Reply to: Comment on De Giorgis et al. “Randomized Phase 3 Study of Triheptanoin for Glut1 Deficiency Syndrome–Associated Paroxysmal Movement Disorders”

IF 7.4 1区 医学 Q1 CLINICAL NEUROLOGY
Valentina De Giorgis, Darryl C. De Vivo
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引用次数: 0

Abstract

From a metabolic and basic science point of view, triheptanoin was an excellent therapeutic candidate for patients with Glut1DS. Earlier studies in humans were promising; however, these studies were open-label, observational studies with a small number of participants.1-4 Two randomized placebo-controlled trials have failed to demonstrate triheptanoin efficacy to control seizure frequency and movement disorders in GLUT1DS.5, 6 To our knowledge, no other double-blind, placebo-controlled trials have been conducted. Additionally, triheptanoin has been tested in many other metabolic and mitochondrial pathologies but has demonstrated efficacy in only one disease: long-chain fatty acid oxidation disorders (LC-FAOD).7, 8

Dr. Mochel and colleagues9 point out some limitations of our trial. These same limitations were described in detail in our article.5 Briefly, the dietary restrictions, dietary instructions, and dosing schedules used in our study mimic those used in earlier studies by Dr. Mochel and others.1-4 These earlier open-label studies did show a strong effect for triheptanoin, whereas in the more demanding clinical trials we did not. As these factors are similar among studies with different outcomes, it is unlikely that these factors are driving the differences.

Safflower oil was used as a placebo to match the appearance, taste, and smell of triheptanoin. This was necessary to maintain blinding, though as discussed in the article, “any oil, in a condition such as Glut1DS that may respond to additional dietary fat, may have a treatment effect, and therefore, may not function as a true placebo.”

Finally, treatment duration was 10–12 weeks of titration and 8 weeks of maintenance. This was followed by an open-label extension period of up to 3 years. No differences were seen during the double-blind portion of the study. No differences were seen during the open-label extension. Therefore, it seems unlikely that a longer duration of follow-up would reveal belated results.

In summary, triheptanoin failed to meet the primary endpoint, or any other endpoints in this clinical trial. While some patients may have benefited from triheptanoin, perhaps those with more subtle symptoms, these are single, anecdotal results that cannot be generalized without solid evidence of efficacy. The trial was, unfortunately, negative. We hope the details provided in our article5 and in this discussion are helpful to patients, caregivers, and other researchers working on therapies for this challenging disease.

(1) Conception; (2) A. Writing of the First Draft, B. Review and Critique.

V.D.G.: 1, 2A, 2B

D.C.D.: 1, 2B

V.D.G. has received speaker honoraria from Nutricia, Vitaflo, Kanso; has served as advisor/consultant for Vitaflo and Longboard Pharmaceuticals; has been an investigator for clinical trials for Eisai, UCB Pharma, and Marinus; and received travel reimbursement from GW Pharmaceuticals, Lusofarmaco. D.C.D. is an advisor/consultant for AveXis, Biogen, Cytokinetics, Ionis Pharmaceuticals, Metafora Biosystems, Roche, Sanofi, Sarepta, and SMA Foundation; has received research grants from Hope for Children Research Foundation, National Institutes of Health, SMA Foundation, Cure SMA, Glut1 Deficiency Foundation, and United States Department of Defense; has received clinical trial funding from Biogen, Mallinckrodt, PTC Therapeutics, Sarepta, Scholar Rock, and Ultragenyx Pharmaceutical; and has received compensation as a member of a data and safety monitoring board (Canavan disease) for Aspa Therapeutics. The phase III trial of triheptanoin in Glut1DS was funded by Ultragenyx Pharmaceutical Inc. Drs. De Giorgis and De Vivo were principal investigators in the trial.

回复:对 De Giorgis 等人 "三苯氧胺治疗 Glut1 缺失综合征相关阵发性运动障碍的 3 期随机研究 "的评论
从新陈代谢和基础科学的角度来看,三庚酸是治疗 Glut1DS 患者的绝佳候选药物。1-4 两项随机安慰剂对照试验未能证明三庚酸具有控制 GLUT1DS 患者癫痫发作频率和运动障碍的疗效。此外,三庚酸已在许多其他代谢和线粒体病症中进行了测试,但只在一种疾病中显示出疗效:长链脂肪酸氧化紊乱(LC-FAOD)。简而言之,我们的研究中使用的饮食限制、饮食指导和给药时间表与莫切尔博士等人早期研究中使用的相同。1-4 这些早期的开放标签研究确实显示三七皂苷具有很强的疗效,而在要求更高的临床试验中,我们却没有显示出很强的疗效。由于这些因素在不同结果的研究中相似,因此不太可能是这些因素导致了差异。红花油被用作安慰剂,以匹配三七皂苷的外观、味道和气味。这对于保持盲法是必要的,但正如文章中所讨论的,"任何油类,在 Glut1DS 这种可能对额外膳食脂肪有反应的情况下,都可能产生治疗效果,因此,可能无法起到真正安慰剂的作用。"最后,治疗持续时间为 10-12 周的滴定和 8 周的维持。随后是长达 3 年的开放标签延长期。研究的双盲部分未发现差异。开放标签延长期也未发现差异。总之,在这项临床试验中,三苯氧胺未能达到主要终点或任何其他终点。虽然有些患者可能从三七宁中获益,也许是那些症状较轻微的患者,但这些都是单一的、传闻性的结果,在没有确凿的疗效证据的情况下,不能一概而论。遗憾的是,试验结果是否定的。我们希望我们的文章5 和本讨论中提供的细节能对患者、护理人员和其他研究这种挑战性疾病疗法的研究人员有所帮助。 (1) 构思;(2) A. 撰写初稿,B. 审阅和评论。从 Nutricia、Vitaflo 和 Kanso 领取演讲酬金;担任 Vitaflo 和 Longboard Pharmaceuticals 的顾问;担任 Eisai、UCB Pharma 和 Marinus 临床试验的研究员;从 GW Pharmaceuticals 和 Lusofarmaco 领取差旅费报销。D.C.D.是 AveXis、Biogen、Cytokinetics、Ionis Pharmaceuticals、Metafora Biosystems、Roche、Sanofi、Sarepta 和 SMA 基金会的顾问;曾获得希望儿童研究基金会、美国国立卫生研究院、SMA 基金会、Cure SMA、Glut1 Deficiency 基金会和美国国防部的研究基金;曾获得百健、Mallinckrodt、PTC Therapeutics、Sarepta、Scholar Rock 和 Ultragenyx Pharmaceutical 的临床试验资助;并作为 Aspa Therapeutics 的数据和安全监控委员会(卡纳文病)成员获得报酬。三苯氧胺在 Glut1DS 中的 III 期试验由 Ultragenyx Pharmaceutical Inc.De Giorgis 博士和 De Vivo 博士是该试验的主要研究者。
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来源期刊
Movement Disorders
Movement Disorders 医学-临床神经学
CiteScore
13.30
自引率
8.10%
发文量
371
审稿时长
12 months
期刊介绍: Movement Disorders publishes a variety of content types including Reviews, Viewpoints, Full Length Articles, Historical Reports, Brief Reports, and Letters. The journal considers original manuscripts on topics related to the diagnosis, therapeutics, pharmacology, biochemistry, physiology, etiology, genetics, and epidemiology of movement disorders. Appropriate topics include Parkinsonism, Chorea, Tremors, Dystonia, Myoclonus, Tics, Tardive Dyskinesia, Spasticity, and Ataxia.
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