新型组织蛋白酶 K 抑制剂在骨关节炎中的疾病修饰作用:一项随机对照试验。
Disease-Modifying Effects of a Novel Cathepsin K Inhibitor in Osteoarthritis: A Randomized Controlled Trial.
机构信息
Leeds Institute of Rheumatic and Musculoskeletal Medicine, University of Leeds and NIHR Leeds Biomedical Research Centre, Leeds, United Kingdom (P.G.C., S.R.K.).
Imorphics, Manchester, United Kingdom (M.A.B., A.B., G.G.).
出版信息
Ann Intern Med. 2020 Jan 21;172(2):86-95. doi: 10.7326/M19-0675. Epub 2019 Dec 31.
BACKGROUND
MIV-711 is a novel selective cathepsin K inhibitor with beneficial effects on bone and cartilage in preclinical osteoarthritis models.
OBJECTIVE
To evaluate the efficacy, safety, and tolerability of MIV-711 in participants with symptomatic, radiographic knee osteoarthritis.
DESIGN
26-week randomized, double-blind, placebo-controlled phase 2a study with a 26-week open-label safety extension substudy. (EudraCT: 2015-003230-26 and 2016-001096-73).
SETTING
Six European sites.
PARTICIPANTS
244 participants with primary knee osteoarthritis, Kellgren-Lawrence grade 2 or 3, and pain score of 4 to 10 on a numerical rating scale (NRS).
INTERVENTION
MIV-711, 100 (n = 82) or 200 (n = 81) mg daily, or matched placebo (n = 77). Participants (46 who initially received 200 mg/d and 4 who received placebo) received 200 mg of MIV-711 daily during the extension substudy.
MEASUREMENTS
The primary outcome was change in NRS pain score. The key secondary outcome was change in bone area on magnetic resonance imaging (MRI). Other secondary end points included cartilage thickness on quantitative MRI and type I and II collagen C-telopeptide biomarkers. Outcomes were assessed over 26 weeks.
RESULTS
Changes in NRS pain scores with MIV-711 were not statistically significant (placebo, -1.4; MIV-711, 100 mg/d, -1.7; MIV-711, 200 mg/d, -1.5). MIV-711 significantly reduced medial femoral bone area progression (P = 0.002 for 100 mg/d and 0.004 for 200 mg/d) and medial femoral cartilage thinning (P = 0.023 for 100 mg/d and 0.125 for 200 mg/d) versus placebo and substantially reduced bone and cartilage biomarker levels. Nine serious adverse events occurred in 6 participants (1 in the placebo group, 3 in the 100 mg group, and 2 in the 200 mg group); none were considered to be treatment-related.
LIMITATION
The trial was relatively short.
CONCLUSION
MIV-711 was not more effective than placebo for pain, but it significantly reduced bone and cartilage progression with a reassuring safety profile. This treatment may merit further evaluation as a disease-modifying osteoarthritis drug.
PRIMARY FUNDING SOURCE
Medivir.
背景
MIV-711 是一种新型的组织蛋白酶 K 选择性抑制剂,在临床前骨关节炎模型中对骨骼和软骨具有有益作用。
目的
评估 MIV-711 对有症状、放射照相膝关节骨关节炎患者的疗效、安全性和耐受性。
设计
26 周随机、双盲、安慰剂对照的 2a 期研究,有 26 周的开放性安全性扩展亚研究。(EudraCT:2015-003230-26 和 2016-001096-73)。
地点
欧洲六个地点。
参与者
244 名原发性膝关节骨关节炎患者,Kellgren-Lawrence 分级 2 或 3 级,数字评分量表(NRS)上疼痛评分为 4 至 10。
干预措施
MIV-711,每日 100(n=82)或 200 mg(n=81),或匹配的安慰剂(n=77)。参与者(最初接受 200 mg/d 的 46 人和接受安慰剂的 4 人)在扩展亚研究中接受 MIV-711 每日 200 mg。
测量
主要结局是 NRS 疼痛评分的变化。关键次要结局是磁共振成像(MRI)上骨面积的变化。其他次要终点包括定量 MRI 上的软骨厚度和 I 型和 II 型胶原 C 端肽生物标志物。在 26 周内评估结果。
结果
MIV-711 治疗的 NRS 疼痛评分变化无统计学意义(安慰剂,-1.4;MIV-711,100 mg/d,-1.7;MIV-711,200 mg/d,-1.5)。MIV-711 显著降低内侧股骨骨面积进展(100 mg/d 时 P=0.002,200 mg/d 时 P=0.004)和内侧股骨软骨变薄(100 mg/d 时 P=0.023,200 mg/d 时 P=0.125),与安慰剂相比,并且大大降低了骨和软骨生物标志物水平。6 名参与者发生 9 例严重不良事件(安慰剂组 1 例,100 mg 组 3 例,200 mg 组 2 例);均认为与治疗无关。
限制
试验相对较短。
结论
与安慰剂相比,MIV-711 对疼痛的效果并不更有效,但它显著减少了骨骼和软骨的进展,具有可靠的安全性。这种治疗方法可能值得进一步评估作为一种治疗骨关节炎的药物。
主要资金来源
Medivir。
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