Phase 2b program with sonlicromanol in patients with mitochondrial disease due to m.3243A>G mutation.

IF 10.6 1区 医学 Q1 CLINICAL NEUROLOGY
Brain Pub Date : 2024-11-06 DOI:10.1093/brain/awae277
Jan Smeitink, Just van Es, Brigitte Bosman, Mirian C H Janssen, Thomas Klopstock, Grainne Gorman, John Vissing, Gerrit Ruiterkamp, Chris J Edgar, Evertine J Abbink, Rob van Maanen, Oksana Pogoryelova, Claudia Stendel, Almut Bischoff, Ivan Karin, Mahtab Munshi, Anne Kümmel, Lydia Burgert, Christianne Verhaak, Herma Renkema
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引用次数: 0

Abstract

Mitochondrial disease is a group of rare conditions, with no approved treatment to date, except for Leber hereditary optic neuropathy. Therapeutic options to alleviate the symptoms of mitochondrial disease are urgently needed. Sonlicromanol is a promising candidate, as it positively alters the key metabolic and inflammatory pathways associated with mitochondrial disease. Sonlicromanol is a reductive and oxidative distress modulator, selectively inhibiting microsomal prostaglandin E1 synthase activity. This Phase 2b program, aiming at evaluating sonlicromanol in adults with m.3243A>G mutation and primary mitochondrial disease, consisted of a randomized controlled (RCT) study (dose-selection) followed by a 52-week open-label extension study (EXT, long-term tolerability, safety, and efficacy of sonlicromanol). Patients were randomized (1:1:1) to receive 100- or 50-mg sonlicromanol, or placebo twice daily (bid) for 28 days with ≥2-week wash-out period between treatments. Patients who completed the RCT study entered the EXT study wherein they received 100-mg sonlicromanol bid. Overall, 27 patients were randomized (24 RCT patients completed all periods). 15 patients entered the EXT, and 12 patients were included in the EXT analysis set. All patients reported good tolerability and favourable safety, with pharmacokinetic results comparable to the earlier Phase 2a study. The RCT primary endpoint (change from placebo in the attentional domain of cognition score [IDN: visual identification, Cogstate]) did not reach statistical significance. Using a categorisation of the subject's period baseline a treatment effect over placebo was observed if their baseline was more affected (p=0.0338). Using this approach, there were signals of improvements over placebo in at least one dose in the Beck Depression Inventory (BDI, p=0.0143), Cognitive Failure Questionnaire (CFQ, p=0.0113), and the Depression subscale of the Hospital Anxiety and Depression Scale (p=0.0256). Statistically and/or clinically meaningful improvements were observed in the patient- and clinician-reported outcome measures at the end of the EXT study (Test of attentional performance [TAP] with alarm, p=0.0102; TAP without alarm, p=0.0047; BDI somatic, p=0.0261; BDI Total, p=0.0563; SF12 physical component score, p=0.0008). Seven of nine domains of RAND-Short form-36 like SF-36 pain improved (p=0.0105). Other promising results were observed in Neuro QoL-Fatigue-SF (p=0.0036), MiniBESTest (p=0.0009), McGill Pain Questionnaire (p=0.0105), EQ-5D-5L-VAS (p=0.0213) and EQ-5D-5L-index (p=0.0173). Most patients showed improvement in the 5× sit-to-stand test. Sonlicromanol was well-tolerated and demonstrated a favourable benefit/risk ratio for up to one year. Sonlicromanol was efficacious in patients when affected at baseline, as seen across a variety of clinically relevant domains. Long-term treatment showed more pronounced changes from baseline.

在 m.3243A>G 突变导致的线粒体疾病患者中使用 sonlicromanol 的 2b 阶段计划。
线粒体疾病是一类罕见疾病,除了 Leber 遗传性视神经病变外,迄今为止尚无其他治疗方法获得批准。目前迫切需要缓解线粒体疾病症状的治疗方案。Sonlicromanol 是一种很有前景的候选药物,因为它能积极改变与线粒体疾病相关的关键代谢和炎症途径。Sonlicromanol 是一种还原和氧化窘迫调节剂,可选择性地抑制微粒体前列腺素 E1 合酶的活性。该 2b 期项目旨在对 m.3243A>G 突变和原发性线粒体疾病的成人患者进行评估,包括一项随机对照(RCT)研究(剂量选择)和一项为期 52 周的开放标签扩展研究(EXT、sonlicromanol 的长期耐受性、安全性和有效性)。患者被随机(1:1:1)分配接受 100 毫克或 50 毫克的桑利色莫醇或安慰剂,每天两次(bid),持续 28 天,两次治疗之间的间隔期≥2 周。完成 RCT 研究的患者进入 EXT 研究,在 EXT 研究中,他们每天两次服用 100 毫克桑利色醇。共有 27 名患者接受了随机治疗(24 名 RCT 患者完成了所有疗程)。15 名患者参加了 EXT,12 名患者被纳入 EXT 分析集。所有患者都报告了良好的耐受性和安全性,药代动力学结果与早期的 2a 期研究相当。该研究的主要终点(与安慰剂相比,认知注意力领域得分[IDN:视觉识别,Cogstate]的变化)未达到统计学意义。如果受试者的基线受到的影响更大,则采用受试者时期基线分类法可观察到治疗效果优于安慰剂(P=0.0338)。采用这种方法,在贝克抑郁量表(BDI,p=0.0143)、认知失败问卷(CFQ,p=0.0113)以及医院焦虑和抑郁量表的抑郁分量表(p=0.0256)中,至少有一种剂量的治疗效果比安慰剂有改善。在 EXT 研究结束时,患者和临床医生报告的结果指标均有统计学和/或临床意义的改善(有警报的注意力表现测试 [TAP],p=0.0102;无警报的注意力表现测试,p=0.0047;BDI 躯体评分,p=0.0261;BDI 总分,p=0.0563;SF12 身体成分评分,p=0.0008)。在 RAND-Short form-36 的九个领域中,有七个领域(如 SF-36 疼痛)有所改善(p=0.0105)。在神经 QoL-疲劳-SF(p=0.0036)、MiniBESTest(p=0.0009)、麦吉尔疼痛问卷(p=0.0105)、EQ-5D-5L-VAS(p=0.0213)和 EQ-5D-5L-index (p=0.0173)方面也观察到了其他令人鼓舞的结果。大多数患者在 5× 坐立测试中均有改善。Sonlicromanol 的耐受性良好,并在长达一年的时间里显示出良好的效益/风险比。从各种临床相关领域来看,索尼咯玛诺对基线受影响的患者具有疗效。长期治疗显示出与基线相比更明显的变化。
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
Brain
Brain 医学-临床神经学
CiteScore
20.30
自引率
4.10%
发文量
458
审稿时长
3-6 weeks
期刊介绍: Brain, a journal focused on clinical neurology and translational neuroscience, has been publishing landmark papers since 1878. The journal aims to expand its scope by including studies that shed light on disease mechanisms and conducting innovative clinical trials for brain disorders. With a wide range of topics covered, the Editorial Board represents the international readership and diverse coverage of the journal. Accepted articles are promptly posted online, typically within a few weeks of acceptance. As of 2022, Brain holds an impressive impact factor of 14.5, according to the Journal Citation Reports.
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