alendronate and Hangman Fracture studies

alendronic acid : A 1,1-bis(phosphonic acid) that is methanebis(phosphonic acid) in which the two methylene hydrogens are replaced by hydroxy and 3-aminopropyl groups.

Research Excerpts

Excerpt	Relevance	Reference
"In this randomized, controlled trial, sequential therapy with once-weekly subcutaneous injection of teriparatide for 72 weeks, followed by alendronate for 48 weeks resulted in a significantly lower incidence of morphometric vertebral fracture than monotherapy with alendronate for 120 weeks in women with osteoporosis at high risk of fracture."	9.69	Sequential therapy with once-weekly teriparatide injection followed by alendronate versus monotherapy with alendronate alone in patients at high risk of osteoporotic fracture: final results of the Japanese Osteoporosis Intervention Trial-05. ( Hagino, H; Mitomo, Y; Mori, S; Nakamura, T; Soen, S; Sone, T; Sugimoto, T; Takahashi, K; Tanaka, S, 2023)
"In this randomized, controlled trial, treatment with once-weekly subcutaneous injection of teriparatide for 72 weeks was found to be associated with a significant reduction in the incidence of morphometric vertebral fractures compared with alendronate in women with primary osteoporosis who were at high risk of fracture."	9.41	A randomized, controlled trial of once-weekly teriparatide injection versus alendronate in patients at high risk of osteoporotic fracture: primary results of the Japanese Osteoporosis Intervention Trial-05. ( Hagino, H; Mori, S; Nakamura, T; Sasaki, K; Soen, S; Sone, T; Sugimoto, T; Tanaka, S, 2021)
"Glucocorticoid-induced osteoporosis (GIOP) is the most common secondary osteoporosis, alendronate (ALE) and teriparatide (TPTD) are widely used in the treatment of GIOP."	9.22	The efficiency and safety of alendronate versus teriparatide for treatment glucocorticoid-induced osteoporosis: A meta-analysis and systematic review of randomized controlled trials. ( Guan, XQ; Liu, ZM; Shen, ZB; Yin, F; Zhang, D; Zhang, M; Zong, Y, 2022)
"A 3-year, randomized, double-blind, placebo-controlled trial evaluated the effect of oral alendronate on the BMD of 64 adult patients with osteogenesis imperfecta."	9.12	Effects of oral alendronate on BMD in adult patients with osteogenesis imperfecta: a 3-year randomized placebo-controlled trial. ( Arlot, M; Charrin, JE; Chevrel, G; Duboeuf, F; Fontanges, E; Garnero, P; Lina-Granade, G; Meunier, PJ; Raynal, C; Schott, AM, 2006)
"Our trial was a 3-year, open-label, prospective, comparative, clinical study comparing the effects of oral alendronate (ALN), 10 mg daily, and alfacalcidol (AC), 1 microg daily, on bone mineral density (BMD), fracture events, height, back pain, safety and tolerability in 134 men with established primary osteoporosis."	9.11	Alendronate treatment of established primary osteoporosis in men: 3-year results of a prospective, comparative, two-arm study. ( Dorst, A; Faber, H; Ibach, K; Ringe, JD, 2004)
"The purpose of the present study was to compare the effects of treatment with etidronate and alendronate on bone resorption, back pain, and activities of daily living (ADL) in elderly women with vertebral fractures."	9.10	Comparative effects of treatment with etidronate and alendronate on bone resorption, back pain, and activities of daily living in elderly women with vertebral fractures. ( Ichimura, S; Iwamoto, J; Takeda, T; Uzawa, M, 2003)
" Eighteen GHD patients with osteoporosis were randomized to continue their rhGH maintenance dose or to receive combination therapy with rhGH and alendronate for 12 months."	9.09	Additional beneficial effects of alendronate in growth hormone (GH)-deficient adults with osteoporosis receiving long-term recombinant human GH replacement therapy: a randomized controlled trial. ( Biermasz, NR; Hamdy, NA; Janssen, YJ; Roelfsema, F, 2001)
"In a two-year double-blind trial, we studied the effect of 10 mg of alendronate or placebo, given daily, on bone mineral density in 241 men (age, 31 to 87 years; mean, 63) with osteoporosis."	9.09	Alendronate for the treatment of osteoporosis in men. ( Adami, S; Ettinger, M; Graham, J; Kendler, D; Lombardi, A; Lorenc, R; Miller, P; Orwoll, E; Pietschmann, P; Vandormael, K; Weber, K; Weiss, S, 2000)
"To determine the effect of alendronate therapy on days affected by back pain in postmenopausal women with existing vertebral fractures."	9.09	Effect of alendronate on limited-activity days and bed-disability days caused by back pain in postmenopausal women with existing vertebral fractures. Fracture Intervention Trial Research Group. ( Black, DM; Cummings, SR; Ensrud, K; Nevitt, MC; Rubin, SR; Thompson, DE; Yates, AJ, 2000)
"From January 2018 to January 2020, we recruited 165 female osteoporosis patients after percutaneous vertebroplasty who were assigned into sequential treatment of teriparatide followed by alendronate group (TPTD + ALN group) and alendronate alone group (ALN group)."	8.31	Sequential treatment of teriparatide and alendronate versus alendronate alone for elevation of bone mineral density and prevention of refracture after percutaneous vertebroplasty in osteoporosis: a prospective study. ( Han, W; Huang, K; Long, Y; Tan, J; Wang, M; Yang, D; Yi, W; Zeng, S; Zhu, S, 2023)
"A retrospective study was performed to evaluate the outcome of alendronate treatment for 7 years among Japanese men with osteoporosis or osteopenia and clinical risk factors for fractures."	7.83	Experience with alendronate treatment for 7 years among Japanese men with osteoporosis or osteopenia and clinical risk factors for fractures. ( Iwamoto, J; Uzawa, M, 2016)
"Alendronate therapy was well tolerated and produced a significantly greater increase in BMD over 12 months compared with placebo."	6.73	Alendronate once weekly for the prevention and treatment of bone loss in Canadian adult cystic fibrosis patients (CFOS trial). ( Adachi, JD; Berthiaume, Y; Freitag, A; Ioannidis, G; Jeanneret, A; Kennedy, CC; Matouk, E; Nixon, M; O'Neill, J; Papaioannou, A; Paterson, N; Pui, M; Rabin, HR; Villeneuve, J; Webber, C, 2008)
"Osteoporosis is a common complication of long-term glucocorticoid therapy for which there is no well-proved preventive or restorative treatment."	6.69	Alendronate for the prevention and treatment of glucocorticoid-induced osteoporosis. Glucocorticoid-Induced Osteoporosis Intervention Study Group. ( Brown, JP; Czachur, M; Daifotis, AG; Delmas, PD; Emkey, R; Goemaere, S; Hawkins, F; Liberman, UA; Malice, MP; Saag, KG; Schnitzer, TJ; Thamsborg, G, 1998)
"Alendronate has demonstrated its ability to increase bone mass significantly above the placebo values at any studied skeletal site in a wide variety of patient subgroups regardless of age, race, baseline rate of bone turnover or baseline bone mineral density."	6.40	A risk-benefit assessment of alendronate in the treatment of involutional osteoporosis. ( Devogelaer, JP, 1998)
"In this randomized, controlled trial, sequential therapy with once-weekly subcutaneous injection of teriparatide for 72 weeks, followed by alendronate for 48 weeks resulted in a significantly lower incidence of morphometric vertebral fracture than monotherapy with alendronate for 120 weeks in women with osteoporosis at high risk of fracture."	5.69	Sequential therapy with once-weekly teriparatide injection followed by alendronate versus monotherapy with alendronate alone in patients at high risk of osteoporotic fracture: final results of the Japanese Osteoporosis Intervention Trial-05. ( Hagino, H; Mitomo, Y; Mori, S; Nakamura, T; Soen, S; Sone, T; Sugimoto, T; Takahashi, K; Tanaka, S, 2023)
"To assess the effectiveness and safety of denosumab (Prolia®) compared to bisphosphonates (alendronate, ibandronate, risedronate, zoledronate), selective estrogen receptor modulators (SERMs; bazedoxifene, raloxifene) or placebo, for the treatment of osteoporosis in postmenopausal women (PMW)."	5.41	The Clinical Effectiveness of Denosumab (Prolia®) for the Treatment of Osteoporosis in Postmenopausal Women, Compared to Bisphosphonates, Selective Estrogen Receptor Modulators (SERM), and Placebo: A Systematic Review and Network Meta-Analysis. ( Jenal, M; Ma, N; Moshi, MR; Nicolopoulos, K; Stringer, D; Vreugdenburg, T, 2023)
"Bisphosphonates, denosumab, abaloparatide, teriparatide, and romosozumab, followed by alendronate, reduce clinical fractures in postmenopausal females with osteoporosis."	5.41	Effectiveness and Safety of Treatments to Prevent Fractures in People With Low Bone Mass or Primary Osteoporosis: A Living Systematic Review and Network Meta-analysis for the American College of Physicians. ( Ayers, C; Fu, R; Harrod, C; Kansagara, D; Kwon, A; Lazur, B, 2023)
"This study assessed the effectiveness and safety of denosumab (Prolia®) compared to bisphosphonates (alendronate, ibandronate, risedronate, zoledronate), selective estrogen receptor modulators (SERMs) (bazedoxifene, raloxifene) and placebo for the treatment of osteoporosis in hormone-sensitive cancer patients receiving endocrine therapy (men with prostate cancer [MPC] on hormone ablation therapy [HAT], and women with breast cancer [WBC] on adjuvant aromatase inhibitor therapy [AAIT])."	5.41	The clinical effectiveness of denosumab (Prolia®) in patients with hormone-sensitive cancer receiving endocrine therapy, compared to bisphosphonates, selective estrogen receptor modulators (SERM), and placebo: a systematic review and network meta-analysis ( Jenal, M; Ma, N; Moshi, MR; Nicolopoulos, K; Stringer, D; Vreugdenburg, T, 2023)
"In this randomized, controlled trial, treatment with once-weekly subcutaneous injection of teriparatide for 72 weeks was found to be associated with a significant reduction in the incidence of morphometric vertebral fractures compared with alendronate in women with primary osteoporosis who were at high risk of fracture."	5.41	A randomized, controlled trial of once-weekly teriparatide injection versus alendronate in patients at high risk of osteoporotic fracture: primary results of the Japanese Osteoporosis Intervention Trial-05. ( Hagino, H; Mori, S; Nakamura, T; Sasaki, K; Soen, S; Sone, T; Sugimoto, T; Tanaka, S, 2021)
