHg or reduction in diastolic BP>=10 mmHg at the 1 and/or 3 minute standing BP measurements. For systolic BP >150 mmHg (mean supine): Reduction in systolic BP>=30 mmHg or reduction in diastolic BP>=15 mmHg at the 1 and/or 3 minute standing BP measurements. If the 1 minute or 3 minute standing BP in a sequence met the orthostatic hypotension criteria, then that sequence was considered positive. If 2 of 2 or 2 of 3 sequences were positive, then orthostatic hypotension was considered confirmed. (NCT02528188)
Timeframe: Baseline, Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56, 64 and 80

Number of Participants With Progression of Osteoarthritis in the Index Hip (Kellgren-Lawrence Grade 2 or 3) According to Bland and Altman Method at Weeks 56 and 80

Progression of OA according to Bland-Altman methodology as defined by a decrease in JSW >=1.96 times within-participant standard deviation of the change in JSW in the index hip. The number of participants with progression of OA in the index hip per Bland-Altman methodology are reported. Kellgren-Lawrence grade system was a method of classifying the severity of hip OA using five grades i.e. 0 (no radiographic features of OA), 1 (doubtful JSN and possible osteophytic lipping), 2 (definite osteophytes and possible JSN on anteroposterior weight-bearing radiograph), 3 (multiple osteophytes, definite JSN, sclerosis, possible bony deformity), 4 (large osteophytes, marked JSN, severe sclerosis and definite bony deformity). Higher grade indicating worse hip function. (NCT02528188)
Timeframe: Weeks 56 and 80

Number of Participants With Progression of Osteoarthritis in the Index Knee (Kellgren-Lawrence Grade 2 or 3) According to Bland and Altman Method at Weeks 56 and 80

Progression of OA according to Bland-Altman as defined by a decrease JSW >=1.96 times within-participant standard deviation of change in JSW. The number of participants with progression of OA in the index knee are summarized separately by the compartment of OA at baseline (medial or lateral). Kellgren-Lawrence grade system was a method of classifying the severity of knee OA using five grades i.e. 0 [no radiographic features of OA], 1 [doubtful joint space narrowing (JSN) and possible osteophytic lipping], 2 [definite osteophytes and possible JSN on anteroposterior weight-bearing radiograph], 3 [multiple osteophytes, definite JSN, sclerosis, possible bony deformity], 4 [large osteophytes, marked JSN, severe sclerosis and definite bony deformity]. Higher grade indicating worse knee function. (NCT02528188)
Timeframe: Weeks 56 and 80

Number of Participants With Treatment-Emergent Adverse Events (AEs) and Serious Adverse Events (SAEs)

An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. SAE was an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly. Treatment-emergent were events between first dose of study drug and up to Week 80 that were absent before treatment or that worsened relative to pre-treatment state. AEs included both serious and non-serious AEs. Clinically significant physical examination abnormalities were reported as AEs. (NCT02528188)
Timeframe: Baseline up to Week 80

Number of Participants With Treatment-Related Treatment-Emergent Adverse Events (AEs) and Serious Adverse Events (SAEs)

Treatment-related AE was any untoward medical occurrence attributed to study drug in a participant who received study drug. SAE was an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly. Treatment-emergent were events between first dose of study drug and up to Week 80 that were absent before treatment or that worsened relative to pre-treatment state. Relatedness to study drug was assessed by the investigator. (NCT02528188)
Timeframe: Baseline up to Week 80

Observation Time-Adjusted Event Rate of Participants With Individual Adjudicated Joint Safety Outcome

Observation time was defined as the start day of first SC study medication until either the (i) date of completion of or withdrawal from study, if a participant did not have the event, or (ii) date of the event (earliest event within each participant in the case of multiple events). Individual joint safety outcome included rapidly progressive OA (type-1 only), rapidly progressive OA (type-2 only), rapidly progressive OA (type-1 or type-2 combined), subchondral insufficiency fracture, primary osteonecrosis, and pathological fracture. Event rate was calculated as the number of events per 1000 participant-years at risk. (NCT02528188)
Timeframe: Baseline up to Week 80

Percentage of Participants Achieving Improvement of >=2 Points in Patient's Global Assessment (PGA) of Osteoarthritis at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

"PGA of OA was assessed by asking a question from participants: Considering all the ways your OA in your knee or hip affects you, how are you doing today? Participants responded on a scale ranging from 1-5, where, 1=very good (no symptom and no limitation of normal activities), 2= good (mild symptoms and no limitation of normal activities), 3= fair (moderate symptoms and limitation of some normal activities), 4= poor (severe symptoms and inability to carry out most normal activities), and 5 = very poor (very severe symptoms and inability to carry out all normal activities). Higher scores indicated worse condition. Percentage of participants with improvement of at least 2 points from baseline in PGA of OA were reported. Missing data was imputed using mixed BOCF/LOCF." (NCT02528188)
Timeframe: Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Percentage of Participants Achieving Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Reduction >=30 Percent (%), >=50%, >=70% and >=90% Response at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Percentage of participants with reduction in WOMAC pain intensity of >= 30%, 50%, 70% and 90% at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64 compared to baseline were classified as responders to WOMAC pain subscale and are reported here. WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. The WOMAC pain subscale is a 5-item questionnaire used to assess the amount of pain experienced due to OA of index joint (knee or hip) during past 48 hours. It was calculated as the mean of scores from 5 individual questions scored on a NRS. Scores for each question and WOMAC Pain subscale score on NRS ranged from 0 (no pain) to 10 (extreme pain), where higher scores indicated higher pain. Missing data was imputed using mixed BOCF/LOCF. (NCT02528188)
Timeframe: Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Percentage of Participants Achieving Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Physical Function Subscale Reduction of >=30%, >=50%, >=70% and >=90% Response at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Percentage of participants with reduction in WOMAC physical function of >=(30%,50%,70%,90%) at Weeks 2,4,8,16,24,32,40,48,56 and 64 compared to baseline were classified as responders to WOMAC physical function subscale. WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. Physical function:Participant's ability to move around and perform usual activities of daily living. WOMAC physical function subscale17-item questionnaire used to assess the degree of difficulty experienced due to OA in index joint (knee/hip) during past 48 hours, calculated as mean of the scores from 17 individual questions scored on a NRS. Scores for each question and WOMAC physical subscale on NRS ranged from 0 (no difficulty) to 10 (extreme difficulty), where higher scores indicated extreme difficulty/worse physical function. Missing data was imputed using mixed BOCF/LOCF. (NCT02528188)
Timeframe: Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Percentage of Participants Meeting Outcome Measures in Arthritis Clinical Trials-Osteoarthritis Research Society International (OMERACT-OARSI) Responder Index at Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Participants were considered as OMERACT-OARSI responders: if the change (improvement) from baseline to week of interest was >=50 percent and >= 2 units in either WOMAC pain subscale or physical function subscale score; if change (improvement) from baseline to week of interest was >=20 percent and >=1 unit in at least 2 of the following: 1) WOMAC pain subscale score, 2) WOMAC physical function subscale score, 3) PGA of OA. WOMAC pain subscale assess amount of pain experienced (score: 0 [no pain] to 10 [extreme pain], higher score = more pain), WOMAC physical function subscale assess degree of difficulty experienced (score: 0 [no difficulty] to 10 [extreme difficulty], higher score = worse physical function) and PGA of OA (score: 1 [very good] to 5 [very poor], higher score = worse condition). Missing data was imputed using mixed baseline/last observation carried forward (BOCF/LOCF). (NCT02528188)
Timeframe: Weeks 2, 4, 8, 16, 24, 32, 40, 48, 56 and 64

Percentage of Participants With Cumulative Percent Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale at Weeks 16, 24 and 56

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. The WOMAC pain subscale is a 5-item questionnaire used to assess the amount of pain experienced due to OA of index joint during past 48 hours. It was calculated as the mean of scores from 5 individual questions scored on a NRS. Scores for each question and WOMAC Pain subscale score on NRS ranged from 0 (no pain) to 10 (extreme pain), where higher scores indicated higher pain. Percentage of participants with cumulative reduction (as percent) (greater than [>] 0% ; >= 10, 20, 30, 40, 50, 60, 70, 80 and 90%; = 100 %) in WOMAC pain subscale from Baseline to Weeks 16, 24 and 56 were reported, participants (%) are reported more than once in categories specified. Missing data was imputed using mixed BOCF/LOCF. (NCT02528188)
Timeframe: Baseline, Weeks 16, 24 and 56

Percentage of Participants With Cumulative Percent Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Physical Function Subscale at Weeks 16, 24 and 56

