Brown Jacques P, Prince Richard L, Deal Chad, Recker Robert R, Kiel Douglas P, de Gregorio Luiz H, Hadji Peyman, Hofbauer Lorenz C, Alvaro-Gracia Jose M, Wang Huei, Austin Matthew, Wagman Rachel B, Newmark Richard, Libanati Cesar, San Martin Javier, Bone Henry G
Laval University, Le Centre Hospitalier Universitaire de Québec, Quebec City, Québec, Canada.
J Bone Miner Res. 2009 Jan;24(1):153-61. doi: 10.1359/jbmr.0809010.
Denosumab is a fully human monoclonal antibody that inhibits bone resorption by neutralizing RANKL, a key mediator of osteoclast formation, function, and survival. This phase 3, multicenter, doubleblind study compared the efficacy and safety of denosumab with alendronate in postmenopausal women with low bone mass. One thousand one hundred eighty-nine postmenopausal women with a T-score <or= -2.0 at the lumbar spine or total hip were randomized 1:1 to receive subcutaneous denosumab injections (60 mg every 6 mo [Q6M]) plus oral placebo weekly (n = 594) or oral alendronate weekly (70 mg) plus subcutaneous placebo injections Q6M (n = 595). Changes in BMD were assessed at the total hip, femoral neck, trochanter, lumbar spine, and one-third radius at 6 and 12 mo and in bone turnover markers at months 1, 3, 6, 9, and 12. Safety was evaluated by monitoring adverse events and laboratory values. At the total hip, denosumab significantly increased BMD compared with alendronate at month 12 (3.5% versus 2.6%; p < 0.0001). Furthermore, significantly greater increases in BMD were observed with denosumab treatment at all measured skeletal sites (12-mo treatment difference: 0.6%, femoral neck; 1.0%, trochanter; 1.1%, lumbar spine; 0.6%, one-third radius; p <or= 0.0002 all sites). Denosumab treatment led to significantly greater reduction of bone turnover markers compared with alendronate therapy. Adverse events and laboratory values were similar for denosumab- and alendronate-treated subjects. Denosumab showed significantly larger gains in BMD and greater reduction in bone turnover markers compared with alendronate. The overall safety profile was similar for both treatments.
地诺单抗是一种全人源单克隆抗体,通过中和核因子κB受体活化因子配体(RANKL)来抑制骨吸收,RANKL是破骨细胞形成、功能和存活的关键介质。这项3期、多中心、双盲研究比较了地诺单抗与阿仑膦酸钠在低骨量绝经后女性中的疗效和安全性。1189名腰椎或全髋部T值≤ -2.0的绝经后女性按1:1随机分组,分别接受皮下注射地诺单抗(每6个月60mg [Q6M])加每周口服安慰剂(n = 594),或每周口服阿仑膦酸钠(70mg)加每6个月皮下注射安慰剂(n = 595)。在6个月和12个月时评估全髋、股骨颈、大转子、腰椎和桡骨远端三分之一处的骨密度变化,在第1、3、6、9和12个月评估骨转换标志物变化。通过监测不良事件和实验室指标评估安全性。在全髋部,地诺单抗在第12个月时与阿仑膦酸钠相比显著增加了骨密度(3.5%对2.6%;p < 0.0001)。此外,在所有测量的骨骼部位,地诺单抗治疗均观察到骨密度显著更大幅度的增加(12个月治疗差异:股骨颈0.6%;大转子1.0%;腰椎1.1%;桡骨远端三分之一处0.6%;所有部位p≤ 0.0002)。与阿仑膦酸钠治疗相比,地诺单抗治疗导致骨转换标志物显著更大幅度的降低。地诺单抗治疗组和阿仑膦酸钠治疗组的不良事件和实验室指标相似。与阿仑膦酸钠相比,地诺单抗显示出骨密度显著更大的增加和骨转换标志物更大幅度的降低。两种治疗的总体安全性概况相似。