" Among patients with osteoporosis in Taiwan who had experienced a fracture and had started alendronate therapy, compliance with the dosage regimen was suboptimal."	5.37	Alendronate adherence and its impact on hip-fracture risk in patients with established osteoporosis in Taiwan. ( Lin, SJ; Lin, TC; Yang, CY; Yang, YH, 2011)
"Glucocorticoid-induced osteoporosis (GIOP) is the most common secondary osteoporosis, alendronate (ALE) and teriparatide (TPTD) are widely used in the treatment of GIOP."	5.22	The efficiency and safety of alendronate versus teriparatide for treatment glucocorticoid-induced osteoporosis: A meta-analysis and systematic review of randomized controlled trials. ( Guan, XQ; Liu, ZM; Shen, ZB; Yin, F; Zhang, D; Zhang, M; Zong, Y, 2022)
"The fracture intervention trial is a large randomized, placebo-controlled trial of alendronate treatment for osteoporosis."	5.17	Natural history and risk factors for adjacent vertebral fractures in the fracture intervention trial. ( Bauer, DC; Frankel, B; Krishna, V; Nicholas, J; Vandergrift, A, 2013)
"A 3-year, randomized, double-blind, placebo-controlled trial evaluated the effect of oral alendronate on the BMD of 64 adult patients with osteogenesis imperfecta."	5.12	Effects of oral alendronate on BMD in adult patients with osteogenesis imperfecta: a 3-year randomized placebo-controlled trial. ( Arlot, M; Charrin, JE; Chevrel, G; Duboeuf, F; Fontanges, E; Garnero, P; Lina-Granade, G; Meunier, PJ; Raynal, C; Schott, AM, 2006)
"Our trial was a 3-year, open-label, prospective, comparative, clinical study comparing the effects of oral alendronate (ALN), 10 mg daily, and alfacalcidol (AC), 1 microg daily, on bone mineral density (BMD), fracture events, height, back pain, safety and tolerability in 134 men with established primary osteoporosis."	5.11	Alendronate treatment of established primary osteoporosis in men: 3-year results of a prospective, comparative, two-arm study. ( Dorst, A; Faber, H; Ibach, K; Ringe, JD, 2004)
"The purpose of this open-labeled prospective study was to compare the treatment effects of cyclical etidronate and alendronate on the lumbar bone mineral density (BMD), bone resorption, and back pain in elderly women with osteoporosis."	5.11	Comparison of effect of treatment with etidronate and alendronate on lumbar bone mineral density in elderly women with osteoporosis. ( Iwamoto, J; Sato, Y; Takeda, T; Uzawa, M, 2005)
"The purpose of the present study was to compare the effects of treatment with etidronate and alendronate on bone resorption, back pain, and activities of daily living (ADL) in elderly women with vertebral fractures."	5.10	Comparative effects of treatment with etidronate and alendronate on bone resorption, back pain, and activities of daily living in elderly women with vertebral fractures. ( Ichimura, S; Iwamoto, J; Takeda, T; Uzawa, M, 2003)
"The purpose of the present study was to examine the early response of lumbar bone mineral density (BMD), bone resorption, and back pain to alendronate after treatment with cyclical etidronate in postmenopausal women with osteoporosis."	5.10	Early response to alendronate after treatment with etidronate in postmenopausal women with osteoporosis. ( Ichimura, S; Iwamoto, J; Takeda, T; Uzawa, M, 2003)
" Eighteen GHD patients with osteoporosis were randomized to continue their rhGH maintenance dose or to receive combination therapy with rhGH and alendronate for 12 months."	5.09	Additional beneficial effects of alendronate in growth hormone (GH)-deficient adults with osteoporosis receiving long-term recombinant human GH replacement therapy: a randomized controlled trial. ( Biermasz, NR; Hamdy, NA; Janssen, YJ; Roelfsema, F, 2001)
"In a two-year double-blind trial, we studied the effect of 10 mg of alendronate or placebo, given daily, on bone mineral density in 241 men (age, 31 to 87 years; mean, 63) with osteoporosis."	5.09	Alendronate for the treatment of osteoporosis in men. ( Adami, S; Ettinger, M; Graham, J; Kendler, D; Lombardi, A; Lorenc, R; Miller, P; Orwoll, E; Pietschmann, P; Vandormael, K; Weber, K; Weiss, S, 2000)
"To determine the effect of alendronate therapy on days affected by back pain in postmenopausal women with existing vertebral fractures."	5.09	Effect of alendronate on limited-activity days and bed-disability days caused by back pain in postmenopausal women with existing vertebral fractures. Fracture Intervention Trial Research Group. ( Black, DM; Cummings, SR; Ensrud, K; Nevitt, MC; Rubin, SR; Thompson, DE; Yates, AJ, 2000)
"Minodronate has better clinical efficacy in the treatment of osteoporosis than other drugs (alendronate, risedronate, raloxifene, or eldecalcitol)."	5.05	Minodronate in the treatment of osteoporosis: A systematic review and meta-analysis. ( Chen, D; Huang, X; Jin, Z; Liu, Q; Ma, T; Ye, Z, 2020)
" Alendronate effects were also prospectively assessed using CT/FEM in 33 patients with postmenopausal osteoporosis who were treated with alendronate at a dose of 5 mg/day for 1 year."	4.85	[Prediction of vertebral strength using a CT based finite element method--clinical application in evaluation of the efficacy of alendronate]. ( Ohnishi, I, 2009)
"According to the data of a fracture intervention trial, in women aged 55-80 years with vertebral fractures or osteoporosis diagnosed by bone mineral density measurement, treatment with the bisphosphonate alendronate prevented hip fractures with numbers-needed-to-treat within 5 years of treatment of 46 and 66, respectively."	4.81	[Bisphosphonate treatment prevents hip fractures in 70-79 year old women with osteoporotic vertebral fractures]. ( Netelenbos, JC, 2001)
"From January 2018 to January 2020, we recruited 165 female osteoporosis patients after percutaneous vertebroplasty who were assigned into sequential treatment of teriparatide followed by alendronate group (TPTD + ALN group) and alendronate alone group (ALN group)."	4.31	Sequential treatment of teriparatide and alendronate versus alendronate alone for elevation of bone mineral density and prevention of refracture after percutaneous vertebroplasty in osteoporosis: a prospective study. ( Han, W; Huang, K; Long, Y; Tan, J; Wang, M; Yang, D; Yi, W; Zeng, S; Zhu, S, 2023)
" Conservative treatment was conducted using a soft lumbosacral orthosis plus osteoporosis drugs, either weekly alendronate (bisphosphonate) or daily teriparatide."	3.96	Is Bone Nonunion, Vertebral Deformity, or Spinopelvic Malalignment the Best Therapeutic Target for Amelioration of Low Back Pain After Osteoporotic Vertebral Fracture? ( Hashimoto, T; Iwasaki, N; Iwata, A; Kanayama, M; Oha, F; Shimamura, Y; Takahata, M, 2020)
" Alendronate treatment increases bone mass and reduces the risk of fractures in patients with osteoporosis by suppressing bone resorption."	3.85	Risk of long-term infection-related death in clinical osteoporotic vertebral fractures: A hospital-based analysis. ( Chen, YC; Lin, WC, 2017)
"A retrospective study was performed to evaluate the outcome of alendronate treatment for 7 years among Japanese men with osteoporosis or osteopenia and clinical risk factors for fractures."	3.83	Experience with alendronate treatment for 7 years among Japanese men with osteoporosis or osteopenia and clinical risk factors for fractures. ( Iwamoto, J; Uzawa, M, 2016)
" Alendronate, risedronate, zoledronate and denosumab have been shown to prevent spine, nonspine and hip fractures; in addition, teriparatide and strontium ranelate prevent both spine and nonspine fractures, and raloxifene and ibandronate prevent spine fractures."	3.81	Efficacy, effectiveness and side effects of medications used to prevent fractures. ( Reid, IR, 2015)
"While alendronate inhibits atherosclerosis experimentally, its effect on lower limb ischemia risk is unknown."	3.80	Alendronate and risk of lower limb ischemic vascular events: a population-based cohort study. ( Chang, HL; Chang, HT; Chen, CK; Chen, TJ; Chen, YC; Chou, HP; Huang, YC; Lee, MH; Shih, CC, 2014)
"Treatment with alendronate was associated with significantly greater improvements in lumbar spine BMD within one year in breast cancer survivors when compared with treatment with cyclic etidronate or calcium and vitamin D."	3.73	Are oral bisphosphonates effective in improving lumbar bone mineral density in breast cancer survivors with osteopenia or osteoporosis? ( Adachi, JD; Boulos, P; Brown, JP; Goldsmith, CH; Hanley, DA; Ioannidis, G; Josse, RG; Kouroukis, T; Murray, TM; Olszynski, WP; Papaioannou, A; Petrie, A; Sawka, AM; Sebaldt, RJ; Tenenhouse, A; Thabane, L, 2005)
" Etidronate and alendronate are most cost effective in women with borderline osteoporosis (t scores of -1."	3.72	A cost effectiveness analysis of calcium and vitamin D supplementation, etidronate, and alendronate in the prevention of vertebral fractures in women treated with glucocorticoids. ( Buckley, LM; Hillner, BE, 2003)
"Osteoporosis is a disorder of bone mineralisation occurring in about one third of adults with cystic fibrosis."	3.01	Bisphosphonates for osteoporosis in people with cystic fibrosis. ( Chang, AB; Conwell, LS; Jeffery, TC, 2023)
"In women with postmenopausal osteoporosis, we investigated the effects of 24 months of treatment with alendronate (ALN) following 18 months of treatment with abaloparatide (ABL) or placebo (PBO)."	2.87	ACTIVExtend: 24 Months of Alendronate After 18 Months of Abaloparatide or Placebo for Postmenopausal Osteoporosis. ( Bilezikian, JP; Bone, HG; Cosman, F; Dore, RK; Fitzpatrick, LA; Hattersley, G; Hu, MY; Miller, PD; Mitlak, B; Papapoulos, S; Rizzoli, R; Saag, KG; Williams, GC, 2018)
"Alendronate therapy was well tolerated and produced a significantly greater increase in BMD over 12 months compared with placebo."	2.73	Alendronate once weekly for the prevention and treatment of bone loss in Canadian adult cystic fibrosis patients (CFOS trial). ( Adachi, JD; Berthiaume, Y; Freitag, A; Ioannidis, G; Jeanneret, A; Kennedy, CC; Matouk, E; Nixon, M; O'Neill, J; Papaioannou, A; Paterson, N; Pui, M; Rabin, HR; Villeneuve, J; Webber, C, 2008)
"Alendronate-treated women with at least a 30% reduction in bone ALP had a lower risk of non-spine (RH = 0."	2.71	Change in bone turnover and hip, non-spine, and vertebral fracture in alendronate-treated women: the fracture intervention trial. ( Bauer, DC; Black, DM; Delmas, PD; Ewing, SK; Garnero, P; Hochberg, M; Orloff, J; Ott, S; Thompson, DE, 2004)