Percentage of participants with cumulative reduction (as percent) (> 0 %; >= 10%, 20%, 30%, 40%, 50%, 60%, 70%, 80% and 90%; =100%) in WOMAC physical function subscale from baseline to Weeks 16, 24 and 56 were reported. WOMAC:Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. Physical function: participant's ability to move around and perform usual activities of daily living. WOMAC physical function subscale:17-item questionnaire to assess the degree of difficulty experienced due to OA in index joint (knee or hip) during past 48 hours, calculated as mean of the scores from 17 individual questions scored on a NRS. Scores for each question and WOMAC Pain subscale on NRS ranged from 0 (no difficulty) to 10 (extreme difficulty), higher scores indicate extreme difficulty/worse physical function. Missing data was imputed using mixed BOCF/LOCF. (NCT02528188)
Timeframe: Baseline, Weeks 16, 24 and 56

Percentage of Participants With Individual Adjudicated Joint Safety Outcome

Any participant with incidence of an adjudicated outcome of rapidly progressive OA (type-1 only), rapidly progressive OA (type-2 only), rapidly progressive OA (type-1 or type-2 combined), subchondral insufficiency fracture, primary osteonecrosis, and pathological fracture. Rapidly progressive OA type 1 events were those that the Adjudication Committee considered to have significant loss of JSW >=2 mm within approximately 1 year without gross structural failure. Rapidly progressive OA type 2 events were those considered to have abnormal loss/destruction of bone including limited or total collapse of at least one subchondral surface (e.g., medial femoral condyle) that is not normally present in conventional end-stage OA. (NCT02528188)
Timeframe: Baseline up to Week 80

Treatment Satisfaction Questionnaire Medicine Version II (TSQM v.II) Score With Effectiveness, Side Effects, Convenience, and Overall Satisfaction Responses

TSQM v.II is a self-administered 11-item validated scale that quantified participant's level of satisfaction with study medication (scored on a 7-point Likert scale [1= extremely dissatisfied, 2=very dissatisfied, 3=dissatisfied, 4=somewhat satisfied, 5=satisfied, 6=very satisfied, 7=extremely satisfied]) and dissatisfaction with side effects (3 questions scored on 5 point Likert scale [1= extremely dissatisfied, 2=very dissatisfied, 3=somewhat dissatisfied, 4=slightly dissatisfied, 5=not at all dissatisfied] and 1 question on 2 point scale [0 =No, 1=Yes]). Participants were asked to assess their level of satisfaction taking all things into account. The 11 questions of the TSQM were used to calculate the 4 endpoints of effectiveness, side Effects, convenience and global satisfaction, each scored on a 0-100 scale with 100 being the best level of satisfaction. (NCT02528188)
Timeframe: Weeks 16 and 56

Health Care Resource Utilization (HCRU): Number of Participants Who Used Any Aids/Devices for Doing Things Due to Osteoarthritis

OA HCRU assessed healthcare usage during the last 3 months (for Baseline and Week 80) and past 8 weeks (for Week 64). Domain evaluated was number of participants who used any aids/devices for doing things. Aids such as walking aid, wheelchair, device or utensil for dress/bathe/eat and any other aids/devices. (NCT02528188)
Timeframe: Baseline, Weeks 64 and 80

Number of Participants With Categorical Change From Baseline in Lower Extremity Activity Scale (LEAS) at Weeks 4, 8, 16, 24, 56 and 80

The LEAS is a self-administered scale to assess activity level in participants having total knee arthroplasty. The LEAS scale reflected four levels of lower-extremity activity (1)housebound(unable to walk or a minimal ability to walk) (2)more ordinary walking about the house (3)walking about the community (4)walking about the community as well as substantial work or exercise. It consisted of 12 questions resulting in 18-level scale that allowed participants to select a single description that most represented his or her self-perceived activity level. The final score was simply the number of the descriptor selected by the participant as being most representative of his or her activity level. The minimum possible score was 1(entirely bedbound) and the maximum possible score was 18(currently competitive athlete). Higher score indicated increased activity. Categorical changes from baseline were reported in terms of improvement (Change >0), No change and worsening (Change less than [<] 0). (NCT02528188)
Timeframe: Baseline, Weeks 4, 8, 16, 24, 56 and 80

Number of Participants With Responses to European Quality of Life-5 Dimensions-5 Levels (EQ-5D-5L): Anxiety/ Depression Domain

Number of participants with anxiety/ depression domain responses of EQ-5D-5L were provided. EQ-5D-5L is a standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional visual analogue scale (VAS). EQ-5D health state profile is comprised of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1=no problems, 2=slight problems, 3=moderate problems, 4=severe problems, and 5=extreme problems. Higher scores indicated greater levels of problems across the five dimensions. (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 24, 40, 56 and 64

Number of Participants With Responses to European Quality of Life-5 Dimensions-5 Levels (EQ-5D-5L): Mobility Domain

Number of participants with mobility domain responses of EQ-5D-5L were provided. EQ-5D-5L is a standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional visual analogue scale (VAS). EQ-5D health state profile is comprised of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1=no problems, 2=slight problems, 3=moderate problems, 4=severe problems, and 5=extreme problems. Higher scores indicated greater levels of problems across the five dimensions. (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 24, 40, 56 and 64

Number of Participants With Responses to European Quality of Life-5 Dimensions-5 Levels (EQ-5D-5L): Pain/Discomfort Domain

Number of participants with pain/discomfort domain responses of EQ-5D-5L were provided. EQ-5D-5L is a standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional visual analogue scale (VAS). EQ-5D health state profile is comprised of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1=no problems, 2=slight problems, 3=moderate problems, 4=severe problems, and 5=extreme problems. Higher scores indicated greater levels of problems across the five dimensions. (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 24, 40, 56 and 64

Number of Participants With Responses to European Quality of Life-5 Dimensions-5 Levels (EQ-5D-5L): Self-Care Domain

Number of participants with self-care domain responses of EQ-5D-5L were provided. EQ-5D-5L is a standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional visual analogue scale (VAS). EQ-5D health state profile is comprised of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1=no problems, 2=slight problems, 3=moderate problems, 4=severe problems, and 5=extreme problems. Higher scores indicated greater levels of problems across the five dimensions. (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 24, 40, 56 and 64

Number of Participants With Responses to European Quality of Life-5 Dimensions-5 Levels (EQ-5D-5L): Usual Activities Domain

Number of participants with usual activities domain responses of EQ-5D-5L were provided. EQ-5D-5L is a standardized participant completed questionnaire that measures health-related quality of life and translates that score into an index value or utility score. EQ-5D-5L consists of two components: a health state profile and an optional visual analogue scale (VAS). EQ-5D health state profile is comprised of 5 dimensions: mobility, self-care, usual activities, pain/discomfort and anxiety/depression. Each dimension has 5 levels: 1=no problems, 2=slight problems, 3=moderate problems, 4=severe problems, and 5=extreme problems. Higher scores indicated greater levels of problems across the five dimensions. (NCT02528188)
Timeframe: Baseline, Weeks 8, 16, 24, 40, 56 and 64

Patient Reported Treatment Impact Assessment-Modified (mPRTI) Score at Weeks 16 and 56: Participant Global Preference Assessment- Overall, do You Prefer the Drug That You Received in This Study to Previous Treatment?

The mPRTI is a self-administered questionnaire containing participant global preference assessment (to assess previous treatment and preference to continue using the investigational product) and participant willingness to use drug again assessment. To assess preference to continue using the investigational product, participants responded using IRT on a 5 point Likert scale from 1-5, where, 1= yes, I definitely prefer the drug that I am receiving now, 2= I have a slight preference for the drug that I am receiving now, 3= I have no preference either way, 4= I have a slight preference for my previous treatment, 5= No, I definitely prefer my previous treatment. Higher scores indicate lesser preference to use the investigational product. Number of participants who responded for the specified question were reported. (NCT02528188)
Timeframe: Weeks 16 and 56

Patient Reported Treatment Impact Assessment-Modified (mPRTI) Score at Weeks 16 and 56: Participant Willingness to Use Drug Again Assessment- Willing to Use the Same Drug That You Have Received in This Study for Your Osteoarthritis Pain?

The mPRTI is a self-administered questionnaire containing participant global preference assessment (to assess previous treatment and preference to continue using the investigational product) and participant willingness to use drug again assessment. To assess participant willingness to use drug again, participants responded using IRT on a 5 point likert scale from 1-5, where, 1= yes, I would definitely want to use the same drug again, 2= I might want to use the same drug again, 3= I am not sure, 4= I might not want to use the same drug again, 5= no, I definitely would not want to use the same drug again. Higher scores indicate lesser willingness to use the investigational product. Number of participants who responded for the specified question were reported. (NCT02528188)
Timeframe: Weeks 16 and 56

Patient-Reported Treatment Impact Assessment- Modified (mPRTI) Score at Weeks 16 and 56: Participant Global Preference Assessment- What is The Current or Most Recent Treatment You Were Receiving for Osteoarthritis Pain Before Enrolling?

