Department of Neurology, Northwestern University, Chicago, Illinois, USA.
Nerve and Muscle Center of Texas, Texas Medical Center, Houston, Texas, USA.
Clin Transl Sci. 2021 May;14(3):1176-1184. doi: 10.1111/cts.12977. Epub 2021 Feb 2.
VM202 is a plasmid DNA encoding two isoforms of hepatocyte growth factor (HGF). A previous phase II study in subjects with painful diabetic peripheral neuropathy (DPN) showed significant reductions in pain. A phase III study was conducted to evaluate the safety and efficacy of VM202 in DPN. The trial was conducted in two parts, one for 9 months (DPN 3-1) with 500 subjects (VM202: 336 subjects; and placebo: 164) and a preplanned subset of 101 subjects (VM202: 65 subjects; and placebo: 36) with a noninterventional extension to 12 months (DPN 3-1b). VM202 or placebo was administered to calf muscles on days 0 and 14, and on days 90 and 104. The primary end point in DPN 3-1 was change from baseline in the mean 24-h Numerical Rating Scale (NRS) pain score. In DPN 3-1b, the primary end point was safety, whereas the secondary efficacy end point was change in the mean pain score. VM202 was well-tolerated in both studies without significant adverse events. VM202 failed to meet its efficacy end points in DPN 3-1. In DPN 3-1b, however, VM202 showed significant and clinically meaningful pain reduction versus placebo. Pain reduction in DPN 3-1b was even greater in subjects not receiving gabapentin or pregabalin, confirming an observation noted in the phase II study. In DPN 3-1b, symptomatic relief was maintained for 8 months after the last injection suggesting that VM202 treatment might change disease progression. Despite the perplexing discrepancy between the two studies, the safety and long-lasting pain-relieving effects of VM202 observed in DPN 3-1b warrant another rigorous phase III study. Study Highlights WHAT IS THE CURRENT KNOWLEDGE ON THE TOPIC? Current therapies for painful diabetic peripheral neuropathy (DPN) are palliative and do not target the underlying mechanisms. Moreover, symptomatic relief is often limited with existing neuropathic pain drugs. Thus, there is a great medical need for safer and effective treatments for DPN. WHAT QUESTION DID THIS STUDY ADDRESS? Can nonviral gene delivery of hepatocyte growth factor reduce pain in patients with DPN and potentially modify progression of the disorder? WHAT DOES THIS STUDY ADD TO OUR KNOWLEDGE? Nonviral gene therapy can be used safely and practically to treat DPN. HOW MIGHT THIS CHANGE CLINICAL PHARMACOLOGY OR TRANSLATIONAL SCIENCE? As the first gene medicine to enter advanced clinical trials for the treatment of DPN, this study provides the proof of concept of an entirely new potential approach to the disorder.
VM202 是一种质粒 DNA,可编码两种肝细胞生长因子(HGF)同工型。一项针对有疼痛性糖尿病周围神经病变(DPN)的受试者的 II 期研究表明,疼痛显著减轻。一项 III 期研究旨在评估 VM202 在 DPN 中的安全性和疗效。该试验分两部分进行,第一部分为 9 个月(DPN 3-1),共有 500 名受试者(VM202:336 名;安慰剂:164 名)和 101 名预先计划的亚组(VM202:65 名;安慰剂:36 名),随后进行非干预性延长至 12 个月(DPN 3-1b)。VM202 或安慰剂在第 0 天和第 14 天、第 90 天和第 104 天给药于小腿肌肉。DPN 3-1 的主要终点是从基线到 24 小时平均数字评定量表(NRS)疼痛评分的变化。在 DPN 3-1b 中,主要终点是安全性,次要疗效终点是平均疼痛评分的变化。在两项研究中,VM202 均耐受良好,无明显不良事件。VM202 在 DPN 3-1 中未达到其疗效终点。然而,在 DPN 3-1b 中,与安慰剂相比,VM202 显示出显著且具有临床意义的疼痛减轻。在未接受加巴喷丁或普瑞巴林的受试者中,DPN 3-1b 中的疼痛减轻更大,证实了 II 期研究中的观察结果。在 DPN 3-1b 中,末次注射后 8 个月仍保持症状缓解,提示 VM202 治疗可能改变疾病进展。尽管两项研究之间存在令人费解的差异,但 DPN 3-1b 中观察到的 VM202 的安全性和持久的止痛作用值得进行另一项严格的 III 期研究。研究亮点 关于这个话题,目前有哪些知识? 目前用于治疗疼痛性糖尿病周围神经病变(DPN)的疗法是姑息性的,不能针对潜在的发病机制。此外,现有的神经病理性疼痛药物往往只能缓解症状。因此,DPN 患者需要更安全、更有效的治疗方法。 这项研究解决了什么问题? 肝细胞生长因子的非病毒基因传递能否减轻 DPN 患者的疼痛,并可能改变疾病的进展? 这项研究为我们的知识增加了什么? 非病毒基因治疗可以安全且实际地用于治疗 DPN。 这将如何改变临床药理学或转化科学? 作为首个进入 DPN 治疗的高级临床试验的基因药物,这项研究为该疾病的全新潜在治疗方法提供了概念验证。