"Alendronate is an effective, well-tolerated therapy for the prevention and treatment of glucocorticoid-induced osteoporosis, with sustained treatment advantages for up to 2 years."	2.70	Two-year effects of alendronate on bone mineral density and vertebral fracture in patients receiving glucocorticoids: a randomized, double-blind, placebo-controlled extension trial. ( Adachi, JD; Block, JA; Brown, J; Carofano, W; Correa-Rotter, R; Czachur, M; Daifotis, A; Delmas, PD; Dumortier, T; Emkey, RD; Gruber, BL; Hawkins, F; Kaufman, JM; Lane, NE; Leite, MO; Liberman, UA; Malice, MP; McIlwain, HH; Melo-Gomes, JA; Menkes, CJ; Nevitt, MC; Poubelle, PE; Rodriguez-Portales, JA; Saag, KG; Schnitzer, TJ; Seeman, E; Sharp, JT; Siminoski, KG; Westhovens, R; Wing, J; Yanover, MJ, 2001)
"Treatment with alendronate, 10 mg daily, significantly increased BMD in patients with Crohn's disease and was safe and well tolerated."	2.69	Alendronate increases lumbar spine bone mineral density in patients with Crohn's disease. ( Haderslev, KV; Sorensen, HA; Staun, M; Tjellesen, L, 2000)
"Osteoporosis is a common complication of long-term glucocorticoid therapy for which there is no well-proved preventive or restorative treatment."	2.69	Alendronate for the prevention and treatment of glucocorticoid-induced osteoporosis. Glucocorticoid-Induced Osteoporosis Intervention Study Group. ( Brown, JP; Czachur, M; Daifotis, AG; Delmas, PD; Emkey, R; Goemaere, S; Hawkins, F; Liberman, UA; Malice, MP; Saag, KG; Schnitzer, TJ; Thamsborg, G, 1998)
"Postmenopausal osteoporosis is a serious health problem, and additional treatments are needed."	2.68	Effect of oral alendronate on bone mineral density and the incidence of fractures in postmenopausal osteoporosis. The Alendronate Phase III Osteoporosis Treatment Study Group. ( Bell, NH; Bröll, J; Dequeker, J; Downs, RW; Favus, M; Liberman, UA; Minne, HW; Quan, H; Rodriguez-Portales, J; Weiss, SR, 1995)
" Glucocorticoid (GC) dosage (P = ."	2.66	Meta-regression analysis of the efficacy of alendronate for prevention of glucocorticoid-induced fractures. ( Ding, L; Huang, H; Li, K; Lin, J; Qiu, M; Zhang, M, 2020)
"In women with osteopenia or osteoporosis, 6 years of zoledronic acid reduced clinical fractures (HR, 0."	2.61	Long-Term Drug Therapy and Drug Discontinuations and Holidays for Osteoporosis Fracture Prevention: A Systematic Review. ( Brasure, M; Butler, M; Ensrud, KE; Fink, HA; Forte, ML; MacDonald, R; Nelson, VA; Olson, CM; Rosebush, CE; Schousboe, JT; Taylor, BC; Ullman, K; Wilt, TJ, 2019)
"Many drugs for the treatment of osteoporosis have also been associated with increased risks of serious adverse events."	2.52	Osteoporosis: the emperor has no clothes. ( Aspenberg, P; Järvinen, TL; Michaëlsson, K; Sievänen, H, 2015)
"Alendronate effects were also prospectively assessed in 33 patients with postmenopausal osteoporosis who were treated with alendronate at a dose of 5 mg/day for 18 months."	2.47	Vertebral fracture risk and alendronate effects on osteoporosis assessed by a computed tomography-based nonlinear finite element method. ( Imai, K, 2011)
"Osteoporosis is a systemic skeletal disorder characterized by low bone mass and microarchitectural deterioration of bone tissue resulting in compromised bone strength and an increased risk of fracture."	2.44	Nonvertebral fracture risk reduction with nitrogen-containing bisphosphonates. ( Hochberg, MC, 2008)
"Alendronate has been found to reduce the risk of fractures in postmenopausal women as demonstrated in multiple randomized controlled trials enrolling thousands of women."	2.43	Does alendronate reduce the risk of fracture in men? A meta-analysis incorporating prior knowledge of anti-fracture efficacy in women. ( Adachi, JD; Gafni, A; Hanley, DA; Papaioannou, A; Sawka, AM; Thabane, L, 2005)
"The main goal of postmenopausal osteoporosis treatment is to reduce the risk of fragility fractures."	2.43	[Osteoporosis: Optimizing treatment strategy]. ( Thomas, T, 2006)
"In 2002, Adequate Treatment of Osteoporosis (A-TOP) Research Group was organized to obtain the evidence for treatment of osteoporosis in Japan."	2.43	[Current research in adequate treatment by Osteoporosis Research Group]. ( Kuroda, T; Miyakawa, N; Orimo, H, 2006)
"Osteoporosis affects postmenopausal women and patients on glucocorticoid therapy."	2.43	Rapid prevention of vertebral fractures associated with osteoporosis. ( Wallace, DJ, 2005)
"Alendronate has been approved for treatment of osteoporosis in men, and other treatments for men are under evaluation."	2.41	Osteoporosis in elderly: prevention and treatment. ( Deal, C; Srivastava, M, 2002)
" In addition, alendronate was shown to have no adverse effects on bone mineralization or microstructure."	2.40	Alendronate for osteoporosis. Safe and efficacious nonhormonal therapy. ( Adachi, JD, 1998)
"Alendronate has demonstrated its ability to increase bone mass significantly above the placebo values at any studied skeletal site in a wide variety of patient subgroups regardless of age, race, baseline rate of bone turnover or baseline bone mineral density."	2.40	A risk-benefit assessment of alendronate in the treatment of involutional osteoporosis. ( Devogelaer, JP, 1998)
"Alendronate was ineffective to avoid spontaneous clinical vertebral fractures."	1.51	Alendronate after denosumab discontinuation in women previously exposed to bisphosphonates was not effective in preventing the risk of spontaneous multiple vertebral fractures: two case reports. ( Aguado, P; Aubry-Rozier, B; Benavent-Núñez, D; Fernández-Fernández, E; Gonzalez-Rodriguez, E; Lamy, O; Monjo-Henry, I; Stoll, D, 2019)
" Among patients with osteoporosis in Taiwan who had experienced a fracture and had started alendronate therapy, compliance with the dosage regimen was suboptimal."	1.37	Alendronate adherence and its impact on hip-fracture risk in patients with established osteoporosis in Taiwan. ( Lin, SJ; Lin, TC; Yang, CY; Yang, YH, 2011)
"Alendronate-treated patients are at higher risk of hip and subtrochanteric/diaphyseal fracture than matched control subjects."	1.36	Cumulative alendronate dose and the long-term absolute risk of subtrochanteric and diaphyseal femur fractures: a register-based national cohort analysis. ( Abrahamsen, B; Eastell, R; Eiken, P, 2010)
"Treatment with alendronate could lead to a significant reduction in fracture risk in MGUS patients with skeletal fragility."	1.35	The effects of alendronate treatment in osteoporotic patients affected by monoclonal gammopathy of undetermined significance. ( Fassino, V; Mascia, ML; Minisola, S; Pepe, J; Petrucci, MT; Piemonte, S; Romagnoli, E, 2008)
"Alendronate effects were detected at 3 months, and marked bone density increases were noted in juxta-cortical areas compared to inner trabecular areas."	1.35	Assessment of vertebral fracture risk and therapeutic effects of alendronate in postmenopausal women using a quantitative computed tomography-based nonlinear finite element method. ( Imai, K; Matsumoto, T; Nakamura, K; Ohnishi, I; Yamamoto, S, 2009)
"Systemic mastocytosis is a rare but well-recognised cause of secondary osteoporosis, accounting for about 1."	1.35	Systemic mastocytosis presenting as osteoporosis--a case report. ( Dhillon, V; Mathew, R; Shepherd, P, 2009)
"Treatment with alendronate (Fosamax) has been shown to significantly reduce the risk of fragility fractures."	1.34	Cost-effectiveness of alendronate in the treatment of postmenopausal women in 9 European countries--an economic evaluation based on the fracture intervention trial. ( Boonen, S; Borgström, F; Haentjens, P; Johnell, O; Kanis, JA; Sen, SS; Ström, O, 2007)
"Alendronate has been studied extensively by large trials of high quality and its efficacy to reduce the risk of vertebral and nonvertebral fractures is in line with the criteria of evidence-based medicine."	1.33	[Drug therapy for prevention of falls and fractures]. ( Ringe, JD, 2006)
"To investigate the cost-effectiveness of universal bone densitometry in women aged 65 and older combined with alendronate treatment for those diagnosed with osteoporosis (femoral neck T-score < or = -2."	1.33	Universal bone densitometry screening combined with alendronate therapy for those diagnosed with osteoporosis is highly cost-effective for elderly women. ( Ensrud, KE; Kane, RL; Melton, LJ; Nyman, JA; Schousboe, JT, 2005)
"A total of 1,041 postmenopausal osteoporosis cases were classified into 4 categories, Young controls (n = 165) and Old controls (n = 95) (Control group), Young (n = 309) and Old osteoporosis (n = 110) treated with alendronate (ALN group), and Young (n = 238) and Old osteoporosis (n = 124) treated with vitamins D3 or K2 (VDK group)."	1.33	[Very old patients with osteoporosis should be treated with alendronate]. ( Shiraki, M, 2006)
"Alendronate was significantly more effective than risedronate, calcitonin, estrogen, etidronate, and raloxifene (Relative Risks: 0."	1.32	Putting evidence-based medicine into clinical practice: comparing anti-resorptive agents for the treatment of osteoporosis. ( Hochberg, MC; Hosking, D; Wehren, LE, 2004)
"Male osteoporosis is an important disease, with 25-30% of all hip fractures occurring in men."	1.32	An investigation of the predictors of bone mineral density and response to therapy with alendronate in osteoporotic men. ( Drake, WM; Kendler, DL; Orwoll, ES; Rosen, CJ, 2003)
"Up to 80-90% of patients with treatment-requiring osteoporosis are not receiving specific treatment."	1.31	[Weeks of pain, vertebral body fractures during sleep, invalidism. Save your osteoporosis patients from this fate]. ( Begerow, B; Hinz, C; Minne, HW; Pfeifer, M; Pollähne, W, 2002)
"A case review of postmenopausal osteoporosis is presented in the context of recent literature in the field."	1.31	Osteoporotic fractures in older women. ( Elliott, ME, 2002)
" The drug should be absorbed after an overnight fast to improve its bioavailability and with a big glass of plain water to reduce the risk of oesophageal ulcerations."	1.30	[Drug clinics. The drug of the month. Alendronate (Fosamax)]. ( Scheen, AJ, 1998)