The mPRTI is a self-administered questionnaire containing participant's global preference assessment (to assess previous treatment and preference to continue using the investigational product) and participant's willingness to use drug again assessment. To assess current or most recent treatment, participants responded for, 1=injectable prescription medicines, 2=prescription medicines taken by mouth, 3=surgery, 4=prescription medicines and surgery and 5=no treatment. Number of participants who responded for the specified question were reported. (NCT02528188)
Timeframe: Weeks 16 and 56

Number of Participants Who Discontinued Due to Lack of Efficacy

Number of participants who discontinued due to lack of efficacy were reported. (NCT00864097)
Timeframe: Baseline up to end of study (Week 32)

Change From Baseline in 36-Item Short-Form Health Survey Version 2 (SF-36v2) Domain Scores at Week 12 and 24

SF-36v2 was a standardized survey evaluating 8 aspects of functional health and well-being: physical and social functioning, physical and role limitations due to emotional problems, bodily pain, general health, vitality, and mental health. The total score and the score for a section was an average of the individual question scores, which were scaled 0-100. Higher scores reflected better participant status and positive change indicated an improvement. (NCT00864097)
Timeframe: Baseline, Week 12, and 24

Change From Baseline in 36-Item Short-Form Health Survey Version 2 (SF-36v2) Physical and Mental Component Scores at Week 12 and 24

SF-36v2: standardized survey evaluating 8 aspects of functional health and wellbeing (physical and social functioning, role limitations due to physical and emotional problems, bodily pain, general health, vitality, mental health). Total score for each aspect were scaled 0-100. Higher scores reflect better participant status and positive change indicated an improvement. For obtaining physical and mental component scores, z-score for each scale=(observed score - mean score for general 1990 United States [US] population)/corresponding standard deviation. The 2 component scores were obtained by multiplying each aspect z-score by physical or mental factor score coefficient (1990 general US population) and summing the eight products. Component scores indicated how many standard deviations higher (in case of positive z-score [better functioning])/lower (in case of negative z-score [worse functioning]) participant's value was relative to the mean of the reference population. (NCT00864097)
Timeframe: Baseline, Week 12 and 24

Change From Baseline in Average Pain Score in the Index Knee or Hip at Weeks 1, 2, 3, 4, 6, 8, 10, 12, 16, 20, and 24

Participants were asked to assess index joint (knee/hip) pain during the past 24 hours on an 0-10 point integer scale ranging from 0 (no pain) to 10 (worst possible pain). Baseline score was calculated as the mean of the scores in the index joint over the 3 days days in the initial pain assessment period and a weekly mean was calculated using the daily pain scores in the index joint within each study week. The change from Baseline was calculated using the difference between each post-baseline weekly mean and the baseline mean score, where negative change indicated an improvement. (NCT00864097)
Timeframe: Baseline, Weeks 1, 2, 3, 4, 6, 8, 10, 12, 16, 20, and 24

Change From Baseline in European Quality of Life - 5 Dimension (EQ-5D) Index Score at Week 24

EQ-5D was a standardized, participant-administered measure of health outcome. It provides a descriptive profile for 5 dimensions (mobility, self-care, usual activities, pain/discomfort, anxiety/depression), using 3 levels (no, moderate, or extreme dysfunction) and a single index value characterizing current health status using a visual analog scale with score ranging from 0 (worst) to 100 (best). EQ-5D summary index was obtained with a formula that weights each level of the dimensions. The index-based score was interpreted along a continuum of 0 (death) to 1 (perfect health). Negative change from baseline represented worsening. (NCT00864097)
Timeframe: Baseline, Week 24

Change From Baseline in Patient Global Assessment (PGA) of Osteoarthritis Score at Week 16

"Participants answered: Considering all the ways your osteoarthritis in your index joint (knee/hip) affects you, how are you doing today? Participants responded by using a 5-point Likert scale, where 1 = very good (asymptomatic and no limitation of normal activities), 2 = good (mild symptoms and no limitation of normal activities), 3 = fair (moderate symptoms and limitation of some normal activities), 4 = poor (severe symptoms and inability to carry out most normal activities), and 5 = very poor (very severe symptoms which are intolerable and inability to carry out all normal activities). Higher score indicated worst condition." (NCT00864097)
Timeframe: Baseline, Week 16

Change From Baseline in Patient Global Assessment (PGA) of Osteoarthritis Score at Weeks 2, 4, 8, 12, and 24

Change From Baseline in the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score at Weeks 2, 4, 8, 12 and 24

Change From Baseline in the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Physical Function Subscale Score at Weeks 2, 4, 8, 12, and 24

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. WOMAC physical function is a 17-item questionnaire used to assess the degree of difficulty experienced due to osteoarthritis in index knee or hip during past 48 hours. It is calculated as mean of the scores from 17 individual questions, each scored on a NRS of 0 (no difficulty) to 10 (extreme difficulty), where higher scores indicate worse function. Total score range for WOMAC physical function subscale score is 0 (no difficulty) to 10 (extreme difficulty), where higher scores indicate worse function. Physical function refers to participant's ability to move around and perform usual activities of daily living. (NCT00864097)
Timeframe: Baseline, Weeks 2, 4, 8, 12, and 24

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Average Score at Weeks 2, 4, 8, 12, 16, and 24

WOMAC Index: self-administered, disease-specific 24 item questionnaire which assesses clinically important, participant-relevant symptoms for pain (5 items), stiffness (2 items), and physical function (17 items) in participants with osteoarthritis of the hip and/or knee. WOMAC average score is the mean of the WOMAC pain, physical function and stiffness subscale scores and ranges from 0 to 10, with higher score indicating worse response. Greater reduction in WOMAC average score indicated greater improvement. (NCT00864097)
Timeframe: Baseline, Weeks 2, 4, 8, 12, 16, and 24

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Item: Pain When Going Up or Downstairs at Weeks 2, 4, 8, 12, 16, and 24

"Participants answered the question: How much pain have you had when going up or down the stairs? Participants responded by using an 11-point scale, where 0 = no pain and 10 = extreme pain. Where 0 is the best response and negative change indicated an improvement." (NCT00864097)
Timeframe: Baseline, Weeks 2, 4, 8, 12, 16, and 24

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Item: Pain When Walking on a Flat Surface at Weeks 2, 4, 8, 12, 16, and 24

"Participants answered the question: How much pain have you had when walking on a flat surface? Participants responded by using an 11-point scale where 0 = no pain and 10 = extreme pain. Where 0 is the best response and negative change indicated an improvement." (NCT00864097)
Timeframe: Baseline, Week 2, 4, 8, 12, 16, 24

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score at Week 16

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Physical Function Subscale Score at Week 16

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. WOMAC physical function is a 17-item questionnaire used to assess the degree of difficulty experienced due to osteoarthritis in index knee or hip during past 48 hours. It is calculated as mean of the scores from 17 individual questions, each scored on a NRS of 0 (no difficulty) to 10 (extreme difficulty), where higher scores indicate worse function. Total score range for WOMAC physical function subscale score is 0 (no difficulty) to 10 (extreme difficulty), where higher scores indicate worse function. Physical function refers to participant's ability to move around and perform usual activities of daily living. (NCT00864097)
Timeframe: Baseline, Week 16

Change From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Stiffness Subscale Score at Weeks 2, 4, 8, 12, 16, and 24

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with OA. WOMAC stiffness subscale is a 2-item questionnaire used to assess the amount of stiffness experienced due to osteoarthritis in index knee or hip during past 48 hours. It is calculated as mean of the scores from 2 individual questions scored on NRS of (no stiffness) to 10 (extreme stiffness), with higher scores indicate higher stiffness. Total score range for WOMAC stiffness subscale score is (no stiffness) to 10 (extreme stiffness), where higher scores indicate higher stiffness. Stiffness is defined as a sensation of decreased ease in movement of knee/hip. Negative change indicated an improvement. (NCT00864097)
Timeframe: Baseline, Weeks 2, 4, 8, 12, 16, and 24

Number of Participants With Adverse Events (AEs) and Serious Adverse Events (SAEs)

An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. An SAE was an AE resulting in any of the following outcomes or deemed significant for any other reason: death; initial or prolonged inpatient hospitalization; life-threatening experience (immediate risk of dying); persistent or significant disability/incapacity; congenital anomaly. Treatment-emergent are events between first dose of study drug and up to 112 days after last dose that were absent before treatment or that worsened relative to pretreatment state. AEs included SAEs as well as non-serious AEs which occurred during the trial. (NCT00864097)
Timeframe: Baseline up to 112 days after last intravenous dose (up to Week 32)

