BPS804 Anti-Sclerostin Antibody in Adults With Moderate Osteogenesis Imperfecta: Results of a Randomized Phase 2a Trial

被引:114
作者
Glorieux, Francis H. [1 ,2 ]
Devogelaer, Jean-Pierre [3 ]
Durigova, Michaela [1 ,2 ]
Goemaere, Stefan [4 ]
Hemsley, Sarah [5 ]
Jakob, Franz [6 ]
Junker, Uwe [5 ]
Ruckle, Jon [7 ]
Seefried, Lothar [6 ]
Winkle, Peter J. [8 ]
机构
[1] Shriners Hosp Children, Res Ctr, 1003 Decarie Blvd, Montreal, PQ H4A 0A9, Canada
[2] McGill Univ, Montreal, PQ, Canada
[3] Catholic Univ Louvain, St Luc Univ Hosp, Brussels, Belgium
[4] Ghent Univ Hosp, Ghent, Belgium
[5] Novartis Inst BioMed Res, Basel, Switzerland
[6] Univ Wurzburg, Orthoped Ctr Musculoskeletal Res Expt & Clin Oste, Dept Orthoped, Wurzburg, Germany
[7] Pacific Pharma Grp, Tacoma, WA USA
[8] Anaheim Clin Trials, Anaheim, CA USA
来源
JOURNAL OF BONE AND MINERAL RESEARCH | 2017年 / 32卷 / 07期
关键词
ANTI-SCLEROSTIN ANTIBODY; CLINICAL TRIALS; DXA; OSTEOGENESIS IMPERFECTA; WNT; BONE-MINERAL DENSITY; PLACEBO-CONTROLLED TRIAL; BRTL/+ MOUSE MODEL; INTRAVENOUS PAMIDRONATE; BISPHOSPHONATE THERAPY; ORAL BISPHOSPHONATES; POSTMENOPAUSAL WOMEN; FRACTURE RATE; CHILDREN; HISTOMORPHOMETRY;
D O I
10.1002/jbmr.3143
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
This 21-week, open-label, phase 2a trial aimed to evaluate the pharmacodynamics and safety of multiple, escalating infusions of BPS804, a neutralizing, anti-sclerostin antibody, in adults with moderate osteogenesis imperfecta (OI). Patients received BPS804 (three escalating doses each separated by 2 weeks [5, 10, and 20 mg/kg]) or no treatment (reference group). The primary efficacy endpoints were mean changes from baseline to day 43 in: procollagen type 1 N-terminal propeptide (P1NP), procollagen type 1 C-terminal propeptide (P1CP), bone-specific alkaline phosphatase (BSAP), osteocalcin (OC), and type 1 collagen cross-linked C-telopeptide (CTX-1). Mean change from baseline to day 141 in lumbar spine areal bone mineral density (aBMD) was also assessed. BPS804 safety and tolerability were assessed every 2 weeks. Overall, 14 adults were enrolled (BPS804 group: n = 9, mean age 30.7 years, mean aBMD Z-score -2.6; reference group, n = 5, mean age 27.4 years, mean aBMD Z-score -2.2). In the BPS804 group, P1NP, P1CP, BSAP, and OC were increased by 84% (p< 0.001), 53% (p = 0.003), 59% (p< 0.001), and 44% (p = 0.012), respectively, versus baseline (reference: P1NP, +6% [p = 0.651]; P1CP, +5% [p = 0.600]; BSAP, -13% [p = 0.582]; OC, -19% [p = 0.436]). BPS804 treatment downregulated CTX-1 by 44% from baseline (reference: -7%; significance was not tested for this biomarker), and increased aBMD by 4% (p = 0.038; reference group: +1%; p = 0.138). BPS804 was generally well tolerated. There were 32 adverse events reported in nine patients; none was suspected to be treatment-related. There were no treatment-related fractures. BPS804 stimulates bone formation, reduces bone resorption, and increases lumbar spine aBMD in adults with moderate OI. This paves the way for a longerterm, phase 3 trial into the efficacy, safety, and tolerability of BPS804 in patients with OI. (C) 2017 American Society for Bone and Mineral Research.
引用
收藏
页码:1496 / 1504
页数:9
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