Research

Studies (175)

Authors

Clinical Trials (20)

Trial Overview

Trial Outcomes

Number of Participants With New Vertebral Fractures at 18 Months

Number of Participants With Non-vertebral Fractures at 18 Months

Number of Treatment-Emergent Adverse Events Associated With Hypercalcemia at 18 Months

Percent Change in Bone Mineral Density (BMD) of Femoral Neck From Baseline to Month 18

Percent Change in Bone Mineral Density (BMD) of Lumbar Spine From Baseline to 18 Months

Percent Change in Bone Mineral Density (BMD) of Total Hip From Baseline to Month 18

Kaplan-Meier Estimated Event Rate of the First Incident of Nonvertebral Fracture Since Study BA058-05-003 Baseline (Data From Studies BA058-05-005 and BA058-05-003 Combined)

Timeframe	Studies, this research(%)	All Research%
pre-1990	0 (0.00)	18.7374
1990's	18 (10.29)	18.2507
2000's	101 (57.71)	29.6817
2010's	35 (20.00)	24.3611
2020's	21 (12.00)	2.80

Authors	Studies
Liu, ZM	1
Zhang, M	2
Zong, Y	2
Zhang, D	1
Shen, ZB	1
Guan, XQ	1
Yin, F	1
Li, P	1
Wu, X	1
Li, Y	1
Huang, J	1
Mori, S	2
Hagino, H	3
Sugimoto, T	2
Tanaka, S	2
Mitomo, Y	1
Takahashi, K	1
Sone, T	2
Nakamura, T	5
Soen, S	4
Ayers, C	1
Kansagara, D	1
Lazur, B	1
Fu, R	1
Kwon, A	1
Harrod, C	1
Tutaworn, T	1
Nieves, JW	1
Wang, Z	1
Levin, JE	1
Yoo, JE	1
Lane, JM	1
Nicolopoulos, K	2
Moshi, MR	2
Stringer, D	2
Ma, N	2
Jenal, M	2
Vreugdenburg, T	2
Jeffery, TC	1
Chang, AB	1
Conwell, LS	1
Yang, D	1
Tan, J	1
Long, Y	1
Huang, K	1
Han, W	1
Wang, M	1
Zhu, S	1
Zeng, S	1
Yi, W	1
Gharanizadeh, K	1
Ravanbod, H	1
Aminian, A	1
Hatami, S	1
Chaleshtori, AS	1
Kazerani, S	1
Everts-Graber, J	1
Bonel, H	1
Lehmann, D	1
Gahl, B	1
Häuselmann, H	1
Studer, U	1
Ziswiler, HR	1
Reichenbach, S	1
Lehmann, T	1
Koiwai, H	1
Kamimura, M	1
Takahashi, J	1
Nakamura, Y	1
Kato, H	1
Leder, BZ	1
Mitlak, B	2
Hu, MY	3
Hattersley, G	3
Bockman, RS	1
Iwata, A	2
Kanayama, M	2
Oha, F	2
Shimamura, Y	1
Hashimoto, T	2
Takahata, M	1
Iwasaki, N	2
Liu, Q	1
Chen, D	1
Ye, Z	1
Jin, Z	1
Ma, T	1
Huang, X	1
Qiu, M	1
Ding, L	1
Lin, J	1
Huang, H	1
Li, K	1
Ouyang, Y	1
Chen, S	1
Wan, T	1
Zheng, G	1
Sun, G	1
Gou, PG	1
Zhao, ZH	1
Zhou, JM	1
Ren, LH	1
Wang, XY	1
Mu, YF	1
Wang, YG	1
Chang, F	1
Xue, Y	2
Mori, T	1
Crandall, CJ	1
Fujii, T	1
Ganz, DA	1
Sasaki, K	1
Grassi, G	1
Chiodini, I	1
Palmieri, S	1
Cairoli, E	1
Arosio, M	1
Eller-Vainicher, C	1
Albert, SG	1
Reddy, S	1
Chen, YC	3
Lin, WC	1
Hsu, E	1
Nanes, M	1
Saag, KG	5
Petersen, J	1
Brandi, ML	1
Karaplis, AC	1
Lorentzon, M	1
Thomas, T	3
Maddox, J	1
Fan, M	1
Meisner, PD	1
Grauer, A	1
Bone, HG	2
Cosman, F	2
Miller, PD	2
Williams, GC	2
Fitzpatrick, LA	2
Papapoulos, S	1
Rizzoli, R	1
Dore, RK	1
Bilezikian, JP	2
Wang, Y	1
Jia, G	1
Song, J	1
Kong, X	1
Zhang, W	1
Meng, C	1
Lamy, O	2
Fernández-Fernández, E	1
Monjo-Henry, I	1
Stoll, D	1
Aubry-Rozier, B	1
Benavent-Núñez, D	1
Aguado, P	1
Gonzalez-Rodriguez, E	1
Bandeira, F	1
Torres, G	1
Bandeira, E	1
Duarte, MB	1
Nóbrega, AM	1
Bandeira, L	1
Fink, HA	2
MacDonald, R	1
Forte, ML	1
Rosebush, CE	1
Ensrud, KE	10
Schousboe, JT	6
Nelson, VA	1
Ullman, K	1
Butler, M	1
Olson, CM	1
Taylor, BC	1
Brasure, M	1
Wilt, TJ	1
Ikeda, S	1
Nakamura, E	1
Narusawa, K	1
Fukuda, F	1
Matsumoto, H	1
Nakai, K	1
Sakata, T	1
Yoshioka, T	1
Fujino, Y	1
Sakai, A	1
Chen, CK	1
Chang, HT	1
Chou, HP	1
Lee, MH	1
Huang, YC	1
Chen, TJ	1
Chang, HL	1
Shih, CC	1
Serrano, AJ	1
Begoña, L	1
Anitua, E	1
Cobos, R	1
Orive, G	1
Frankel, B	1
Krishna, V	1
Vandergrift, A	1
Bauer, DC	9
Nicholas, J	1
Messori, A	1
Fadda, V	1
Maratea, D	1
Trippoli, S	1
Marinai, C	1
Iwamoto, J	5
Uzawa, M	5
Reid, IR	1
Järvinen, TL	1
Michaëlsson, K	1
Aspenberg, P	1
Sievänen, H	1
Su, FM	1
Cheng, TT	1
Lai, HM	1
Yu, SF	1
van de Glind, EM	1
Willems, HC	1
Eslami, S	1
Abu-Hanna, A	1
Lems, WF	1
Hooft, L	1
de Rooij, SE	1
Black, DM	13
van Munster, BC	1
Zhao, Y	2
Xue, R	1
Shi, N	1
Lin, W	1
Pei, B	1
Sun, C	1
Fan, R	1
Jiang, Y	1
Tetsunaga, T	2
Nishida, K	1
Tanaka, M	1
Sugimoto, Y	1
Takigawa, T	1
Takei, Y	1
Ozaki, T	1
Valter, I	1
Riis, BJ	1
Christiansen, C	1
Black, D	4
Moriwaki, K	1
Mouri, M	1
Nayak, S	1
Greenspan, SL	1
Pepe, J	1
Petrucci, MT	1
Mascia, ML	1
Piemonte, S	1
Fassino, V	1
Romagnoli, E	1
Minisola, S	1
Roerholt, C	1
Eiken, P	2
Abrahamsen, B	2
Ofluoglu, O	1
Ofluoglu, D	1
Papaioannou, A	3
Kennedy, CC	1
Freitag, A	1
Ioannidis, G	2
O'Neill, J	1
Webber, C	1
Pui, M	1
Berthiaume, Y	1
Rabin, HR	1
Paterson, N	1
Jeanneret, A	1
Matouk, E	1
Villeneuve, J	1
Nixon, M	1
Adachi, JD	7
Hochberg, MC	9
Imai, K	2
Ohnishi, I	2
Matsumoto, T	1
Yamamoto, S	2
Nakamura, K	1
Curtis, JR	2
Westfall, AO	1
Cheng, H	1
Delzell, E	2
Bize, R	1
Peytremann-Bridevaux, I	1
Mathew, R	1
Dhillon, V	1
Shepherd, P	1
Donaldson, MG	2
Palermo, L	6
Cummings, SR	13
Harada, A	2
Schwartz, AV	3
Cauley, JA	4
Wallace, RB	2
Feldstein, AC	1
Lombardi, A	3
Husein-Elahmed, H	1
Aneiros-Fernandez, J	1
Arias-Santiago, S	1
Aneiros-Cachaza, J	1
Naranjo-Sintes, R	1
Eastell, R	1
Chen, L	1
Ensrud, K	4
Judd, S	1
Safford, MM	1
Lin, TC	1
Yang, CY	1
Yang, YH	1
Lin, SJ	1
Tseng, YY	1
Su, CH	1
Lui, TN	1
Yeh, YS	1
Yeh, SH	1
Robinson, PJ	1
Bell, RJ	1
Lanzafame, A	1
Segal, L	1
Kirby, C	1
Piterman, L	1
Davis, SR	1
Elliott, ME	1
Srivastava, M	1
Deal, C	1
Heijckmann, AC	1
Juttmann, JR	1
Wolffenbuttel, BH	1
Minne, HW	3
Pollähne, W	2
Pfeifer, M	2
Begerow, B	2
Hinz, C	1
Buckley, LM	1
Hillner, BE	1
Fonderico, F	1
Fittipaldi, MR	1
Vitale, G	1
Ciccarelli, A	1
Lupoli, GA	1
Panico, A	1
Cascella, T	1
Lupoli, G	1
Deal, CL	1
Nelson, DB	1
Kerani, RP	1
Schreiner, PJ	1
Nevitt, MC	9
Thompson, DE	9
Takeda, T	4
Ichimura, S	2
Ringe, JD	3
Dorst, A	1
Faber, H	1
Ibach, K	1
Ettinger, MP	1
Drake, WM	1
Kendler, DL	1
Rosen, CJ	1
Orwoll, ES	1
Sarikaya, S	1
Ozdolap, S	1
Açikgöz, G	1
Erdem, CZ	1
Hosking, D	2
Devogelaer, JP	2
Tucci, JR	1
Emkey, RD	2
Tonino, RP	1
Rodriguez-Portales, JA	2
Downs, RW	2
Gupta, J	1
Santora, AC	2
Liberman, UA	4
Naka, H	1
Kobayashi, S	1
Shiraki, M	3
Takaoka, K	1
Wehren, LE	2
Garnero, P	3
Hochberg, M	1
Ott, S	1
Orloff, J	1
Ewing, SK	2
Delmas, PD	3
Kushida, K	1
Kishimoto, H	3
Morii, H	1
Yamamoto, K	1
Kaneda, K	1
Fukunaga, M	1
Inoue, T	1
Nakashima, M	1
Orimo, H	2
Sato, Y	2
Chapurlat, RD	1
Ramsay, P	1
Bartl, R	1
Quandt, SA	4
Schneider, DL	1
Kaplan, RJ	1
Vo, AN	1
Stitik, TP	1
Kamen, LB	1
Bitar, AA	1
Shih, VC	1
Wallace, DJ	1
Nendaz, M	1
Cauley, J	2
Geusens, P	1
Ross, PD	3
Baran, D	1
Sawka, AM	2
Gafni, A	1
Hanley, DA	3
Thabane, L	2
Nyman, JA	3
Kane, RL	3
Melton, LJ	3
Zein, CO	1
Jorgensen, RA	1
Clarke, B	1
Wenger, DE	1
Keach, JC	1
Angulo, P	1
Lindor, KD	1
Mikhail, N	1
Cope, D	1
Seeman, E	2
Olszynski, WP	1
Brown, JP	2
Murray, TM	1
Josse, RG	1
Sebaldt, RJ	2
Petrie, A	1
Tenenhouse, A	1
Goldsmith, CH	1
Boulos, P	1
Kouroukis, T	1
McKinney, J	1
Santora, A	1
Delmas, P	1
Chevrel, G	1
Schott, AM	1
Fontanges, E	1
Charrin, JE	1
Lina-Granade, G	1
Duboeuf, F	1
Arlot, M	1
Raynal, C	1
Meunier, PJ	1
Kabi, F	1
Mkinsi, O	1
Zrigui, J	1
Kurato, S	1
Iwase, T	1
Inoue, K	1
Sasaki, Y	1
Tanaka, T	1
Fujita, M	1
Nakano, T	1
Ando, F	1
Miyakawa, N	1
Kuroda, T	1
Roux, C	1
Briot, K	1
Dumarcet, N	1
Bourgoin, M	1
Chapurlat, R	1
Christin-Maitre, S	1
Cortet, B	1
Costagliola, D	1
Diebolt, V	1
Lacoin, F	1
Letombe, B	1
Oberlin, F	1
Orcel, P	1
Ravaud, P	1
Seret, P	1
Vogel, JY	1
Barna, A	1
Nouyrigat, E	1
Veyries, ML	1
Yoldjian, I	1
Levis, S	1
Satterfield, S	1
Farahmand, P	1
Schacht, E	1
Rozehnal, A	1
Ström, O	1
Borgström, F	1
Sen, SS	1
Boonen, S	1

Trial	Phase	Enrollment	Study Type	Start Date	Status
A Randomized, Double-blind, Placebo-Controlled, Comparative Multicenter Phase 3 Study to Evaluate the Safety and Efficacy of BA058 (Abaloparatide) for Injection for Prevention of Fracture in Ambulatory Postmenopausal Women With Severe Osteoporosis and at [NCT01343004]	Phase 3	2,463 participants (Actual)	Interventional	2011-04-30	Completed
An Extension Study to Evaluate 24 Months of Standard-of-Care Osteoporosis Management Following Completion of 18 Months of BA058 or Placebo Treatment in Protocol BA058-05-003[NCT01657162]	Phase 3	1,139 participants (Actual)	Interventional	2012-11-20	Completed
Orthopaedic Conservative Treatment in the Time of Covid-19 Pandemic[NCT04623346]		262 participants (Anticipated)	Observational	2020-03-11	Active, not recruiting
A Multicenter, International, Randomized, Double-blind, Alendronate-controlled Study to Determine the Efficacy and Safety of Romosozumab in the Treatment of Postmenopausal Women With Osteoporosis[NCT01631214]	Phase 3	4,093 participants (Actual)	Interventional	2012-05-04	Completed
Effects of Romosozumab on Bone Health in Women With Spinal Cord Injury and Osteoporosis[NCT04708886]	Phase 2	12 participants (Anticipated)	Interventional	2021-03-01	Active, not recruiting
Risedronate With High-dose Vitamin D Resolves Hyperparathyroidism and Hypovitaminosis D But Not Osteoporosis in Mexican Postmenopausal Patients[NCT05346419]		33 participants (Actual)	Interventional	2021-07-01	Completed
Vitamin D Improves Osteoporosis in Postmenopausal Women With Denosumab Failure[NCT05372224]		55 participants (Actual)	Interventional	2020-06-22	Completed
STOP Vertigo: Supplementation of Vitamin D for Termination of Recurrences From Benign Paroxysmal Positional Vertigo[NCT05863949]		860 participants (Anticipated)	Interventional	2023-07-31	Not yet recruiting
An Open-Label, Single-Arm, Multicenter Study to Evaluate the Early Effects of Abaloparatide on Tissue-Based Indices of Bone Formation and Resorption[NCT03710889]	Phase 3	23 participants (Actual)	Interventional	2018-09-20	Completed
A Multicentre, Double-Blind, Randomized Placebo-Controlled Study of 70mg Alendronate Once Weekly for the Prevention and Treatment of Osteoporosis in Canadian Adult Cystic Fibrosis Patients[NCT00157690]	Phase 4	56 participants (Actual)	Interventional	2003-12-31	Completed
Predictive Value of Bone Turnover Markers During Discontinuation With Alendronate[NCT03051620]		142 participants (Actual)	Observational	2017-02-01	Completed
A 5-year, Double-blind, Randomized, Placebo-controlled Extension Study to Examine the Long-term Safety and Efficacy of Oral Alendronate in Postmenopausal Women Who Previously Received Alendronate in Conjunction With the Fracture Intervention Trial[NCT00398931]	Phase 3	1,099 participants (Actual)	Interventional	1998-02-28	Completed
Genetic Analysis of Familial Cases of Premature Ovarian Failure[NCT01177891]		110 participants (Actual)	Observational	2010-10-31	Completed
Comparison of 3 Month PTHrP(1-36) and PTH(1-34) on Post-Menopausal Osteoporosis[NCT00853723]	Phase 2	105 participants (Actual)	Interventional	2009-05-31	Completed
Impact of Neoadjuvant Chemotherapy With or Without Zometa on Occult Micrometastases and Bone Density in Women With Locally Advanced Breast Cancer[NCT00242203]	Phase 2	120 participants (Actual)	Interventional	2002-10-31	Completed
Prevention of Glucocorticoid-Induced Osteoporosis in Patients With Rheumatic Diseases. The STOP-Study: a Randomized Placebo Controlled Trial With Alendronate Versus Alfacalcidol.[NCT00138983]	Phase 3	200 participants	Interventional	2000-05-31	Completed
Teriparatide for Joint Erosions in Rheumatoid Arthritis: The TERA Trial[NCT01400516]	Phase 4	26 participants (Actual)	Interventional	2011-08-31	Completed
A Phase II, Randomized, Double-Blind, Placebo-Controlled Study of Once-Weekly Alendronate in HIV-Infected Subjects With Decreased Bone Mineral Density Receiving Calcium and Vitamin D[NCT00061256]	Phase 2	80 participants	Interventional		Completed
Finding the Optimal Resistance Training Intensity For Your Bones: A Randomized Controlled Trial (FORTIFY Bones)[NCT05541432]		324 participants (Anticipated)	Interventional	2022-09-13	Recruiting
Preoperative Optimization Levosimendan in Heart Failure Patients Undergoing Hip Fracture[NCT02972918]		19 participants (Actual)	Observational	2014-05-31	Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