Number of Participants With Change From Baseline in European Quality of Life - 5 Dimension (EQ-5D) Individual Health State Profile at Week 24

"EQ-5D was a standardized, participant-administered measure of health outcome. It provides a descriptive profile for 5 dimensions (mobility, self-care, usual activities, pain/discomfort, anxiety/depression), using 3 levels (no, moderate, or extreme dysfunction) and a single index value characterizing current health status using a visual analog scale with score ranging from 0 (worst) to 100 (best). Baseline EQ-5D individual health state profile was determined as number of participants no dysfunction, moderate or some dysfunction and extreme dysfunction and change from baseline in EQ-5D individual health state profile was determined as number of participants improved, no change or worsened." (NCT00864097)
Timeframe: Baseline, Week 24

Number of Participants With Intravenous Doses of Study Medication

Number of participants were reported based on the maximum number of intravenous (IV) doses of either tanezumab or placebo received. (NCT00864097)
Timeframe: Day 1 up to Week 16

Percentage of Participants With At Least 30%, 50%, 70% and 90% Reduction From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score; LOCF

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with osteoarthritis (OA). WOMAC pain subscale is a 5-item questionnaire used to assess the amount of pain experienced due to osteoarthritis in index knee or hip during past 48 hours. It is calculated as mean of the scores from 5 individual questions, each scored on a numerical rating scale (NRS) of 0 (no pain) to 10 (extreme pain), where higher scores indicate higher pain. Total score range for WOMAC pain subscale score is 0 (no pain) to 10 (extreme pain), where higher scores indicate higher pain. Greater percentage reduction indicates greater improvement. Percentage of participants with reduction in WOMAC pain intensity of at least (>=) 30%, 50%, 70% and 90% at Weeks 2, 4, 8, 12, 16, 24 and 32 compared to baseline were classified as responders to WOMAC pain subscale and are reported here. (NCT00864097)
Timeframe: Baseline, Weeks 2, 4, 8, 12, 16, and 24

Percentage of Participants With Cumulative Reduction From Baseline in Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score at Week 16 and 24

WOMAC: Self-administered, disease-specific questionnaire which assesses clinically important, participant-relevant symptoms for pain, stiffness and physical function in participants with osteoarthritis (OA). WOMAC pain subscale is a 5-item questionnaire used to assess the amount of pain experienced due to osteoarthritis in index knee or hip during past 48 hours. It is calculated as mean of the scores from 5 individual questions, each scored on a numerical rating scale (NRS) of 0 (no pain) to 10 (extreme pain), where higher scores indicate higher pain. Total score range for WOMAC pain subscale score is 0 (no pain) to 10 (extreme pain), where higher scores indicate higher pain. Greater percentage reduction indicates greater improvement. Percentage of participants with cumulative reduction (as percent) (greater than 0%; >= 10, 20, 30, 40, 50, 60, 70, 80 and 90%; = 100 %) in WOMAC pain subscale from Baseline to Weeks 16 and 24 were reported. (NCT00864097)
Timeframe: Baseline, Week 16 and 24

Percentage of Participants With Improvement of at Least 2 Points in Patient Global Assessment (PGA) of Osteoarthritis; Baseline Observation Carried Forward (BOCF)

Percentage of Participants With Improvement of at Least 2 Points in Patient Global Assessment (PGA) of Osteoarthritis; LOCF

Percentage of Participants With Outcome Measures in Rheumatology - Osteoarthritis Research Society International (OMERACT-OARSI) Response; LOCF

OMERACT-OARSI responder: participant has >=50 percent (%) change and >=2 absolute change from Baseline in either WOMAC pain or physical function subscale scores or at least 2 of the following being true: >=20% change and >=1 absolute change from Baseline in WOMAC pain subscale; >=20% change and >=1 absolute change from Baseline in the WOMAC physical function subscale; >=20% change and >=1 absolute change from Baseline in PGA of osteoarthritis. WOMAC pain and physical function score: 0 to 10 with higher score = worse response. PGA score: 1 = very good and 5 = very poor. (NCT00864097)
Timeframe: Weeks 2, 4, 8, 12, 16, and 24

Time to Discontinuation (TTD) Due to Lack of Efficacy

Median time to discontinuation due to lack of efficacy was estimated using Kaplan-Meier method. (NCT00864097)
Timeframe: Baseline up to Week 16 and 24

Change From Baseline to the Average of Weeks 2, 6, and 12 After Trial Entry in Osteoarthritis Pain Measured on the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score.

"The pain in subjects with osteoarthritis was measured using the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) pain subscale score. The WOMAC pain subscale score is calculated as the average of the visual analogue scale (VAS) scores from 5 pain subscale questions. Subjects mark the VAS, which is a horizontal line 100 mm in length, with a single vertical line to indicate their pain level over the last 24 hours, with 0 mm representing No Pain and 100 mm representing Extreme Pain.~The WOMAC pain subscale score difference was calculated as the WOMAC pain subscale score assessed at Weeks 2, 6, and 12 minus the average of the WOMAC pain subscale score assessed at baseline." (NCT01461369)
Timeframe: Baseline to Week 12/Early Termination

Change From Baseline to the Average of Weeks 2, 6, and 12 After Trial Entry in Osteoarthritis Pain, Stiffness, and Function Measured Using the Total (Composite) Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Score.

"Pain, stiffness, and function in subjects with osteoarthritis were measured using the Western Ontario and McMaster Universities (WOMAC) Index, which is a 24-item questionnaire. The total (composite) WOMAC score is calculated as the average of the mean visual analogue scale (VAS) scores from the questions in the pain, stiffness, and function subscales. Subjects mark the VAS, which is a horizontal line 100 mm in length, with a single vertical line to indicate their response to each of the questions, with 0 mm representing No Pain, Stiffness, or Difficulty and 100 mm representing Extreme Pain, Stiffness, and Difficulty.~The total (composite) WOMAC score difference was calculated as the total (composite) WOMAC score assessed at Weeks 2, 6, and 12 minus the total (composite) WOMAC score assessed at baseline." (NCT01461369)
Timeframe: Baseline to Week 12/Early Termination

Change From Baseline to the Average of Weeks 2, 6, and 12 After Trial Entry in Pain Intensity Difference Measured Using the 100-mm Visual Analogue Scale.

"The pain intensity is assessed using a visual analogue scale (VAS), which is a horizontal line 100 mm in length. Subjects mark the VAS with a single vertical line to indicate their current pain level, with 0 mm representing No Pain and 100 mm representing Worst Pain Imaginable.~The VAS pain intensity difference is calculated as the average of the VAS pain intensity scores at Weeks 2, 6, and 12 minus the VAS pain intensity at baseline." (NCT01461369)
Timeframe: Baseline to Week 12/Early Termination

Change From Baseline to Week 12 After Trial Entry in Osteoarthritis Pain Measured on the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score.

"The pain in subjects with osteoarthritis was measured using the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) pain subscale score. The WOMAC pain subscale score is calculated as the average of the visual analogue scale (VAS) scores from 5 pain subscale questions. Subjects mark the VAS, which is a horizontal line 100 mm in length, with a single vertical line to indicate their pain level over the last 24 hours, with 0 mm representing No Pain and 100 mm representing Extreme Pain.~The WOMAC pain subscale score difference is calculated as the WOMAC pain subscale score assessed at Week 12 minus the WOMAC pain subscale score assessed at baseline." (NCT01461369)
Timeframe: Baseline to Week 12/Early Termination

Change From Baseline to Week 2 After Trial Entry in Osteoarthritis Pain Measured on the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score.

"The pain in subjects with osteoarthritis was measured using the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) pain subscale score. The WOMAC pain subscale score is calculated as the average of the visual analogue scale (VAS) scores from 5 pain subscale questions. Subjects mark the VAS, which is a horizontal line 100 mm in length, with a single vertical line to indicate their pain level over the last 24 hours, with 0 mm representing No Pain and 100 mm representing Extreme Pain.~The WOMAC pain subscale score difference was calculated as the WOMAC pain subscale score assessed at Week 2 minus the WOMAC pain subscale score assessed at baseline." (NCT01461369)
Timeframe: Baseline to Week 2

Change From Baseline to Week 6 After Trial Entry in Osteoarthritis Pain Measured on the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Pain Subscale Score.

