Clenbuterol Treatment Is Safe and Associated With Slowed Disease Progression in a Small Open-Label Trial in Patients With Amyotrophic Lateral Sclerosis.

Q3 Medicine
Xiaoyan Li, Dwight D Koeberl, Michael W Lutz, Richard Bedlack
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Abstract

Objective: Clenbuterol, a beta-agonist, has plausible mechanisms for treating amyotrophic lateral sclerosis (ALS). In this highly inclusive open-label trial (NCT04245709), we aimed to study the safety and efficacy of clenbuterol in patients with ALS.

Methods: All participants received clenbuterol starting at 40 μg daily and increased to 80 μg twice daily. Outcomes included safety, tolerability, ALS Functional Rating Score (ALSFRS-R) progression, forced vital capacity (FVC) progression, and myometry. ALSFRS-R and FVC slopes measured during treatment were compared with slopes before treatment (calculated by assuming ALSFRS-R was 48 and FVC was 100% at ALS onset).

Results: The 25 participants had a mean age of 59, mean disease duration of 43 months, ALSFRS-R score at enrollment 34, and FVC at enrollment 77%. Forty-eight percent were female, 68% were taking riluzole, and none were taking edaravone. Two participants experienced severe adverse events, neither related to the study. Twenty-four participants experienced adverse events, most commonly tremors/jitters, cramps/spasms, insomnia, and stiffness/spasticity. Fourteen participants withdrew early from the trial, 13 due to adverse events. Patients who withdrew early were significantly older and more likely to be male. Per-protocol and intention-to-treat analyses showed meaningfully slower ALSFRS-R and FVC progression during treatment. Hand grip dynamometry and myometry changes were highly variable between participants; most declined slowly, but some showed improvements.

Conclusions: Clenbuterol was safe but less tolerable at the doses we selected compared with an earlier Italian case series. Consistent with that series, our study suggested benefits on ALS progression. However, the latter result should be interpreted with caution as our study is limited by small sample size, large drop out, lack of randomization, and blinding and placebo controls. A larger, more traditional trial now seems warranted.

在肌萎缩性侧索硬化症患者的小型开放标签试验中,盐酸克仑特罗治疗是安全的,并与疾病进展减缓有关。
目的:盐酸克仑特罗是一种β激动剂,具有治疗肌萎缩性侧索硬化症(ALS)的合理机制。在这项高度包容性的开放标签试验(NCT04245709)中,我们旨在研究盐酸克仑特罗在ALS患者中的安全性和有效性。方法:所有受试者服用盐酸克仑特罗,从每天40 μg开始,逐渐增加到80 μg,每天2次。结果包括安全性、耐受性、ALS功能评分(ALSFRS-R)进展、用力肺活量(FVC)进展和肌力测定。将治疗期间测量的ALSFRS-R和FVC斜率与治疗前的斜率进行比较(假设ALS发病时ALSFRS-R为48,FVC为100%)。结果:25名参与者的平均年龄为59岁,平均病程为43个月,入组时ALSFRS-R评分为34,入组时FVC为77%。48%是女性,68%服用利鲁唑,没有人服用依达拉奉。两名参与者经历了严重的不良事件,与研究无关。24名参与者经历了不良事件,最常见的是震颤/颤抖,痉挛/痉挛,失眠和僵硬/痉挛。14名受试者提前退出试验,13名因不良事件退出。早期退出治疗的患者明显年龄更大,而且更有可能是男性。按方案和意向治疗分析显示,治疗期间ALSFRS-R和FVC进展明显减慢。参与者之间的握力测量和肌力测量变化差异很大;大多数人下降缓慢,但有些人有所改善。结论:与早期意大利病例系列相比,我们选择的剂量盐酸克仑特罗是安全的,但耐受性较差。与该系列一致,我们的研究表明对ALS进展有益。然而,后一个结果应该谨慎解释,因为我们的研究受到样本量小、退出量大、缺乏随机化以及盲法和安慰剂对照的限制。现在看来,更大规模、更传统的试验是有必要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
1.60
自引率
0.00%
发文量
64
期刊介绍: Journal of Clinical Neuromuscular Disease provides original articles of interest to physicians who treat patients with neuromuscular diseases, including disorders of the motor neuron, peripheral nerves, neuromuscular junction, muscle, and autonomic nervous system. Each issue highlights the most advanced and successful approaches to diagnosis, functional assessment, surgical intervention, pharmacologic treatment, rehabilitation, and more.
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