Intervention	participants (Number)
Placebo	30
BA058 80 mcg (Abaloparatide)	4
Teriparatide	6

Intervention	Participants (Number)
Placebo	33
BA058 80 mcg (Abaloparatide)	18
Teriparatide	24

Intervention	Hypercalcemic events (Number)
Placebo	5
BA058 80 mcg (Abaloparatide)	15
Teriparatide	34

Intervention	percent change (Mean)
Placebo	-0.44
BA058 80 mcg (Abaloparatide)	2.90
Teriparatide	2.26

Intervention	percent change from baseline (Mean)
Placebo	0.48
BA058 80 mcg (Abaloparatide)	9.20
Teriparatide	9.12

Intervention	percent change (Mean)
Placebo	-0.08
BA058 80 mcg (Abaloparatide)	3.44
Teriparatide	2.81

Nonvertebral fractures were defined as clinical fractures that included: 1) those of the hip, wrist, forearm, shoulder, collar bone, upper arm, ribs, upper leg (not hip), knee, lower leg (not knee or ankle), foot, ankle, hand, pelvis (not hip), tailbone, and other; and 2) those associated with low trauma, defined as a fall from standing height or less; a fall on stairs, steps or curbs; a minimal trauma other than a fall; or moderate trauma other than a fall. Complete results for Study BA058-05-003 are reported in the ClinicalTrials.gov Study Record NCT02653417. (NCT01657162)
Timeframe: Study BA058-05-003 Baseline (Day 1) up to Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Number of Participants With ≥1 New Vertebral Fracture Since Study BA058-05-003 Baseline

Intervention	percentage of events (Number)
Abaloparatide-SC/Alendronate	2.7
Placebo/Alendronate	5.6

Vertebral fractures were determined clinically and via protocol directed radiograph evaluation. Complete results for Study BA058-05-003 are reported in the ClinicalTrials.gov Study Record NCT02653417. (NCT01657162)
Timeframe: Study BA058-05-003 Baseline (Day 1) up to Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Number of Participants With a Clinically Notable Coagulation Laboratory Value (Data From Study BA058-05-005 Only)

Intervention	Participants (Count of Participants)
Abaloparatide-SC/Alendronate	3
Placebo/Alendronate	25

Coagulation laboratory parameters that were evaluated via notable criteria (presented in parentheses) included: Activated Partial Thromboplastin Time (≥1.41*ULN), Prothrombin Time (≥1.21*ULN). Because the Activated Partial Thromboplastin Time was the only coagulation laboratory parameter with at least 1 participant with a notable laboratory value, this is the only parameter presented below. (NCT01657162)
Timeframe: Study BA058-05-005 Baseline (Day 1) up to Study BA058-05-005 Month 24

Number of Participants With a Nonvertebral Fracture Since Study BA058-05-003 Baseline (Data From Studies BA058-05-005 and BA058-05-003 Combined)

Intervention	Participants (Count of Participants)
Abaloparatide-SC/Alendronate	9
Placebo/Alendronate	4

Percent Change From Study BA058-05-003 Baseline in Femoral Neck BMD at Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Intervention	Participants (Count of Participants)
Abaloparatide-SC/Alendronate	15
Placebo/Alendronate	32

Femoral neck BMD were measured via DXA. Complete results for Study BA058-05-003 are reported in the ClinicalTrials.gov Study Record NCT02653417. (NCT01657162)
Timeframe: Study BA058-05-003 Baseline (Day 1), Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Percent Change From Study BA058-05-003 Baseline in Lumbar Spine BMD at Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Intervention	percent change (Mean)
Abaloparatide-SC/Alendronate	4.5113
Placebo/Alendronate	0.4649

Lumbar spine BMD were measured via DXA. Complete results for Study BA058-05-003 are reported in the ClinicalTrials.gov Study Record NCT02653417. (NCT01657162)
Timeframe: Study BA058-05-003 Baseline (Day 1), Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Percent Change From Study BA058-05-003 Baseline in Total Hip BMD at Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Intervention	percent change (Mean)
Abaloparatide-SC/Alendronate	12.7921
Placebo/Alendronate	3.5133

Total hip BMD were measured via DXA. Complete results for Study BA058-05-003 are reported in the ClinicalTrials.gov Study Record NCT02653417. (NCT01657162)
Timeframe: Study BA058-05-003 Baseline (Day 1), Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Number of Participants With a Clinically Notable Hematology Laboratory Value (Data From Study BA058-05-005 Only)

Intervention	percent change (Mean)
Abaloparatide-SC/Alendronate	5.4737
Placebo/Alendronate	1.3698

Hematology laboratory parameters that were evaluated via notable criteria (presented in parentheses) included: Absolute Eosinophils (>5000 cells/mm^3), Absolute Lymphocytes (≤499 cells/mm^3), Absolute Neutrophils (≤999 cells/mm^3), % Eosinophils (>50%), % Lymphocytes (≤5%), % Neutrophils (≤10%), Hemoglobin (Low: ≤9.4 g/dL; High: change from baseline ≥2.1 g/dL), Platelets (≤99000 cells/mm^3), and White Blood Cells (Low: ≤1499 cells/mm^3; High: ≥20001 cells/mm^3). Only the hematology parameters with at least 1 participant with a notable laboratory value are presented. (NCT01657162)
Timeframe: Study BA058-05-005 Baseline (Day 1) up to Study BA058-05-005 Month 24

Number of Participants With a Clinically Notable Serum Chemistry Laboratory Value (Data From Study BA058-05-005 Only)

Intervention	Participants (Count of Participants)
	Absolute Lymphocytes	Lymphocytes (Absolute Count or Percentage)	Absolute Neutrophils	Neutrophils (Absolute Count or Percentage)	Hemoglobin (Low)	Hemoglobin (High)	Platelets
Abaloparatide-SC/Alendronate	15	15	0	0	7	19	1
Placebo/Alendronate	11	11	2	2	2	17	0

Serum Chemistry laboratory parameters that were evaluated via notable criteria (presented in parentheses) included: sodium (Low: ≤129; High: ≥148 milliequivalent per liter [mEq/L]), potassium (Low: ≤3.2; High: ≥5.5 mEq/L), albumin (<2.5 grams [g]/deciliter [dL]), total protein (<5 g/dL), glucose (Low: ≤54; High: >125 mg/dL [fasting] or >200 milligrams [mg]/dL [random]), creatinine (≥2.1 mg/dL), aspartate aminotransferase (AST) (≥5.1*upper limit of normal [ULN]), alanine aminotransferase (ALT) (≥5.1*ULN), alkaline phosphatase (AP) (≥3.1*ULN), total bilirubin (≥1.51*ULN [with any increase in liver function tests] ≥2.0*ULN [with normal liver function tests]), creatine kinase (≥3.1*ULN), total cholesterol (>226 mg/dL), and total calcium (Low: ≤7.4; High: ≥11.6 mg/dL). Only the serum chemistry parameters with at least 1 participant with a notable laboratory value are presented. (NCT01657162)
Timeframe: Study BA058-05-005 Baseline (Day 1) up to Study BA058-05-005 Month 24

Number of Participants With a Clinically Notable Urine Laboratory Value (Data From Study BA058-05-005 Only)

Intervention	Participants (Count of Participants)
	Alkaline Phosphatase	Cholesterol Total	Creatine Kinase	Glucose (Fasting; High)	Glucose (Random)	Potassium (Low)	Potassium (High)	Sodium (Low)	Sodium (High)
Abaloparatide-SC/Alendronate	1	75	2	22	1	1	4	1	6
Placebo/Alendronate	0	73	1	18	2	3	3	1	2

Urine laboratory parameters that were evaluated via notable criteria (presented in parentheses) included: Glucose (2+), Protein (2+), Blood (>50 red blood cells per high-power field [rbc/hpf]). (NCT01657162)
Timeframe: Study BA058-05-005 Baseline (Day 1) up to Study BA058-05-005 Month 24

Number of Participants With Treatment Emergent Adverse Events (TEAEs) (Data From Study BA058-05-005 Only)

Intervention	Participants (Count of Participants)
	Glucose	Protein	Blood
Abaloparatide-SC/Alendronate	4	6	77
Placebo/Alendronate	3	6	50

A TEAE is any untoward medical occurrence or undesirable event(s) experienced in a participant that begins or worsens following administration of study drug, whether or not considered related to study drug by Investigator. A serious adverse event (SAE) was an adverse event (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), congenital anomaly/birth defect, or persistent or significant disability/incapacity. Intensity for each AE was defined as mild, moderate, or severe. AEs included both SAEs and non-serious AEs. AEs whose causal relation was characterized as Possible or Probable were considered as related to study drug. AEs were coded using Medical Dictionary for Regulatory Activities (MedDRA). A summary of serious and all other non-serious adverse events, regardless of causality, is located in the Reported Adverse Events module. (NCT01657162)
Timeframe: Study BA058-05-005 Baseline (Day 1) up to Study BA058-05-005 Month 24

Percent Change From Baseline in Bone Mineral Density at the Femoral Neck at Month 12

Intervention	Participants (Count of Participants)
	TEAEs	TEAEs Related to Study Treatment	Severe TEAEs	Serious TEAEs	TEAEs Leading to Death	TEAEs Leading to Discontinuation
Abaloparatide-SC/Alendronate	452	85	38	65	0	30
Placebo/Alendronate	466	80	40	58	2	36

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 12

Percent Change From Baseline in Bone Mineral Density at the Lumbar Spine at Month 12

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	1.7
Romosozumab/Alendronate	4.9

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 12

Percent Change From Baseline in Bone Mineral Density at the Lumbar Spine at Month 24

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	5.0
Romosozumab/Alendronate	13.7

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 24

Percent Change From Baseline in Bone Mineral Density at the Total Hip at Month 12

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	7.2
Romosozumab/Alendronate	15.3

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 12

Percent Change From Baseline in Bone Mineral Density of the Femoral Neck at at Month 24

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	2.8
Romosozumab/Alendronate	6.2

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 24

Percent Change From Baseline in Bone Mineral Density of the Femoral Neck at Month 36

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	2.3
Romosozumab/Alendronate	6.0

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 36

Percent Change From Baseline in Bone Mineral Density of the Lumbar Spine at Month 36

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	2.4
Romosozumab/Alendronate	6.0

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 36

Percent Change From Baseline in Bone Mineral Density of the Total Hip at Month 24

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	7.8
Romosozumab/Alendronate	15.2

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 24

Percent Change From Baseline in Bone Mineral Density of the Total Hip at Month 36

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	3.5
Romosozumab/Alendronate	7.2

Bone mineral density (BMD) was measured by dual-energy x-ray absorptiometry (DXA). DXA scans were analyzed by a central imaging center. (NCT01631214)
Timeframe: Baseline and month 36

Percentage of Participants With a Clinical Fracture at the Primary Analysis

Intervention	percent change (Least Squares Mean)
Alendronate/Alendronate	3.5
Romosozumab/Alendronate	7.2

All fracture assessments were performed by blinded central imaging readers. Clinical fractures included clinical vertebral and nonvertebral fractures (excluding skull, facial, mandible, cervical vertebrae, thoracic vertebrae, lumbar vertebrae, metacarpus, finger phalanges, and toe phalanges) that were associated with signs and/or symptoms indicative of a fracture. Clinical vertebral fractures were included regardless of trauma severity or pathologic fractures; nonvertebral fractures associated with high trauma severity or pathologic fractures were excluded. (NCT01631214)
Timeframe: The primary analysis was performed when clinical fracture events had been confirmed in at least 330 patients and all participants had completed the month 24 visit. The median follow-up was 2.7 years (interquartile range, 2.2 to 3.3).