"The pain in subjects with osteoarthritis was measured using the Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) pain subscale score. The WOMAC pain subscale score is calculated as the average of the visual analogue scale (VAS) scores from 5 pain subscale questions. Subjects mark the VAS, which is a horizontal line 100 mm in length, with a single vertical line to indicate their pain level over the last 24 hours, with 0 mm representing No Pain and 100 mm representing Extreme Pain.~The WOMAC pain subscale score difference was calculated as the WOMAC pain subscale score assessed at Week 6 minus the WOMAC pain subscale score assessed at baseline." (NCT01461369)
Timeframe: Baseline to Week 6

Mean Short Form-36 Mental Component Summary Scores at Week 52/Early Termination (ET) and Change From Baseline to Week 52/ET

The Short Form-36 is a validated 11-item health survey that assesses subject views about his/her functional health and well-being. The survey consists of 36 questions concerning daily or recent health-related activities and assesses 8 health domains using scaled scores. The mental component score is composed of a subset of the 8 health domains. Each scale is directly transformed into a 0 to 100 scale on the assumption that each question carries equal weight. A score of 0 is equal to maximum disability, and a score of 100 is equivalent to no disability. (NCT01510912)
Timeframe: Baseline to Week 52/Early Termination

Mean Short Form-36 Physical Component Summary Scores at Week 52/Early Termination (ET) and Change From Baseline to Week 52/ET

The Short Form-36 is a validated 11-item health survey that assesses subject views about his/her functional health and well-being. The survey consists of 36 questions concerning daily or recent health-related activities and assesses 8 health domains using scaled scores. The physical component score is composed of a subset of the 8 health domains. Each scale is directly transformed into a 0 to 100 scale on the assumption that each question carries equal weight. A score of 0 is equal to maximum disability, and a score of 100 is equivalent to no disability. (NCT01510912)
Timeframe: Baseline to Week 52/Early Termination

Safety of Diclofenac 35 mg Capsules as Assessed by the Incidence of Adverse Events From Baseline to Week 52 or Early Termination

The safety of Diclofenac 35 mg capsules was assessed by the number of subjects with treatment-emergent adverse events (TEAEs), severe TEAEs, and serious adverse events. (NCT01510912)
Timeframe: Baseline to Week 52/Early Termination

Percent Change From Baseline in Pain Score During Week 1

Participants assessed their knee pain using a visual analog scale (VAS) where 0=no pain and 100=worst possible pain. Pain scores were recorded in an electronic diary prior to and 4 hours after the first daily application of diclofenac gel for breakthrough pain. The daily percent change in pain scores over the 7 days prior to Week 1 were averaged. Percent change from Baseline (average pain score 7 days prior to first treatment) was calculated as (value at baseline - value at post-baseline visit) / (value at baseline) x 100. A positive change from Baseline indicates improvement. (NCT01383954)
Timeframe: Baseline and Week 1

Percent Change From Baseline in Pain Score During Week 2

Participants assessed their knee pain using a visual analog scale (VAS) where 0=no pain and 100=worst possible pain. Pain scores were recorded in an electronic diary prior to and 4 hours after the first daily application of diclofenac gel for breakthrough pain. The daily percent change in pain scores over the 7 days prior to Week 2 were averaged. Percent change from baseline (average pain score 7 days prior to first treatment) was calculated as (value at baseline - value at post-baseline visit)/ (value at baseline) x 100. A positive change from baseline indicates improvement. (NCT01383954)
Timeframe: Baseline and Week 2

The Proportion of Subjects Treated With Long-term Acetaminophen (4 g/Day) That Develops Persistent ALT Elevations.

ALT was measured on Day 0 and 16 for all study participants. Subjects with an elevated ALT at Day 16 continued dosing with study drug and continued to have their ALT measured every three days until the ALT elevation resolved or until Day 40. Persistent ALT elevation was defined as any subject with an unresolved ALT elevation at study Day 40. (NCT00743093)
Timeframe: serial samples for 16-40 days

Intervention	units on a scale (Least Squares Mean)
	Change at Week 16: Percent Work Time Missed	Change at Week 16:Percent Impairment While Working	Change at Week 16: Percent Overall Work Impairment	Change at Week 16: Percent Activity Impairment	Change at Week 24: Percent Work Time Missed	Change at Week 24:Percent Impairment While Working	Change at Week 24: Percent Overall Work Impairment	Change at Week 24: Percent Activity Impairment	Change at Week 56: Percent Work Time Missed	Change at Week 56:Percent Impairment While Working	Change at Week 56: Percent Overall Work Impairment	Change at Week 56: Percent Activity Impairment
NSAID	-2.92	-26.59	-27.04	-29.38	-2.73	-25.15	-25.90	-29.76	-0.81	-34.59	-34.26	-36.17
Tanezumab 2.5 mg	-2.33	-28.07	-28.67	-30.59	-2.70	-25.34	-26.05	-29.88	-0.12	-31.49	-31.21	-34.47
Tanezumab 5 mg	-3.35	-26.94	-27.51	-31.36	-2.19	-26.66	-27.33	-30.53	-1.84	-29.92	-29.29	-32.91

Intervention	years (Median)
	Baseline	Week 64	Week 80
NSAID	2.4	4.0	1.8
Tanezumab 2.5 mg	2.0	2.4	2.0
Tanezumab 5 mg	1.8	1.8	2.0

Intervention	visits (Median)
	Baseline: Primary Care Physician	Baseline: Neurologist	Baseline: Rheumatologist	Baseline:Physician Assistant or Nurse Practitioner	Baseline: Pain Specialist	Baseline: Orthopedist	Baseline: Physical Therapist	Baseline: Chiropractor	Baseline: Alternative Medicine or Therapy	Baseline: Podiatrist	Baseline: Nutritionist/Dietitian	Baseline: Radiologist	Baseline: Home Healthcare Services	Baseline: Other Practitioner	Week 64: Primary Care Physician	Week 64: Neurologist	Week 64: Rheumatologist	Week 64: Physician Assistant Or Nurse Practitioner	Week 64: Pain Specialist	Week 64: Orthopedist	Week 64: Physical Therapist	Week 64: Chiropractor	Week 64: Alternative Medicine or Therapy	Week 64: Podiatrist	Week 64: Nutritionist/Dietitian	Week 64: Radiologist	Week 64: Home Healthcare Services	Week 64: Other Practitioner	Week 80: Primary Care Physician	Week 80: Neurologist	Week 80: Rheumatologist	Week 80: Physician Assistant or Nurse Practitioner	Week 80: Pain Specialist	Week 80: Orthopedist	Week 80: Physical Therapist	Week 80: Chiropractor	Week 80: Alternative Medicine or Therapy	Week 80: Podiatrist	Week 80: Nutritionist/Dietitian	Week 80: Radiologist	Week 80: Home Healthcare Services	Week 80: Other Practitioner
NSAID	1.0	1.0	2.0	1.0	1.0	2.0	3.0	3.0	2.0	1.0	1.0	1.0	3.0	2.0	1.0	1.0	1.0	2.0	1.0	1.0	3.0	3.0	2.0	1.0	1.0	1.0	5.0	1.0	1.0	1.0	1.0	1.0	1.0	1.0	3.0	3.0	2.0	3.0	1.0	1.0	1.0	1.0
Tanezumab 2.5 mg	1.0	1.0	1.0	1.0	1.0	2.0	4.0	3.0	2.0	1.0	1.0	1.0	2.0	2.0	1.0	1.0	1.0	1.0	1.0	1.0	4.0	3.0	1.0	1.0	2.0	1.0	4.0	1.0	1.0	1.0	1.0	1.0	1.5	1.5	8.0	3.0	3.5	1.0	1.0	1.0	2.5	1.0
Tanezumab 5 mg	1.0	1.0	2.0	1.0	2.0	1.0	3.0	3.0	2.0	1.0	1.0	1.0	1.0	2.0	1.0	1.0	1.0	1.0	1.0	1.0	4.5	2.0	2.0	1.0	1.0	1.0	4.0	1.0	1.0	1.0	1.0	1.0	2.0	1.0	5.5	4.5	1.0	1.0	1.5	1.0	4.0	1.0

Intervention	Participants (Count of Participants)
	Decreased medial JSW at Week 56	Decreased medial JSW at Week 80	Decreased lateral JSW at Week 56	Decreased lateral JSW at Week 80
NSAID	20	16	9	7
Tanezumab 2.5 mg	33	29	5	9
Tanezumab 5 mg	43	38	8	4

Intervention	Participants (Count of Participants)
	Treatment Related AEs	Treatment Related SAEs
NSAID	179	7
Tanezumab 2.5 mg	190	7
Tanezumab 5 mg	250	20

Intervention	events per 1000 participant-years (Number)
	Rapidly Progressive OA Type 1 or 2	Rapidly Progressive OA Type 1	Rapidly Progressive OA Type 2	Primary Osteonecrosis	Pathological Fracture	Subchondral Insufficiency Fracture
NSAID	11.9	10.9	1.0	0	0	3.9
Tanezumab 2.5 mg	31.4	28.4	2.9	1.0	0	5.8
Tanezumab 5 mg	63.3	49.1	13.9	1.0	0	6.9

