Department of Medicine III, Center for Healthy Aging and Division of Endocrinology, Diabetes, and Bone Disease, Universitätsklinikum Carl Gustav Carus der Technischen Universität Dresden, Dresden, Germany.
Department of Orthopedics and Traumatology, Ziekenhuis Oost-Limburg, Schiepse Bos, Genk, Belgium.
Lancet Healthy Longev. 2021 May;2(5):e263-e274. doi: 10.1016/S2666-7568(21)00084-2.
Older adult patients (ie, those aged ≥60 years) undergoing surgery for hip fracture repair frequently experience loss of muscle mass and strength due to poor mobility and delayed functional recovery. No proven treatment is currently available to enhance recovery of physical function in this growing patient population. This study aimed to investigate whether bimagrumab, a human monoclonal antibody targeting activin type 2 receptors, can improve post-surgical recovery.
This multicentre, double-blind, randomised, parallel-group, placebo-controlled, phase 2a/b trial was done at 50 clinical research centres in 18 countries. Participants aged 60 years or older with a body-mass index of 15-35 kg/m who had undergone internal fixation or hemiarthroplasty for a proximal femoral fracture (confirmed by radiography) in the previous 6 weeks were eligible. Patients with a history of a high-energy subtrochanteric fracture or any other lower limb fracture in the past 6 months, or any major surgery of the lower limbs in the past 3 months were excluded. Participants were randomly assigned (2:1:2:2) via interactive response technology to receive intravenous treatment with placebo, bimagrumab 70 mg, bimagrumab 210 mg, or bimagrumab 700 mg every 4 weeks for 24 weeks. Participants, investigators, site personnel, and study sponsor personnel in participating countries were masked to treatment assignment. The primary endpoint was the change from baseline in total lean body mass, measured by dual-energy x-ray absorptiometry, at week 24 in the full analysis set, which included all randomised participants who had received at least one dose of the assigned treatment. Key secondary endpoints included changes in habitual gait speed (measured in m/s) and short physical performance battery score between baseline and 24 weeks. Safety and tolerability were assessed by recording adverse events and vital signs on weeks 4, 8, 12, 24, and 48, and by laboratory assessments and electrocardiography at the screening visit and on days 1, 84, and 168. Safety was assessed in all randomised participants who had received at least one dose of study drug, analysed according to treatment received. This study was registered with ClinicalTrials.gov, NCT02152761.
Between Sept 16, 2014, and Dec 15, 2017, 384 patients were screened, of whom 250 patients were enrolled and randomly assigned to the placebo group (n=72), the bimagrumab 70 mg group (n=34), the bimagrumab 210 mg group (n=69), or the bimagrumab 700 mg group (n=75). A total of 207 (83%) participants completed the 24-week treatment period. There was a significant absolute increase in lean body mass from baseline compared with placebo (0·2 kg [SD 2·0]) in the bimagrumab 210 mg group (1·9 kg [1·7]; p<0·0001) and in the bimagrumab 700 mg group 2·8 kg [2·2]; p<0·0001) but not in the bimagrumab 70 mg group (0·6 kg [SD 2·2]; significance not assessed). Changes in habitual gait speed and short physical performance battery scores between baseline and week 24 were not significantly different across the treatment groups, suggesting no enhancement of physical recovery with bimagrumab over placebo. Bimagrumab was safe and well tolerated. The most frequently reported treatment-emergent adverse events were falls (six [18%] of 34 participants in the bimagrumab 70 mg group; 12 [17%] of 69 participants in the bimagrumab 210 mg group; 14 [19%] of 75 participants in the bimagrumab 700 mg group; and 13 [18%] of 72 participants in the placebo group), muscle spasms (two [6%] in the bimagrumab 70 mg group; 17 [25%] in the bimagrumab 210 mg group; 12 [16%] in the bimagrumab 700 mg group; and six [8%] in the placebo group), and arthralgia (five [15%] in the bimagrumab 70 mg group; six [9%] in the bimagrumab 210 mg group; nine [12%] in the bimagrumab 700 mg group; and five [7%] in the placebo group). Six deaths were reported during the study, none of which were considered by investigators as related to the study drug.