Percentage of Participants With a Clinical Fracture Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	13.0
Romosozumab/Alendronate	9.7

Clinical fractures included clinical vertebral and nonvertebral fractures (excluding skull, facial, mandible, cervical vertebrae, thoracic vertebrae, lumbar vertebrae, metacarpus, finger phalanges, and toe phalanges) that were associated with signs and/or symptoms indicative of a fracture. Clinical vertebral fractures were included regardless of trauma severity or pathologic fractures; nonvertebral fractures associated with high trauma severity or pathologic fractures were excluded. (NCT01631214)
Timeframe: 12 months

Percentage of Participants With a Clinical Fracture Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	5.4
Romosozumab/Alendronate	3.9

Percentage of Participants With a Clinical Vertebral Fracture Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	9.6
Romosozumab/Alendronate	7.1

A clinical vertebral fracture is a new or worsening vertebral fracture assessed at either a scheduled or unscheduled visit and associated with any signs and/or symptoms of back pain indicative of a fracture, regardless of trauma severity or whether it is pathologic. (NCT01631214)
Timeframe: 12 months

Percentage of Participants With a Clinical Vertebral Fracture Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	0.9
Romosozumab/Alendronate	0.5

Percentage of Participants With a Hip Fracture at the Primary Analysis

Intervention	percentage of participants (Number)
Alendronate/Alendronate	2.1
Romosozumab/Alendronate	0.9

Hip fractures were defined as a subset of nonvertebral fractures including fractures of the femur neck, femur intertrochanter, and femur subtrochanter. (NCT01631214)
Timeframe: The primary analysis was performed when clinical fracture events had been confirmed in at least 330 patients and all participants had completed the month 24 visit. The median follow-up was 2.7 years (interquartile range, 2.2 to 3.3).

Percentage of Participants With a Hip Fracture Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	3.2
Romosozumab/Alendronate	2.0

Hip fractures were defined as a subset of nonvertebral fractures including fractures of the femur neck, femur intertrochanter, and femur subtrochanter. (NCT01631214)
Timeframe: 12 months

Percentage of Participants With a Hip Fracture Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	1.1
Romosozumab/Alendronate	0.7

Hip fractures were defined as a subset of nonvertebral fractures including fractures of the femur neck, femur intertrochanter, and femur subtrochanter. (NCT01631214)
Timeframe: 24 months

Percentage of Participants With a Major Nonvertebral Fracture at the Primary Analysis

Intervention	percentage of participants (Number)
Alendronate/Alendronate	2.1
Romosozumab/Alendronate	1.5

Major nonvertebral fractures included a subset of nonvertebral fractures including pelvis, distal femur (ie, femur excluding hip), proximal tibia (ie, tibia excluding ankle), ribs, proximal humerus (ie, humerus excluding elbow), forearm, and hip. (NCT01631214)
Timeframe: The primary analysis was performed when clinical fracture events had been confirmed in at least 330 patients and all participants had completed the month 24 visit. The median follow-up was 2.7 years (interquartile range, 2.2 to 3.3).

Percentage of Participants With a Major Osteoporotic Fracture Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	9.6
Romosozumab/Alendronate	7.1

Major osteoporotic fractures included clinical vertebral fractures and fractures of the hip, forearm and humerus. Fractures associated with high trauma severity or pathologic fractures were excluded. (NCT01631214)
Timeframe: 12 months

Percentage of Participants With a New or Worsening Vertebral Fracture Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	4.2
Romosozumab/Alendronate	3.0

"A new or worsening vertebral fracture was identified when there was a ≥ 1 grade increase from the previous grade in any vertebra from T4 to L4 according to the Genant Semiquantitative Scoring method based on assessment of x-rays according to the following scale:~Grade 0 (Normal) = no fracture;~Grade 1 (Mild) = mild fracture, 20 to 25% reduction in vertebral height (anterior, middle, or posterior);~Grade 2 (Moderate) = moderate fracture, 25 to 40% reduction in anterior, middle, and/or posterior height;~Grade 3 (Severe) = severe fracture, greater than 40% reduction in anterior, middle, and/or posterior height.~Incident vertebral fractures were confirmed by a second independent reader using the Semiquantitative method." (NCT01631214)
Timeframe: 24 months

Percentage of Participants With a Nonvertebral Fracture at the Primary Analysis

Intervention	percentage of participants (Number)
Alendronate/Alendronate	9.2
Romosozumab/Alendronate	4.8

A nonvertebral fracture was defined as a documented fracture excluding skull, facial, mandible, cervical vertebrae, thoracic vertebrae, lumbar vertebrae, metacarpus, finger phalanges, and toe phalanges. In addition, fractures associated with high trauma severity or pathologic fractures were excluded. (NCT01631214)
Timeframe: The primary analysis was performed when clinical fracture events had been confirmed in at least 330 patients and all participants had completed the month 24 visit. The median follow-up was 2.7 years (interquartile range, 2.2 to 3.3).

Percentage of Participants With a Nonvertebral Fracture Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	10.6
Romosozumab/Alendronate	8.7

A nonvertebral fracture was defined as a fracture present on a copy of radiographs or other diagnostic images such as computerized tomography (CT) or magnetic resonance imaging confirming the fracture within 14 days of reported fracture image date recorded by the study site, and/or documented in a copy of the radiology report, surgical report, or discharge summary, excluding skull, facial, mandible, cervical vertebrae, thoracic vertebrae, lumbar vertebrae, metacarpus, finger phalanges, and toe phalanges. In addition, fractures associated with high trauma severity or pathologic fractures were excluded. (NCT01631214)
Timeframe: 12 months

Percentage of Participants With a Nonvertebral Fracture Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	4.6
Romosozumab/Alendronate	3.4

Percentage of Participants With Any Fracture at the Primary Analysis

Intervention	percentage of participants (Number)
Alendronate/Alendronate	7.8
Romosozumab/Alendronate	6.3

All fractures include any osteoporotic nonvertebral fractures that are not associated with high trauma severity or pathologic fractures and new or worsening vertebral fractures regardless of trauma severity or pathologic fractures. (NCT01631214)
Timeframe: The primary analysis was performed when clinical fracture events had been confirmed in at least 330 patients and all participants had completed the month 24 visit. The median follow-up was 2.7 years (interquartile range, 2.2 to 3.3).

Percentage of Participants With Any Fracture Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	19.1
Romosozumab/Alendronate	13.0

Percentage of Participants With Multiple New or Worsening Vertebral Fractures Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	9.2
Romosozumab/Alendronate	6.5

A new or worsening vertebral fracture was identified when there was a ≥ 1 grade increase from the previous grade in any vertebra from T4 to L4 according to the Genant Semiquantitative Scoring method. A participant had multiple new or worsening vertebral fractures when there were ≥ 2 vertebrae from T4 to L4 with ≥ 1 grade increase from the previous grade. The multiple new or worsening vertebral fractures need not have occurred at the same visit. Incident vertebral fractures were confirmed by a second independent reader. (NCT01631214)
Timeframe: 24 months

Percentage of Participants With New Vertebral Fractures Through Month 12

Intervention	percentage of participants (Number)
Alendronate/Alendronate	2.5
Romosozumab/Alendronate	1.3

"New vertebral fractures occurred when there was ≥ 1 grade increase from the previous grade of 0 in any vertebra from T4 to L4 using the Genant Semiquantitative Scoring method based on assessment of x-rays according to the following scale:~Grade 0 (Normal) = no fracture;~Grade 1 (Mild) = mild fracture, 20 to 25% reduction in vertebral height (anterior, middle, or posterior);~Grade 2 (Moderate) = moderate fracture, 25 to 40% reduction in anterior, middle, and/or posterior height;~Grade 3 (Severe) = severe fracture, greater than 40% reduction in anterior, middle, and/or posterior height.~Incident vertebral fractures were confirmed by a second independent reader." (NCT01631214)
Timeframe: 12 months

Percentage of Participants With New Vertebral Fractures Through Month 24

Intervention	percentage of participants (Number)
Alendronate/Alendronate	5.0
Romosozumab/Alendronate	3.2

"All fracture assessments were performed by blinded central imaging readers.~New vertebral fractures occurred when there was ≥ 1 grade increase from the previous grade of 0 in any vertebra from T4 to L4 using the Genant Semiquantitative Scoring method based on assessment of x-rays according to the following scale:~Grade 0 (Normal) = no fracture;~Grade 1 (Mild) = mild fracture, 20 to 25% reduction in vertebral height (anterior, middle, or posterior);~Grade 2 (Moderate) = moderate fracture, 25 to 40% reduction in anterior, middle, and/or posterior height;~Grade 3 (Severe) = severe fracture, greater than 40% reduction in anterior, middle, and/or posterior height.~Incident vertebral fractures were confirmed by a second independent reader using the Semiquantitative method." (NCT01631214)
Timeframe: 24 months

Change From Baseline in Bone Formation Rate/Bone Surface (BFR/BS) in the Cancellous Envelope at Month 3

Intervention	percentage of participants (Number)
Alendronate/Alendronate	8.0
Romosozumab/Alendronate	4.1

Change in dynamic histomorphometry indices was assessed in the cancellous envelope. BFR/BS was reported as cubic millimeter/square millimeter/year (mm^3/mm^2/year). (NCT03710889)
Timeframe: Baseline (Day 1), Month 3

Change From Baseline in Mineralizing Surface/Bone Surface (MS/BS) in the Cancellous Envelope at Month 3

Intervention	mm^3/mm^2/year (Mean)
	Baseline	Change at Month 3
Abaloparatide	0.011	0.034

Change in dynamic histomorphometry indices was assessed in the cancellous envelope. (NCT03710889)
Timeframe: Baseline (Day 1), Month 3

Change in Serum Carboxy-Terminal Cross-Linking Telopeptide of Type I Collagen (s-CTX) From Baseline at Month 1 and Month 3

Blood samples were taken to measure efficacy-related markers of bone metabolism at Day 1, Month 1, and Month 3. (NCT03710889)
Timeframe: Baseline (Day 1), Months 1 and 3

Change in Serum Procollagen Type I N-terminal Propeptide (s-P1NP) From Baseline at Month 1 and Month 3

Blood samples were taken to measure efficacy related markers of bone metabolism at Day 1, Month 1, and Month 3. (NCT03710889)
Timeframe: Baseline (Day 1), Months 1 and 3

Number of Participants in Which CTX Increased Above the Least Significant Change

"Number of participants in which CTX increased above the least significant change.~The Department of Clinical Biochemistry, Rigshospitalet, Glostrup, Denmark provided the the least significant change for p-CTX > 30%." (NCT03051620)
Timeframe: From baseline to month 24

If Baseline Bone Turnover Markers at the Time of Alendronate Discontinuation Predict Changes in BMD After One and Two Years.

We constructed receiver operating characteristic (ROC) curves to evaluate if baseline p-CTX or baseline p-PINP at the time of alendronate discontinuation predicted TH BMD loss above the least significant change at month 12 and/or month 24 at the individual level. (NCT03051620)
Timeframe: Changes in TH BMD after one and two years.

If Carboxy-terminal Collagen Crosslinks (CTX) Three and Six Months After Stopping Alendronate Predicted TH BMD (Total Hip BMD) Loss Above the Least Significant Change at Month 12 at the Individual Level.

We constructed receiver operating characteristic (ROC) curves to evaluate if carboxy-terminal collagen crosslinks (CTX) three and six months after stopping alendronate predicted TH BMD loss above the least significant change (LSC) at month 12 at the individual level. (NCT03051620)
Timeframe: Baseline and one year after baseline

Percent Change in Bone Turnover Markers Measured Three and Six Months After Stopping Alendronate Treatment and BMD After One and Two Years

We constructed receiver operating characteristic (ROC) curves to evaluate if changes in p-CTX or p-PINP measured three and six months after stopping alendronate predicted TH BMD loss above the least significant change at month 12 and/or month 24 at the individual level. (NCT03051620)
Timeframe: one and two years after baseline

The Number of Participants Who Lost BMD Beyond the Least Significant Change (LSC) at the Lumbar Spine and Total Hip.

the number of patients who lost BMD beyond the LSC at the lumbar spine (>3%) and total hip (>5%) (NCT03051620)
Timeframe: from baseline to month 24

Changes in Bone Mineral Density of the Distal 1/3 Radius.

Changes in Bone Mineral Density of the Femoral Neck.

Changes in Bone Mineral Density of the Forearm.

Changes in Bone Mineral Density of the Lumbar Spine.

Changes in Bone Mineral Density of the Total Hip.