Intervention	percentage of participants (Number)
	Week 2: At least 30% reduction	Week 2: At least 50% reduction	Week 2: At least 70% reduction	Week 2: At least 90% reduction	Week 4: At least 30% reduction	Week 4: At least 50% reduction	Week 4: At least 70% reduction	Week 4: At least 90% reduction	Week 8: At least 30% reduction	Week 8: At least 50% reduction	Week 8: At least 70% reduction	Week 8: At least 90% reduction	Week 16: At least 30% reduction	Week 16: At least 50% reduction	Week 16: At least 70% reduction	Week 16: At least 90% reduction	Week 24: At least 30% reduction	Week 24: At least 50% reduction	Week 24: At least 70% reduction	Week 24: At least 90% reduction	Week 32: At least 30% reduction	Week 32: At least 50% reduction	Week 32: At least 70% reduction	Week 32: At least 90% reduction	Week 40: At least 30% reduction	Week 40: At least 50% reduction	Week 40: At least 70% reduction	Week 40: At least 90% reduction	Week 48: At least 30% reduction	Week 48: At least 50% reduction	Week 48: At least 70% reduction	Week 48: At least 90% reduction	Week 56: At least 30% reduction	Week 56: At least 50% reduction	Week 56: At least 70% reduction	Week 56: At least 90% reduction	Week 64: At least 30% reduction	Week 64: At least 50% reduction	Week 64: At least 70% reduction	Week 64: At least 90% reduction
NSAID	32.4	14.7	6.2	1.8	44.4	24.9	11.9	3.1	54.1	32.6	15.9	4.2	68.9	51.5	28.8	8.5	59.4	47.5	29.0	11.5	56.3	46.3	27.4	10.0	54.8	46.0	29.3	10.4	54.2	44.4	28.5	10.6	52.7	43.5	27.5	10.1	81.3	60.2	34.2	12.6
Tanezumab 2.5 mg	34.8	17.8	7.7	2.4	50.2	30.4	14.5	4.3	55.9	36.8	19.3	4.7	71.8	54.9	28.9	10.3	59.4	49.3	30.8	10.3	56.8	47.4	31.2	10.3	55.7	47.2	30.0	10.8	54.6	46.2	29.6	10.3	53.1	44.3	28.2	10.1	73.0	55.4	31.1	9.6
Tanezumab 5 mg	30.5	16.5	7.1	2.5	49.5	30.5	16.4	4.9	59.0	39.3	22.4	6.6	72.9	56.5	35.0	12.7	61.1	49.4	33.8	13.3	55.7	45.8	31.5	12.9	54.6	45.2	30.4	12.0	52.9	43.2	29.4	11.4	51.2	41.5	27.0	10.5	69.0	47.3	24.3	7.9

Intervention	percentage of participants (Number)
	Week 16: >0%	Week 16: >=10%	Week 16: >=20%	Week 16: >=30%	Week 16: >=40%	Week 16: >=50%	Week 16: >=60%	Week 16: >=70%	Week 16: >=80%	Week 16: >=90%	Week 16: =100%	Week 24: >0%	Week 24: >=10%	Week 24: >=20%	Week 24: >=30%	Week 24: >=40%	Week 24: >=50%	Week 24: >=60%	Week 24: >=70%	Week 24: >=80%	Week 24: >=90%	Week 24: =100%	Week 56: >0%	Week 56: >=10%	Week 56: >=20%	Week 56: >=30%	Week 56: >=40%	Week 56: >=50%	Week 56: >=60%	Week 56: >=70%	Week 56: >=80%	Week 56: >=90%	Week 56: =100%
NSAID	87.1	82.8	75.8	68.9	59.9	51.5	38.8	28.8	18.8	8.5	3.3	64.8	63.4	62.1	59.4	54.7	47.5	38.1	29.0	20.2	11.5	3.4	59.7	58.1	56.3	52.7	48.6	43.5	36.3	27.5	18.6	10.1	4.1
Tanezumab 2.5 mg	89.5	85.0	78.1	71.8	63.7	54.9	40.9	28.9	19.4	10.3	4.4	66.7	64.9	62.2	59.4	55.2	49.3	40.7	30.8	20.6	10.3	3.9	60.8	59.1	55.9	53.1	48.6	44.3	37.0	28.2	18.9	10.1	4.5
Tanezumab 5 mg	87.6	82.8	78.3	72.9	63.5	56.5	44.8	35.0	23.9	12.7	3.9	68.2	66.4	65.2	61.1	55.7	49.4	41.2	33.8	24.0	13.3	4.5	59.1	57.0	54.8	51.2	46.8	41.5	33.8	27.0	19.1	10.5	5.3

Intervention	units on a scale (Least Squares Mean)
	Week 16: Effectiveness	Week 16: Side Effects	Week 16: Convenience	Week 16: Global Satisfaction	Week 56: Effectiveness	Week 56: Side Effects	Week 56: Convenience	Week 56: Global Satisfaction
NSAID	61.61	71.03	73.70	67.13	67.64	71.34	76.18	73.37
Tanezumab 2.5 mg	64.26	68.61	75.50	70.32	69.79	78.62	78.03	75.31
Tanezumab 5 mg	66.27	73.32	75.78	70.69	67.91	62.00	77.67	73.37

Intervention	Participants (Count of Participants)
	Baseline: Walking Aid Use72578291					Baseline: Walking Aid Use72578290	Baseline: Walking Aid Use72578289	Baseline: Wheelchair Use72578291	Baseline: Wheelchair Use72578289	Baseline: Wheelchair Use72578290	Baseline: Device/Utensil to Dress Bathe Eat72578289	Baseline: Device/Utensil to Dress Bathe Eat72578291	Baseline: Device/Utensil to Dress Bathe Eat72578290	Baseline: Other Aids Or Devices72578289	Baseline: Other Aids Or Devices72578290	Baseline: Other Aids Or Devices72578291	Week 64: Walking Aid Use72578290	Week 64: Walking Aid Use72578289	Week 64: Walking Aid Use72578291	Week 64: Wheelchair Use72578291	Week 64: Wheelchair Use72578290	Week 64: Wheelchair Use72578289	Week 64: Device/Utensil to Dress Bathe Eat72578291	Week 64: Device/Utensil to Dress Bathe Eat72578289	Week 64: Device/Utensil to Dress Bathe Eat72578290	Week 64: Other Aids Or Devices72578289	Week 64: Other Aids Or Devices72578291	Week 64: Other Aids Or Devices72578290	Week 80: Walking Aid Use72578289	Week 80: Walking Aid Use72578291	Week 80: Walking Aid Use72578290	Week 80: Wheelchair Use72578291	Week 80: Wheelchair Use72578289	Week 80: Wheelchair Use72578290	Week 80: Device/Utensil to Dress Bathe Eat72578290	Week 80: Device/Utensil to Dress Bathe Eat72578289	Week 80: Device/Utensil to Dress Bathe Eat72578291	Week 80: Other Aids Or Devices72578291	Week 80: Other Aids Or Devices72578289	Week 80: Other Aids Or Devices72578290
	Never	Rarely	Sometimes	Always	Often
Tanezumab 2.5 mg	852
Tanezumab 5 mg	838
NSAID	851
Tanezumab 5 mg	18
NSAID	24
Tanezumab 2.5 mg	71
Tanezumab 5 mg	69
NSAID	75
Tanezumab 2.5 mg	32
Tanezumab 5 mg	43
NSAID	26
Tanezumab 5 mg	29
NSAID	19
Tanezumab 2.5 mg	992
Tanezumab 5 mg	989
NSAID	988
NSAID	1
Tanezumab 2.5 mg	970
Tanezumab 5 mg	976
NSAID	977
NSAID	0
Tanezumab 2.5 mg	7
NSAID	6
Tanezumab 2.5 mg	16
NSAID	7
Tanezumab 2.5 mg	6
NSAID	5
Tanezumab 2.5 mg	932
Tanezumab 5 mg	935
NSAID	921
NSAID	9
Tanezumab 2.5 mg	27
NSAID	41
NSAID	14
NSAID	10
Tanezumab 2.5 mg	662
Tanezumab 5 mg	662
NSAID	714
Tanezumab 2.5 mg	21
Tanezumab 5 mg	9
NSAID	12
Tanezumab 2.5 mg	48
Tanezumab 5 mg	47
NSAID	37
Tanezumab 2.5 mg	20
Tanezumab 5 mg	30
NSAID	17
Tanezumab 2.5 mg	22
Tanezumab 5 mg	34
Tanezumab 2.5 mg	765
Tanezumab 5 mg	776
NSAID	794
Tanezumab 2.5 mg	760
Tanezumab 5 mg	768
NSAID	792
NSAID	2
Tanezumab 2.5 mg	733
Tanezumab 5 mg	720
NSAID	771
NSAID	11
Tanezumab 2.5 mg	19
Tanezumab 5 mg	26
NSAID	8
Tanezumab 5 mg	20
Tanezumab 5 mg	7
NSAID	3
Tanezumab 2.5 mg	373
Tanezumab 5 mg	322
NSAID	386
Tanezumab 2.5 mg	12
Tanezumab 5 mg	10
Tanezumab 2.5 mg	25
Tanezumab 5 mg	25
Tanezumab 2.5 mg	14
Tanezumab 5 mg	17
Tanezumab 2.5 mg	8
Tanezumab 5 mg	22
Tanezumab 2.5 mg	430
Tanezumab 5 mg	389
NSAID	421
Tanezumab 2.5 mg	0
Tanezumab 2.5 mg	1
Tanezumab 5 mg	1
Tanezumab 2.5 mg	425
Tanezumab 5 mg	383
NSAID	422
Tanezumab 5 mg	0
Tanezumab 5 mg	6
Tanezumab 2.5 mg	3
Tanezumab 5 mg	5
Tanezumab 5 mg	2
Tanezumab 2.5 mg	416
Tanezumab 5 mg	375
NSAID	410
Tanezumab 2.5 mg	4
NSAID	4
Tanezumab 5 mg	11
Tanezumab 2.5 mg	5
Tanezumab 5 mg	4
Tanezumab 2.5 mg	2
Tanezumab 5 mg	3

