Safety and tolerability of phenylbutyrate in inclusion body myositis

D. Jabari, A. Heim, A. Ciersdorff, Heather Wilkins, Abdulbaki Agbas, E. Kosa, Suzanne Hunt, M. Pasnoor, M. Dimachkie, R. Barohn
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Abstract

Introduction Phenylbutyrate (PBA) showed positive effect on the muscle cell model of Inclusion Body Myositis (IBM) by improving lysosomal activity, ameliorating consequences of impaired autophagy, and decreasing vacuolization. This provides rationale to study this medication in patients with IBM. Objectives To evaluate the safety and tolerability of phenylbutyrate in IBM, and monitor for any early signal of effectiveness. Methods Open-label study of 10 subjects with IBM who received treatment with PBA for 3 months after a 3-month run-in period. The PBA dose was 3 gm twice daily. The primary outcome measure was adverse event reporting. Secondary outcome measures included manual muscle testing, timed up and go test, IBM functional rating scale, and grip strength, along with exploratory biomarkers evaluating the mitochondrial function, stress response, degenerative process, and apoptosis. Results Ten subjects completed the study. PBA was well tolerated with no serious adverse events related to it. The most common adverse events were gastrointestinal related and did not require stopping treatment. One of the biomarkers (MitoTracker) showed a statistically significant drop over the treatment period of the study (p-value of 0.02 for the mean change). There were no statistically significant changes in other secondary outcome measures, but the study was limited by a small sample size and short treatment period. Conclusions Phenylbutyrate was safe and well tolerated in patients with IBM in this pilot study. The change in the MitoTracker suggests target engagement, but a Phase II study is needed to confirm and study the efficacy of PBA in IBM
苯丁酸盐治疗包涵体肌炎的安全性和耐受性
引言 丁酸苯酯(PBA)对包涵体肌炎(IBM)的肌肉细胞模型有积极作用,它能提高溶酶体活性,改善自噬功能受损的后果,减少空泡化。这为在 IBM 患者中研究这种药物提供了依据。目的 评估苯丁酸盐治疗 IBM 的安全性和耐受性,并监测任何早期疗效信号。方法 对 10 名 IBM 受试者进行开放标签研究,在 3 个月的磨合期后接受为期 3 个月的 PBA 治疗。PBA 剂量为 3 克,每天两次。主要结果指标为不良事件报告。次要结果指标包括手动肌肉测试、定时起立和走动测试、IBM 功能评分量表和握力,以及评估线粒体功能、应激反应、退化过程和细胞凋亡的探索性生物标志物。结果 10 名受试者完成了研究。受试者对 PBA 的耐受性良好,未出现严重不良反应。最常见的不良反应与胃肠道有关,无需停止治疗。其中一个生物标志物(线粒体追踪器)在研究治疗期间出现了统计学意义上的显著下降(平均变化的 p 值为 0.02)。其他次要结果指标未出现统计学意义上的显著变化,但该研究受到样本量小和治疗时间短的限制。结论 在这项试点研究中,苯丁酸盐对 IBM 患者安全且耐受性良好。线粒体追踪器的变化表明目标参与,但还需要进行二期研究,以确认和研究苯丁酸盐对 IBM 的疗效。
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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