1,25 Vitamin D

24 Hour Urine Calcium

Carboxy-terminal Telopeptides of Collagen-1 (CTX)

Fractional Excretion of Calcium

(Serum Creatinine X Urine Calcium)/(Serum Calcium X Urine Creatinine) (NCT00853723)
Timeframe: Baseline, Day 15, Day 30, Day 60, Day 90

Procallagen-1 Amino-terminal Peptide (P1NP)

Serum Phosphorous

Total Serum Calcium (mg/dl)

Tubular Maximum for Phosphorous/Glomerular Filtration Rate (TMP/GFR)

"Fractional tubular reabsorption of phosphate (TRP) = 1-{(U phos/P phos) x ( P creat/U creat)} if TRP < or = 0.86 then TMP/GFR = TRP x P phos if TRP > 0.86 then TMP/GFR = 0.3 x TRP/{1-(0.8 x TRP)} x P phos~U= urine, P = plasma" (NCT00853723)
Timeframe: Baseline, Day 15, Day 30, Day 60, Day 90

Change From Baseline in Bone Mineral Density (BMD) Measured by Dual-Energy X-ray Absorptiometry (DXA) and Instant Vertebral Assessment (IVA) Scan

BMD was measured at the lumbosacral spine antero-posterior and at the femoral neck using a densitometer. A positive change from Baseline (increased bone density) indicates improvement. (NCT01400516)
Timeframe: Baseline and Month 12

Change From Baseline in Disease Activity Score 28 Joint Count C-Reactive Protein (DAS-28 CRP)

The DAS28 score is a measure of the patient's disease activity calculated using the tender joint count (TJC) [28 joints], swollen joint count (SJC) [28 joints], patient's global assessment of disease activity [visual analog scale: 0=no disease activity to 100=maximum disease activity] and C-Reactive Protein (CRP) for a total possible score of 2 to 10. Higher values indicate higher disease activity. A negative change from baseline indicates improvement. (NCT01400516)
Timeframe: Baseline and Month 12

Change From Baseline in Joint Erosion Volume Measured by 3-Dimensional Computed Tomography (3D CT) Scan

Both hands were scanned using a CT scanner. A semi-automated software tool was used to segment the erosion margins in 3D. A board certified radiologist identified the individual erosions in six sub-regions: radius, ulna, proximal carpals, distal carpals, metacarpophalangeal (MCP) joints and proximal interphalangeal (PIP) joints. The average total in a single hand/wrist was calculated. A negative change from Baseline(less joint erosions) indicates improvement. (NCT01400516)
Timeframe: Baseline and Month 12

Intervention	ng/mL (Median)
	Baseline	Change at Month 1	Change at Month 3
Abaloparatide	0.460	0.052	0.311

Intervention	percentage change (Mean)
	Mean change in TH BMD after one year	Mean change in TH BMD after two years
Study Population	-1.14	-2.65

Intervention	percentage change (Mean)
	Mean change in CTX from baseline to month 3	Mean change in CTX from baseline to month 6	Mean change in TH BMD from baseline to month 12
Study Population	49	64	1.14

Intervention	percentage change (Mean)
	Mean change in PINP from baseline to month 3	Mean change in PINP from baseline to month 6	Mean change in TH BMD from baseline to month 12	Mean change in TH BMD from baseline to month 24
Study Population	36	54	-1.14	-2.65

Intervention	Percent change from baseline (Mean)
PTHrP 400 mcg/Day	-0.35
PTHrP 600 mcg/Day	-0.34
PTH 20 mcg/Day	-0.82

Intervention	Percent change from baseline (Mean)
PTHrP 400 mcg/Day	0.91
PTHrP 600 mcg/Day	0.54
PTH 20 mcg/Day	0.61

Intervention	Percent change from baseline (Mean)
PTHrP 400 mcg/Day	-0.48
PTHrP 600 mcg/Day	-0.99
PTH 20 mcg/Day	-0.97

Intervention	Percent change from baseline (Mean)
PTHrP 400 mcg/Day	1.89
PTHrP 600 mcg/Day	1.52
PTH 20 mcg/Day	2.17

Intervention	Percent change from baseline (Mean)
PTHrP 400 mcg/Day	0.68
PTHrP 600 mcg/Day	0.72
PTH 20 mcg/Day	0.54

Intervention	pg/ml (Mean)
	Baseline	Day 15	Day 30	Day 60	Day 90
PTH 20 mcg/Day	42.51	65.25	67.29	58.15	53.73
PTHrP 400 mcg/Day	49.06	84.92	76.04	67.85	64.36
PTHrP 600 mcg/Day	42.49	63.07	65.15	57.02	55.08

Intervention	grams/centimeters squared (g/cm^2) (Mean)
	Spine, Baseline	Spine, Change from Baseline at Month12	Femoral neck, Baseline	Femoral neck, Change from Baseline at Month 12
Control Arm	0.93	-0.002	0.73	-0.03
Teriparatide	0.91	0.06	0.68	0.03

Intervention	score on a scale (Mean)
	Baseline	Change from Baseline at Month 12
Control Arm	2.73	-0.50
Teriparatide	2.66	0.42

Article	Year
The efficiency and safety of alendronate versus teriparatide for treatment glucocorticoid-induced osteoporosis: A meta-analysis and systematic review of randomized controlled trials. PloS one, 2022, Volume: 17, Issue:5 Topics: Alendronate; Bone Density Conservation Agents; Glucocorticoids; Humans; Osteoporosis; Randomized Con	2022
Denosumab Versus Bisphosphonates for the Prevention of the Vertebral Fractures in Men with Osteoporosis: An Updated Network Meta-Analysis. Clinical and investigative medicine. Medecine clinique et experimentale, 2022, 09-21, Volume: 45, Issue:3 Topics: Alendronate; Bone Density Conservation Agents; Denosumab; Diphosphonates; Humans; Ibandronic Acid; M	2022
Effectiveness and Safety of Treatments to Prevent Fractures in People With Low Bone Mass or Primary Osteoporosis: A Living Systematic Review and Network Meta-analysis for the American College of Physicians. Annals of internal medicine, 2023, Volume: 176, Issue:2 Topics: Adult; Aged; Alendronate; Bone Density Conservation Agents; Denosumab; Diphosphonates; Female; Fract	2023
The clinical effectiveness of denosumab (Prolia®) in patients with hormone-sensitive cancer receiving endocrine therapy, compared to bisphosphonates, selective estrogen receptor modulators (SERM), and placebo: a systematic review and network meta-analysis Archives of osteoporosis, 2023, 01-10, Volume: 18, Issue:1 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Denosumab; Diphosphonates; Female; Horm	2023
Bisphosphonates for osteoporosis in people with cystic fibrosis. The Cochrane database of systematic reviews, 2023, 01-10, Volume: 1 Topics: Adult; Alendronate; Bone Density Conservation Agents; Child; Cystic Fibrosis; Diphosphonates; Female	2023
The Clinical Effectiveness of Denosumab (Prolia®) for the Treatment of Osteoporosis in Postmenopausal Women, Compared to Bisphosphonates, Selective Estrogen Receptor Modulators (SERM), and Placebo: A Systematic Review and Network Meta-Analysis. Calcified tissue international, 2023, Volume: 112, Issue:6 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Denosumab; Diphosphonates; Female; Huma	2023
Minodronate in the treatment of osteoporosis: A systematic review and meta-analysis. Medicine, 2020, Oct-02, Volume: 99, Issue:40 Topics: Aged; Aged, 80 and over; Alendronate; Alkaline Phosphatase; Bone Density Conservation Agents; Case-C	2020
Meta-regression analysis of the efficacy of alendronate for prevention of glucocorticoid-induced fractures. Medicine, 2020, Oct-16, Volume: 99, Issue:42 Topics: Alendronate; Bone Density Conservation Agents; Databases, Factual; Glucocorticoids; Hip Fractures; H	2020
CLINICAL EVALUATION OF COST EFFICACY OF DRUGS FOR TREATMENT OF OSTEOPOROSIS: A META-ANALYSIS. Endocrine practice : official journal of the American College of Endocrinology and the American Association of Clinical Endocrinologists, 2017, Volume: 23, Issue:7 Topics: Alendronate; Bone Density Conservation Agents; Cost-Benefit Analysis; Denosumab; Diphosphonates; Dru	2017
Advances in treatment of glucocorticoid-induced osteoporosis. Current opinion in endocrinology, diabetes, and obesity, 2017, Volume: 24, Issue:6 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Denosumab; Diphosphonates; Glucocortico	2017
Comparative Efficacy of Alendronate upon Vertebral Bone Mineral Density and Fracture Rates in East Asians Versus Non-East Asians with Postmenopausal Osteoporosis: A Systematic Review and Meta-Analysis. Hormone and metabolic research = Hormon- und Stoffwechselforschung = Hormones et metabolisme, 2018, Volume: 50, Issue:10 Topics: Alendronate; Asian People; Bone Density; Female; Humans; Osteoporosis, Postmenopausal; Randomized Co	2018
Long-Term Drug Therapy and Drug Discontinuations and Holidays for Osteoporosis Fracture Prevention: A Systematic Review. Annals of internal medicine, 2019, 07-02, Volume: 171, Issue:1 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Bone Diseases, Metabolic; Diphosphonate	2019
Systematic review and meta-analysis of the efficacy and safety of alendronate and zoledronate for the treatment of postmenopausal osteoporosis. Gynecological endocrinology : the official journal of the International Society of Gynecological Endocrinology, 2013, Volume: 29, Issue:12 Topics: Adult; Aged; Aged, 80 and over; Alendronate; Bone Density; Bone Density Conservation Agents; Diphosp	2013
Anti-reabsorptive agents in women with osteoporosis: determining statistical equivalence according to evidence-based methods. Journal of endocrinological investigation, 2014, Volume: 37, Issue:8 Topics: Alendronate; Antibodies, Monoclonal, Humanized; Bone Density Conservation Agents; Denosumab; Diphosp	2014
Osteoporosis: the emperor has no clothes. Journal of internal medicine, 2015, Volume: 277, Issue:6 Topics: Aging; Alendronate; Bone Density; Bone Density Conservation Agents; Evidence-Based Medicine; Female;	2015
Osteoporosis Treatment Efficacy for Men: A Systematic Review and Meta-Analysis. Journal of the American Geriatrics Society, 2017, Volume: 65, Issue:3 Topics: Alendronate; Bone Density Conservation Agents; Calcitonin; Denosumab; Humans; Male; Osteoporosis; Os	2017
Nonvertebral fracture risk reduction with nitrogen-containing bisphosphonates. Current osteoporosis reports, 2008, Volume: 6, Issue:3 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Diphosphonates; Dose-Response Relations	2008
[Prediction of vertebral strength using a CT based finite element method--clinical application in evaluation of the efficacy of alendronate]. Nihon rinsho. Japanese journal of clinical medicine, 2009, Volume: 67, Issue:5 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Clinical Trials as Topic; Compressive S	2009
[Alendronate for treatment of osteoporoses]. Nihon rinsho. Japanese journal of clinical medicine, 2009, Volume: 67, Issue:5 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Evidence-Based Medicine; Femoral Fractu	2009
[Drug therapy of secondary osteoporosis: glucocorticoid-induced osteoporosis]. Nihon rinsho. Japanese journal of clinical medicine, 2009, Volume: 67, Issue:5 Topics: Alendronate; Bone Density Conservation Agents; Cholecalciferol; Clinical Trials as Topic; Diphosphon	2009
[Measurement of bone mineral density is necessary for monitoring of bisphosphonate treatment]. Clinical calcium, 2011, Volume: 21, Issue:1 Topics: Alendronate; Biomarkers; Bone Density; Diphosphonates; Drug Monitoring; Fractures, Spontaneous; Huma	2011
Vertebral fracture risk and alendronate effects on osteoporosis assessed by a computed tomography-based nonlinear finite element method. Journal of bone and mineral metabolism, 2011, Volume: 29, Issue:6 Topics: Alendronate; Female; Finite Element Analysis; Humans; Osteoporosis, Postmenopausal; Spinal Fractures	2011
Osteoporosis in elderly: prevention and treatment. Clinics in geriatric medicine, 2002, Volume: 18, Issue:3 Topics: Aged; Alendronate; Etidronic Acid; Exercise; Female; Fractures, Bone; Hormone Replacement Therapy; H	2002
[Osteoporosis: prevention of bone loss and fractures]. MMW Fortschritte der Medizin, 2002, Nov-28, Volume: 144, Issue:48 Topics: Absorptiometry, Photon; Aged; Aged, 80 and over; Alendronate; Bone Diseases, Metabolic; Diagnosis, D	2002
Risedronate prevents hip fractures, but who should get therapy? Cleveland Clinic journal of medicine, 2002, Volume: 69, Issue:12 Topics: Accidental Falls; Aged; Aged, 80 and over; Alendronate; Bone Density; Calcium Channel Blockers; Etid	2002
Aging bone and osteoporosis: strategies for preventing fractures in the elderly. Archives of internal medicine, 2003, Oct-13, Volume: 163, Issue:18 Topics: Aged; Alendronate; Calcium Channel Blockers; Diphosphonates; Estrogen Replacement Therapy; Etidronic	2003
[AOS-100]. Nihon rinsho. Japanese journal of clinical medicine, 2004, Volume: 62 Suppl 2 Topics: Absorptiometry, Photon; Alendronate; Bone Density; Etidronic Acid; Humans; Mass Screening; Osteoporo	2004
[Fracture Intervention Trial I and II(alendronate)]. Nihon rinsho. Japanese journal of clinical medicine, 2004, Volume: 62 Suppl 2 Topics: Activities of Daily Living; Alendronate; Back Pain; Controlled Clinical Trials as Topic; Humans; Ost	2004
[Treatment of osteoporosis combined with a bisphosphonate and vitamin D3]. Nihon rinsho. Japanese journal of clinical medicine, 2004, Volume: 62 Suppl 2 Topics: Alendronate; Bone Density; Cholecalciferol; Drug Therapy, Combination; Etidronic Acid; Humans; Multi	2004
Rapid prevention of vertebral fractures associated with osteoporosis. Orthopedics, 2005, Volume: 28, Issue:3 Topics: Aged; Alendronate; Calcitonin; Clinical Trials as Topic; Diphosphonates; Estrogens; Female; Glucocor	2005
Does alendronate reduce the risk of fracture in men? A meta-analysis incorporating prior knowledge of anti-fracture efficacy in women. BMC musculoskeletal disorders, 2005, Jul-11, Volume: 6 Topics: Adult; Aged; Alendronate; Bone Density Conservation Agents; Female; Fractures, Bone; Humans; Male; M	2005
[Current research in adequate treatment by Osteoporosis Research Group]. Clinical calcium, 2006, Volume: 16, Issue:9 Topics: Alendronate; Bone Density Conservation Agents; Cholecalciferol; Clinical Trials as Topic; Drug Thera	2006
[Drug treatment of postmenopausal osteoporosis. What's New in 2006]. Presse medicale (Paris, France : 1983), 2006, Volume: 35, Issue:10 Pt 2 Topics: Absorptiometry, Photon; Adult; Age Factors; Aged; Aged, 80 and over; Alendronate; Body Mass Index; B	2006
[Osteoporosis: Optimizing treatment strategy]. Presse medicale (Paris, France : 1983), 2006, Volume: 35, Issue:10 Pt 2 Topics: Age Factors; Aged; Alendronate; Biomarkers; Bone Density; Bone Density Conservation Agents; Calcium,	2006
[Glucocorticoid-induced osteoporosis]. Polskie Archiwum Medycyny Wewnetrznej, 2007, Volume: 117, Issue:8 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Calcium; Diphosphonates; Female; Fractu	2007
[Efficacy and tolerability of once-weekly administration of 35 mg alendronate and 17.5 mg risedronate]. Nihon rinsho. Japanese journal of clinical medicine, 2007, Nov-28, Volume: 65 Suppl 9 Topics: Alendronate; Bone Density; Bone Density Conservation Agents; Bone Remodeling; Clinical Trials as Top	2007
[Diagnosis, clinical feature and treatment of glucocorticoid-induced osteoporosis in patients with rheumatoid arthritis]. Nihon rinsho. Japanese journal of clinical medicine, 2007, Nov-28, Volume: 65 Suppl 9 Topics: Alendronate; Arthritis, Rheumatoid; Bone Density Conservation Agents; Glucocorticoids; Humans; Osteo	2007
Alendronate for the primary and secondary prevention of osteoporotic fractures in postmenopausal women. The Cochrane database of systematic reviews, 2008, Jan-23, Issue:1 Topics: Alendronate; Bone Density Conservation Agents; Female; Fractures, Bone; Fractures, Spontaneous; Hip	2008
Biomechanics of osteoporosis and vertebral fracture. Spine, 1997, Dec-15, Volume: 22, Issue:24 Suppl Topics: Aged; Aged, 80 and over; Aging; Alendronate; Animals; Bone Density; Female; Humans; Middle Aged; Ost	1997
Alendronate for osteoporosis. Safe and efficacious nonhormonal therapy. Canadian family physician Medecin de famille canadien, 1998, Volume: 44 Topics: Adult; Aged; Alendronate; Bone and Bones; Bone Density; Calcification, Physiologic; Clinical Trials,	1998
A risk-benefit assessment of alendronate in the treatment of involutional osteoporosis. Drug safety, 1998, Volume: 19, Issue:2 Topics: Aged; Alendronate; Bone and Bones; Bone Density; Female; Fractures, Bone; Humans; Osteoporosis; Spin	1998
Bisphosphonates in the treatment of osteoporosis. Principles and efficacy. Annales de medecine interne, 2000, Volume: 151, Issue:6 Topics: Administration, Oral; Alendronate; Animals; Bone and Bones; Bone Density; Calcium Channel Blockers;	2000
[Bisphosphonate treatment prevents hip fractures in 70-79 year old women with osteoporotic vertebral fractures]. Nederlands tijdschrift voor geneeskunde, 2001, Jul-14, Volume: 145, Issue:28 Topics: Age Factors; Aged; Alendronate; Bone Density; Calcium Channel Blockers; Diphosphonates; Etidronic Ac	2001
Improvement in spine bone density and reduction in risk of vertebral fractures during treatment with antiresorptive drugs. The American journal of medicine, 2002, Volume: 112, Issue:4 Topics: Alendronate; Bone Density; Bone Resorption; Female; Fractures, Spontaneous; Humans; Logistic Models;	2002
[Bisphosphonates: pharmacology and use in the treatment of osteoporosis]. Nihon rinsho. Japanese journal of clinical medicine, 2002, Volume: 60 Suppl 3 Topics: Alendronate; Bone Density; Bone Remodeling; Clinical Trials as Topic; Diphosphonates; Etidronic Acid	2002
[Alendronate in the treatment of osteoporosis]. Nihon rinsho. Japanese journal of clinical medicine, 2002, Volume: 60 Suppl 3 Topics: Alendronate; Bone Density; Bone Resorption; Clinical Trials as Topic; Femoral Neck Fractures; Fractu	2002