Intervention	Participants (Count of Participants)
	Change at Week 472578289			Change at Week 472578291	Change at Week 472578290	Change at Week 872578290	Change at Week 872578291	Change at Week 872578289	Change at Week 1672578290	Change at Week 1672578291	Change at Week 1672578289	Change at Week 2472578289	Change at Week 2472578290	Change at Week 2472578291	Change at Week 5672578289	Change at Week 5672578291	Change at Week 5672578290	Change at Week 8072578289	Change at Week 8072578290	Change at Week 8072578291
	Improvement	No Change	Worsening
Tanezumab 2.5 mg	423
Tanezumab 5 mg	421
NSAID	411
Tanezumab 2.5 mg	370
Tanezumab 5 mg	394
NSAID	369
Tanezumab 2.5 mg	207
Tanezumab 5 mg	180
NSAID	214
Tanezumab 2.5 mg	454
Tanezumab 5 mg	443
NSAID	445
Tanezumab 2.5 mg	325
Tanezumab 5 mg	362
NSAID	348
Tanezumab 2.5 mg	221
Tanezumab 5 mg	190
NSAID	201
Tanezumab 2.5 mg	488
Tanezumab 5 mg	470
NSAID	477
Tanezumab 2.5 mg	288
Tanezumab 5 mg	312
NSAID	312
Tanezumab 2.5 mg	224
Tanezumab 5 mg	213
NSAID	205
Tanezumab 2.5 mg	478
Tanezumab 5 mg	458
NSAID	467
Tanezumab 2.5 mg	277
Tanezumab 5 mg	302
NSAID	291
Tanezumab 2.5 mg	245
Tanezumab 5 mg	235
NSAID	236
Tanezumab 2.5 mg	486
Tanezumab 5 mg	429
NSAID	461
Tanezumab 2.5 mg	270
Tanezumab 5 mg	314
NSAID	300
Tanezumab 2.5 mg	244
Tanezumab 5 mg	252
NSAID	233
Tanezumab 2.5 mg	220
Tanezumab 5 mg	196
NSAID	227
Tanezumab 2.5 mg	105
Tanezumab 5 mg	97
NSAID	125
Tanezumab 2.5 mg	113
Tanezumab 5 mg	115
NSAID	80

Intervention	Participants (Count of Participants)
	Baseline72578289					Baseline72578290	Baseline72578291	Week 872578290	Week 872578291	Week 872578289	Week 1672578289	Week 1672578290	Week 1672578291	Week 2472578291	Week 2472578289	Week 2472578290	Week 4072578289	Week 4072578290	Week 4072578291	Week 5672578289	Week 5672578290	Week 5672578291	Week 6472578289	Week 6472578290	Week 6472578291
	Severely anxious or depressed	Extremely anxious or depressed	Not anxious or depressed	Slightly anxious or depressed	Moderately anxious or depressed
Tanezumab 2.5 mg	560
Tanezumab 5 mg	570
NSAID	585
Tanezumab 2.5 mg	252
Tanezumab 5 mg	235
NSAID	236
Tanezumab 2.5 mg	155
Tanezumab 5 mg	151
NSAID	144
Tanezumab 2.5 mg	28
Tanezumab 5 mg	37
NSAID	26
Tanezumab 2.5 mg	5
NSAID	3
Tanezumab 2.5 mg	693
Tanezumab 5 mg	703
NSAID	664
Tanezumab 2.5 mg	189
Tanezumab 5 mg	180
NSAID	206
Tanezumab 2.5 mg	64
Tanezumab 5 mg	71
NSAID	75
Tanezumab 2.5 mg	9
Tanezumab 5 mg	7
NSAID	9
Tanezumab 5 mg	5
Tanezumab 2.5 mg	680
Tanezumab 5 mg	701
NSAID	701
Tanezumab 2.5 mg	170
Tanezumab 5 mg	147
NSAID	151
Tanezumab 2.5 mg	53
Tanezumab 5 mg	62
NSAID	53
NSAID	8
Tanezumab 2.5 mg	2
Tanezumab 5 mg	4
NSAID	2
Tanezumab 2.5 mg	611
Tanezumab 5 mg	606
NSAID	599
Tanezumab 2.5 mg	147
Tanezumab 5 mg	131
Tanezumab 2.5 mg	52
Tanezumab 5 mg	66
NSAID	58
Tanezumab 2.5 mg	7
Tanezumab 5 mg	10
NSAID	11
Tanezumab 2.5 mg	0
Tanezumab 5 mg	3
NSAID	1
Tanezumab 2.5 mg	442
Tanezumab 5 mg	429
NSAID	400
Tanezumab 2.5 mg	92
Tanezumab 5 mg	82
NSAID	107
Tanezumab 2.5 mg	24
Tanezumab 5 mg	35
NSAID	21
Tanezumab 2.5 mg	3
Tanezumab 5 mg	6
NSAID	7
Tanezumab 5 mg	1
NSAID	0
Tanezumab 2.5 mg	351
Tanezumab 5 mg	330
NSAID	338
Tanezumab 2.5 mg	88
Tanezumab 5 mg	90
NSAID	86
Tanezumab 2.5 mg	18
Tanezumab 5 mg	33
NSAID	34
Tanezumab 2.5 mg	1
Tanezumab 5 mg	2
Tanezumab 2.5 mg	308
Tanezumab 5 mg	275
NSAID	315
Tanezumab 2.5 mg	104
Tanezumab 5 mg	96
NSAID	100
Tanezumab 2.5 mg	29
Tanezumab 5 mg	46
Tanezumab 2.5 mg	8
Tanezumab 5 mg	9
NSAID	5

Intervention	Participants (Count of Participants)
Placebo + Diclofenac	9
Tanezumab 2.5 mg + Diclofenac	3
Tanezumab 5 mg + Diclofenac	7
Tanezumab 10 mg + Diclofenac	2

Intervention	units on a scale (Mean)
	Baseline: General Health	Baseline: Physical Function	Baseline: Role Physical	Baseline: Bodily Pain	Baseline: Vitality	Baseline: Social Function	Baseline: Role Emotional	Baseline: Mental Health	Change at Week 12: General Health	Change at Week 12: Physical Function	Change at Week 12: Role Physical	Change at Week 12: Bodily Pain	Change at Week 12: Vitality	Change at Week 12: Social Function	Change at Week 12: Role Emotional	Change at Week 12: Mental Health	Change at Week 24: General Health	Change at Week 24: Physical Function	Change at Week 24: Role Physical	Change at Week 24: Bodily Pain	Change at Week 24: Vitality	Change at Week 24: Social Function	Change at Week 24: Role Emotional	Change at Week 24: Mental Health
Placebo + Diclofenac	46.37	33.51	46.67	32.99	49.08	61.02	68.15	62.80	4.67	7.36	7.61	8.76	3.80	5.02	1.92	3.13	2.41	6.21	5.17	9.14	1.66	4.36	-0.55	1.27
Tanezumab 10 mg + Diclofenac	49.31	36.52	47.46	35.06	51.29	66.55	69.77	65.48	4.96	9.90	8.49	12.76	5.34	4.22	-1.26	1.66	3.08	8.50	5.91	11.52	2.76	1.38	-1.95	0.45
Tanezumab 2.5 mg + Diclofenac	49.41	36.22	47.44	35.66	52.22	67.63	68.96	66.57	5.29	10.96	8.81	12.51	4.23	6.25	2.24	1.55	4.51	8.78	8.41	12.54	2.43	4.09	0.69	2.06
Tanezumab 5 mg + Diclofenac	47.00	34.70	48.50	33.95	53.00	65.83	68.44	64.63	6.55	12.83	7.71	15.18	3.79	4.17	2.17	2.20	4.94	10.50	6.96	13.27	2.58	3.67	-1.33	1.63