Bimagrumab treatment for 24 weeks led to dose-dependent, significant increases in lean body mass in older patients recovering from hip fracture surgery when compared with placebo. However, no functional benefit was observed in recovery of mobility or lower extremity function following bimagrumab treatment compared with placebo.
Novartis Pharma.
接受髋关节骨折修复手术的老年患者(即年龄≥60 岁的患者)由于活动能力差和功能恢复延迟,常出现肌肉质量和力量损失。目前尚无已证实的治疗方法可增强这一不断增长的患者群体的身体功能恢复。本研究旨在探讨靶向激活素型 2 受体的人单克隆抗体 bimagrumab 是否可以改善手术后的恢复情况。
这是一项在 18 个国家的 50 个临床研究中心进行的多中心、双盲、随机、平行分组、安慰剂对照、2a/b 期临床试验。符合条件的参与者为年龄在 60 岁或以上、身体质量指数为 15-35 kg/m2 且在过去 6 周内通过影像学检查确诊为股骨近端骨折(经影像学检查证实)的患者。有高能量转子下骨折或过去 6 个月内任何其他下肢骨折病史,或过去 3 个月内有下肢大手术史的患者被排除在外。参与者通过交互式反应技术随机分配(2:1:2:2),接受安慰剂、bimagrumab 70mg、bimagrumab 210mg 或 bimagrumab 700mg 静脉治疗,每 4 周 1 次,共 24 周。参与者、研究者、现场工作人员和参与国家的研究赞助商人员对治疗分配情况均不知情。主要终点是在 24 周时,根据基线情况,使用双能 X 射线吸收法测量的总瘦体质量变化,在全分析集(包括至少接受过 1 次分配治疗的所有随机参与者)中进行分析。关键次要终点包括习惯性步速(以 m/s 为单位)和短程体能测试电池评分的变化。通过在第 4、8、12、24 和 48 周记录不良事件和生命体征,以及在筛选时和第 1、84 和 168 天进行实验室评估和心电图检查,评估安全性和耐受性。在至少接受过 1 次研究药物治疗的所有随机参与者中,按照接受的治疗进行安全性分析。本研究在 ClinicalTrials.gov 上注册,编号为 NCT02152761。
2014 年 9 月 16 日至 2017 年 12 月 15 日期间,共有 384 名患者接受了筛查,其中 250 名患者入组并随机分配至安慰剂组(n=72)、bimagrumab 70mg 组(n=34)、bimagrumab 210mg 组(n=69)或 bimagrumab 700mg 组(n=75)。共有 207 名(83%)参与者完成了 24 周的治疗期。与安慰剂组相比,bimagrumab 210mg 组(1.9kg[1.7];p<0.0001)和 bimagrumab 700mg 组(2.8kg[2.2];p<0.0001)的瘦体质量有显著的绝对增加,但 bimagrumab 70mg 组(0.6kg[2.2];无显著差异)没有增加。从基线到第 24 周,习惯性步速和短程体能测试电池评分的变化在各治疗组之间没有显著差异,表明 bimagrumab 对安慰剂没有增强身体恢复。bimagrumab 是安全且耐受良好的。最常报告的治疗相关不良事件是跌倒(bimagrumab 70mg 组 34 名参与者中有 6 名[18%];bimagrumab 210mg 组 69 名参与者中有 12 名[17%];bimagrumab 700mg 组 75 名参与者中有 14 名[19%];安慰剂组 72 名参与者中有 13 名[18%])、肌肉痉挛(bimagrumab 70mg 组 2 名[6%];bimagrumab 210mg 组 17 名[25%];bimagrumab 700mg 组 12 名[16%];安慰剂组 6 名[8%])和关节痛(bimagrumab 70mg 组 5 名[15%];bimagrumab 210mg 组 6 名[9%];bimagrumab 700mg 组 9 名[12%];安慰剂组 5 名[7%])。研究期间报告了 6 例死亡,研究者认为均与研究药物无关。
与安慰剂相比,bimagrumab 治疗 24 周可导致髋部骨折手术后老年患者的瘦体质量显著增加,与安慰剂相比,bimagrumab 治疗与安慰剂相比,在恢复移动性或下肢功能方面没有观察到功能益处。
诺华制药。