alendronate and Hangman Fracture

Research Excerpts

Research

Studies (175)

Authors

Clinical Trials (20)

Trial Overview

Trial Outcomes

Number of Participants With New Vertebral Fractures at 18 Months

Number of Participants With Non-vertebral Fractures at 18 Months

Number of Treatment-Emergent Adverse Events Associated With Hypercalcemia at 18 Months

Percent Change in Bone Mineral Density (BMD) of Femoral Neck From Baseline to Month 18

Percent Change in Bone Mineral Density (BMD) of Lumbar Spine From Baseline to 18 Months

Percent Change in Bone Mineral Density (BMD) of Total Hip From Baseline to Month 18

Kaplan-Meier Estimated Event Rate of the First Incident of Nonvertebral Fracture Since Study BA058-05-003 Baseline (Data From Studies BA058-05-005 and BA058-05-003 Combined)

Number of Participants With ≥1 New Vertebral Fracture Since Study BA058-05-003 Baseline

Number of Participants With a Clinically Notable Coagulation Laboratory Value (Data From Study BA058-05-005 Only)

Number of Participants With a Nonvertebral Fracture Since Study BA058-05-003 Baseline (Data From Studies BA058-05-005 and BA058-05-003 Combined)

Percent Change From Study BA058-05-003 Baseline in Femoral Neck BMD at Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Percent Change From Study BA058-05-003 Baseline in Lumbar Spine BMD at Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Percent Change From Study BA058-05-003 Baseline in Total Hip BMD at Study BA058-05-005 Month 6 (Study BA058-05-003 Month 25)

Number of Participants With a Clinically Notable Hematology Laboratory Value (Data From Study BA058-05-005 Only)

Number of Participants With a Clinically Notable Serum Chemistry Laboratory Value (Data From Study BA058-05-005 Only)

Number of Participants With a Clinically Notable Urine Laboratory Value (Data From Study BA058-05-005 Only)

Number of Participants With Treatment Emergent Adverse Events (TEAEs) (Data From Study BA058-05-005 Only)

Percent Change From Baseline in Bone Mineral Density at the Femoral Neck at Month 12

Percent Change From Baseline in Bone Mineral Density at the Lumbar Spine at Month 12

Percent Change From Baseline in Bone Mineral Density at the Lumbar Spine at Month 24

Percent Change From Baseline in Bone Mineral Density at the Total Hip at Month 12

Percent Change From Baseline in Bone Mineral Density of the Femoral Neck at at Month 24

Percent Change From Baseline in Bone Mineral Density of the Femoral Neck at Month 36

Percent Change From Baseline in Bone Mineral Density of the Lumbar Spine at Month 36

Percent Change From Baseline in Bone Mineral Density of the Total Hip at Month 24

Percent Change From Baseline in Bone Mineral Density of the Total Hip at Month 36

Percentage of Participants With a Clinical Fracture at the Primary Analysis

Percentage of Participants With a Clinical Fracture Through Month 12

Percentage of Participants With a Clinical Fracture Through Month 24

Percentage of Participants With a Clinical Vertebral Fracture Through Month 12

Percentage of Participants With a Clinical Vertebral Fracture Through Month 24

Percentage of Participants With a Hip Fracture at the Primary Analysis

Percentage of Participants With a Hip Fracture Through Month 12

Percentage of Participants With a Hip Fracture Through Month 24

Percentage of Participants With a Major Nonvertebral Fracture at the Primary Analysis

Percentage of Participants With a Major Osteoporotic Fracture Through Month 12

Percentage of Participants With a New or Worsening Vertebral Fracture Through Month 24

Percentage of Participants With a Nonvertebral Fracture at the Primary Analysis

Percentage of Participants With a Nonvertebral Fracture Through Month 12

Percentage of Participants With a Nonvertebral Fracture Through Month 24

Percentage of Participants With Any Fracture at the Primary Analysis

Percentage of Participants With Any Fracture Through Month 12

Percentage of Participants With Multiple New or Worsening Vertebral Fractures Through Month 24

Percentage of Participants With New Vertebral Fractures Through Month 12

Percentage of Participants With New Vertebral Fractures Through Month 24

Change From Baseline in Bone Formation Rate/Bone Surface (BFR/BS) in the Cancellous Envelope at Month 3

Change From Baseline in Mineralizing Surface/Bone Surface (MS/BS) in the Cancellous Envelope at Month 3

Change in Serum Carboxy-Terminal Cross-Linking Telopeptide of Type I Collagen (s-CTX) From Baseline at Month 1 and Month 3

Change in Serum Procollagen Type I N-terminal Propeptide (s-P1NP) From Baseline at Month 1 and Month 3

Number of Participants in Which CTX Increased Above the Least Significant Change

If Baseline Bone Turnover Markers at the Time of Alendronate Discontinuation Predict Changes in BMD After One and Two Years.

If Carboxy-terminal Collagen Crosslinks (CTX) Three and Six Months After Stopping Alendronate Predicted TH BMD (Total Hip BMD) Loss Above the Least Significant Change at Month 12 at the Individual Level.

Percent Change in Bone Turnover Markers Measured Three and Six Months After Stopping Alendronate Treatment and BMD After One and Two Years

The Number of Participants Who Lost BMD Beyond the Least Significant Change (LSC) at the Lumbar Spine and Total Hip.

Changes in Bone Mineral Density of the Distal 1/3 Radius.

Changes in Bone Mineral Density of the Femoral Neck.

Changes in Bone Mineral Density of the Forearm.

Changes in Bone Mineral Density of the Lumbar Spine.

Changes in Bone Mineral Density of the Total Hip.

1,25 Vitamin D

24 Hour Urine Calcium

Carboxy-terminal Telopeptides of Collagen-1 (CTX)

Fractional Excretion of Calcium

Procallagen-1 Amino-terminal Peptide (P1NP)

Serum Phosphorous

Total Serum Calcium (mg/dl)

Tubular Maximum for Phosphorous/Glomerular Filtration Rate (TMP/GFR)

Change From Baseline in Bone Mineral Density (BMD) Measured by Dual-Energy X-ray Absorptiometry (DXA) and Instant Vertebral Assessment (IVA) Scan

Change From Baseline in Disease Activity Score 28 Joint Count C-Reactive Protein (DAS-28 CRP)

Change From Baseline in Joint Erosion Volume Measured by 3-Dimensional Computed Tomography (3D CT) Scan

Reviews

Trials