Intervention	z-score (Mean)
	Baseline: Physical Component Score	Baseline: Mental Component Score	Change at Week 12: Physical Component Score	Change at Week 12: Mental Component Score	Change at Week 24: Physical Component Score	Change at Week 24: Mental Component Score
Placebo + Diclofenac	-1.84	-0.30	0.35	0.08	0.32	-0.03
Tanezumab 10 mg + Diclofenac	-1.76	-0.15	0.51	-0.06	0.43	-0.14
Tanezumab 2.5 mg + Diclofenac	-1.76	-0.11	0.50	0.01	0.45	-0.03
Tanezumab 5 mg + Diclofenac	-1.80	-0.17	0.56	-0.03	0.50	-0.10

Intervention	units on a scale (Mean)
	Baseline: Index Score	Change at Week 24: Index Score
Placebo + Diclofenac	0.45	0.11
Tanezumab 10 mg + Diclofenac	0.47	0.16
Tanezumab 2.5 mg + Diclofenac	0.48	0.15
Tanezumab 5 mg + Diclofenac	0.47	0.14

Intervention	Participants (Count of Participants)
	AEs	SAEs
Placebo + Diclofenac	53	8
Tanezumab 10 mg + Diclofenac	72	10
Tanezumab 2.5 mg + Diclofenac	71	12
Tanezumab 5 mg + Diclofenac	73	8

Intervention	Participants (Count of Participants)
	Baseline: Mobility-No Dysfunction	Baseline: Mobility-Moderate Dysfunction	Baseline: Mobility-Extreme Dysfunction	Baseline: Self Care-No Dysfunction	Baseline: Self Care-Moderate Dysfunction	Baseline: Self Care-Extreme Dysfunction	Baseline: Usual Activities-No Dysfunction	Baseline: Usual Activities-Moderate Dysfunction	Baseline: Usual Activities-Extreme Dysfunction	Baseline: Pain/Discomfort-No Dysfunction	Baseline: Pain/Discomfort-Moderate Dysfunction	Baseline: Pain/Discomfort-Extreme Dysfunction	Baseline: Anxiety/Depression-No Dysfunction	Baseline: Anxiety/Depression-Moderate Dysfunction	Baseline: Anxiety/Depression-Extreme Dysfunction	Change at Week 24: Mobility-Improved	Change at Week 24: Mobility-No Change	Change at Week 24: Mobility-Worsened	Change at Week 24: Self Care-Improved	Change at Week 24: Self Care-No Change	Change at Week 24: Self Care-Worsened	Change at Week 24: Usual Activities-Improved	Change at Week 24: Usual Activities-No Change	Change at Week 24: Usual Activities-Worsened	Change at Week 24: Pain/Discomfort-Improved	Change at Week 24: Pain/Discomfort-No Change	Change at Week 24: Pain/Discomfort-Worsened	Change at Week 24: Anxiety/Depression-Improved	Change at Week 24: Anxiety/Depression-No Change	Change at Week 24: Anxiety/Depression-Worsened
Placebo + Diclofenac	8	143	1	65	87	0	25	116	11	0	114	38	74	72	6	21	127	4	19	118	15	16	125	11	28	116	8	27	106	19
Tanezumab 10 mg + Diclofenac	10	135	0	52	92	1	18	123	4	1	111	33	73	66	6	25	120	0	30	104	11	27	111	7	33	105	7	19	107	19
Tanezumab 2.5 mg + Diclofenac	7	148	1	61	92	3	13	141	2	0	125	31	82	72	2	25	129	2	33	112	11	27	125	4	29	125	2	26	111	19
Tanezumab 5 mg + Diclofenac	14	136	0	53	96	1	20	126	4	2	115	33	70	75	5	30	114	6	32	110	8	31	106	13	34	109	7	28	109	13

Intervention	Participants (Count of Participants)
	Number of IV Doses: 1	Number of IV Doses: 2	Number of IV Doses: 3
Placebo + Diclofenac	14	38	100
Tanezumab 10 mg + Diclofenac	13	31	101
Tanezumab 2.5 mg + Diclofenac	9	34	114
Tanezumab 5 mg + Diclofenac	15	26	109

Intervention	percentage of participants (Number)
	Week 16: Greater than 0% reduction	Week 16: >=10% reduction	Week 16: >=20% reduction	Week 16: >=30% reduction	Week 16: >=40% reduction	Week 16: >=50% reduction	Week 16: >=60% reduction	Week 16: >=70% reduction	Week 16: >=80% reduction	Week 16: >=90% reduction	Week 16: 100% reduction	Week 24: Greater than 0% reduction	Week 24: >=10% reduction	Week 24: >=20% reduction	Week 24: >=30% reduction	Week 24: >=40% reduction	Week 24: >=50% reduction	Week 24: >=60% reduction	Week 24: >=70% reduction	Week 24: >=80% reduction	Week 24: >=90% reduction	Week 24: 100% reduction
Placebo + Diclofenac	84.2	73.7	61.8	50.0	38.8	30.9	21.7	13.2	5.9	2.0	0.7	81.6	72.4	60.5	48.0	35.5	28.3	20.4	12.5	6.6	3.9	0.7
Tanezumab 10 mg + Diclofenac	84.1	77.9	75.2	66.2	60.7	49.0	31.7	19.3	13.8	6.9	2.8	84.8	75.2	69.7	59.3	51.0	42.1	31.7	21.4	13.8	8.3	2.8
Tanezumab 2.5 mg + Diclofenac	88.5	82.7	69.9	54.5	48.7	35.9	26.3	17.3	9.0	5.8	2.6	82.7	76.9	67.3	58.3	47.4	38.5	26.3	18.6	11.5	8.3	3.8
Tanezumab 5 mg + Diclofenac	88.7	76.7	68.7	61.3	50.7	40.0	28.7	20.0	10.7	6.7	2.0	82.0	74.7	65.3	59.3	47.3	40.0	34.0	22.7	14.7	8.0	3.3

Intervention	days (Median)
	Week 16	Week 24
Placebo + Diclofenac	NA	NA
Tanezumab 10 mg + Diclofenac	NA	NA
Tanezumab 2.5 mg + Diclofenac	NA	NA
Tanezumab 5 mg + Diclofenac	NA	NA

Intervention	mm (Least Squares Mean)
Diclofenac 35 mg Two Times Daily	-35.62
Diclofenac 35 mg Three Times Daily	-41.38
Placebo	-28.14

Intervention	mm (Least Squares Mean)
Diclofenac 35 mg Two Times Daily	-30.25
Diclofenac 35 mg Three Times Daily	-35.86
Placebo	-23.22

Intervention	mm (Least Squares Mean)
Diclofenac 35 mg Two Times Daily	-36.41
Diclofenac 35 mg Three Times Daily	-41.33
Placebo	-30.95

Intervention	mm (Least Squares Mean)
Diclofenac 35 mg Two Times Daily	-39.04
Diclofenac 35 mg Three Times Daily	-44.14
Placebo	-32.46

Intervention	mm (Least Squares Mean)
Diclofenac 35 mg Two Times Daily	-31.40
Diclofenac 35 mg Three Times Daily	-37.42
Placebo	-21.60

Intervention	mm (Least Squares Mean)
Diclofenac 35 mg Two Times Daily	-36.64
Diclofenac 35 mg Three Times Daily	-43.51
Placebo	-31.08

Intervention	units on a scale (Mean)
	Mean score at Week 52/early termination (ET)	Change from baseline to Week 52/ET
Diclofenac 35 mg Capsules	52.3	0.1

Intervention	units on a scale (Mean)
	Mean score at Week 52/early termination (ET)	Mean change from baseline to Week 52/ET
Diclofenac 35 mg Capsules	44.2	4.5

Intervention	participants (Number)
	Subjects with at least 1 TEAE	Subjects with at least 1 severe TEAE	Subjects with at least 1 serious adverse event
Diclofenac 35 mg Capsules	451	41	42

Intervention	participants (Number)
	Subjects without persisitent ALT elevation	Subjects with persistent ALT elevation
Acetaminophen Arm	204	1
Placebo Arm	47	0