Division of Metabolic Disorders, Children's Hospital of Orange County, 1201 W. La Veta Ave, Orange, CA 92868, United States; Department of Pediatrics, University of California-Irvine, Orange, CA 92868, United States.
Hospital Sabara, Av. Angélica, 1987 Consolação, São Paulo, SP, 01227-200, Brazil; Centro de Biotecnologia /Instituto de Pesquisas de Energéticas e Nucleares IPEN/USP, Av 11 de junho 364, Casa 3, Vila Clementino, São Paulo, 04041-001, Brazil.
Mol Genet Metab. 2020 Mar;129(3):219-227. doi: 10.1016/j.ymgme.2020.01.003. Epub 2020 Jan 11.
Vestronidase alfa (recombinant human beta-glucuronidase) is an enzyme replacement therapy (ERT) for Mucopolysaccharidosis (MPS) VII, a highly heterogeneous, ultra-rare disease. Twelve subjects, ages 8-25 years, completed a Phase 3, randomized, placebo-controlled, blind-start, single crossover study (UX003-CL301; NCT02377921), receiving 24-48 weeks of vestronidase alfa 4 mg/kg IV. All 12 subjects completed the blind-start study, which showed significantly reduced urinary glycosaminoglycans (GAG) and clinical improvement in a multi-domain responder index, and enrolled in a long-term, open-label, extension study (UX003-CL202; NCT02432144). Here, we report the final results of the extension study, up to an additional 144 weeks after completion of the blind-start study. Three subjects (25%) completed all 144 weeks of study, eight subjects (67%) ended study participation before Week 144 to switch to commercially available vestronidase alfa, and one subject discontinued due to non-compliance after receiving one infusion of vestronidase alfa in the extension study. The safety profile of vestronidase alfa in the extension study was consistent with observations in the preceding blind-start study, with most adverse events mild to moderate in severity. There were no treatment or study discontinuations due to AEs and no noteworthy changes in a standard safety chemistry panel. Out of the eleven subjects who tested positive for anti-drug antibodies at any time during the blind-start or extension study, including the baseline assessment in the blind-start study, seven subjects tested positive for neutralizing antibodies and all seven continued to demonstrate a reduction in urinary GAG levels. There was no association between antibody formation and infusion associated reactions. Subjects receiving continuous vestronidase alfa treatment showed a sustained urinary GAG reduction and clinical response evaluated using a multi-domain responder index that includes assessments in pulmonary function, motor function, range of motion, mobility, and visual acuity. Reduction in fatigue was also maintained in the overall population. As ERT is not expected to cross the blood brain barrier, limiting the impact on neurological signs of disease, and not all subjects presented with neurological symptoms, outcomes related to central nervous system pathology are not focused on in this report. Results from this study show the long-term safety and durability of clinical efficacy in subjects with MPS VII with long-term vestronidase alfa treatment.
注射用伊米苷酶(重组人β-葡糖苷酸酶)是一种用于黏多糖贮积症 VII 型(MPS VII)的酶替代疗法(ERT),MPS VII 是一种高度异质性的罕见病。12 名年龄在 8-25 岁的受试者完成了一项 3 期、随机、安慰剂对照、盲法启动、单次交叉研究(UX003-CL301;NCT02377921),接受了 24-48 周的 4mg/kg 静脉注射用伊米苷酶治疗。所有 12 名受试者均完成了盲法启动研究,该研究显示尿液糖胺聚糖(GAG)显著减少,多领域应答指数有临床改善,并入组了一项长期、开放性、扩展研究(UX003-CL202;NCT02432144)。在这里,我们报告了扩展研究的最终结果,即在盲法启动研究完成后,额外增加了 144 周的随访。3 名受试者(25%)完成了全部 144 周的研究,8 名受试者(67%)在 144 周前结束研究,转为使用市售的注射用伊米苷酶,1 名受试者因在扩展研究中接受了一次伊米苷酶输注后不遵守治疗方案而停止研究。扩展研究中注射用伊米苷酶的安全性与之前的盲法启动研究一致,大多数不良反应的严重程度为轻度至中度。没有因不良事件而停药或研究终止,标准安全性化学指标也没有明显变化。在盲法启动或扩展研究的任何时间点检测到抗药物抗体的 11 名受试者中,包括盲法启动研究的基线评估,有 7 名受试者检测到中和抗体,且所有 7 名受试者的尿液 GAG 水平持续下降。抗体形成与输注相关反应之间没有关联。接受持续伊米苷酶治疗的受试者表现出持续的尿液 GAG 减少和使用多领域应答指数评估的临床应答,该指数包括肺功能、运动功能、关节活动度、移动能力和视力评估。总体人群的疲劳减轻也得到维持。由于 ERT 预计不会穿过血脑屏障,从而限制了对疾病神经体征的影响,而且并非所有受试者都有神经症状,因此本报告不重点关注与中枢神经系统病理相关的结果。这项研究的结果表明,MPS VII 受试者长期接受伊米苷酶治疗具有长期的安全性和临床疗效持久性。
