Efficacy results from a 12-month double-blind randomized trial of arimoclomol for treatment of Niemann-Pick disease type C (NPC): Presenting a rescored 4-domain NPC Clinical Severity Scale

IF 1.8 4区医学 Q3 GENETICS & HEREDITY

Molecular Genetics and Metabolism Reports Pub Date : 2025-05-28 DOI:10.1016/j.ymgmr.2025.101233

Eugen Mengel , Marc C. Patterson , Rosalia M. Da Riol , Mireia Del Toro , Federica Deodato , Matthias Gautschi , Stephanie Grunewald , Sabine Weller Grønborg , Paul Harmatz , Julia B. Hennermann , Bénédicte Héron , Esther M. Maier , Agathe Roubertie , Saikat Santra , Anna Tylki-Szymanska , Lisa LaGorio , Elizabeth Berry-Kravis , Forbes D. Porter , Beth Solomon , Louise Himmelstrup , Christine í Dali

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引用次数: 0

Abstract

Background

In the 12-month, randomized, double-blind, placebo-controlled Phase 2/3 NPC-002 study (NCT02612129), arimoclomol significantly reduced annual disease progression versus placebo, measured by the 5-domain NPC Clinical Severity Scale (5DNPCCSS). Arimoclomol has been approved in the US for treatment of Niemann-Pick disease type C (NPC) in combination with miglustat. This paper introduces the rescored 4-domain NPCCSS (R4DNPCCSS) as a post-hoc primary endpoint in NPC-002, discusses its validation, and presents the results of the post-hoc primary analysis.

Methods

To more accurately assess changes in disease course over a 12-month time period in a heterogeneous group of patients, the Cognition domain was removed from the 5DNPCCSS and the Swallow domain was rescored to reflect linearity in disease progression. Rescoring of the Swallow domain was based on input from clinical NPC and swallow experts from a qualitative interview-based study (N = 12), resulting in the R4DNPCCSS. To supplement prior validation analyses, data supporting the overall validity and reliability of the R4DNPCCSS was gathered through additional analyses of construct and convergent validity. The NPC-002 prespecified primary efficacy endpoint analysis based on the 5DNPCCSS score change from baseline to 12 months was repeated with R4DNPCCSS.

Results

Construct validity analysis demonstrated high agreement between the R4DNPCCSS domain scores and the Clinical Global Impression Scale of Severity (CGI-S) and NPC Clinical Database (NPC-cdb) scores. Convergent validity was confirmed by strong correlations between the R4DNPCCSS domains and corresponding items on the Scale for Assessment and Rating of Ataxia (SARA), 9-hole peg test (9-HPT), and Video Fluoroscopic Swallowing Study (VFSS) performance tests. The NPC-002 post-hoc primary analysis showed a mean standard error (SE) change in R4DNPCCSS score of 0.35 (0.40) with arimoclomol (N = 34) versus 2.05 (0.54) with placebo (N = 16), and a treatment effect in favor of arimoclomol over placebo of −1.70 (p = 0.0155). In the miglustat subgroup analysis, mean (SE) change in R4DNPCCSS score was −0.23 (1.02) with arimoclomol (N = 22) versus 1.92 (3.37) with placebo (N = 12), representing a treatment effect of −2.21 (p = 0.0077).

Conclusion

The R4DNPCCSS is a valid and reliable measure of disease progression demonstrating consistent outcomes with the prespecified 5DNPCCSS endpoint. Arimoclomol significantly slowed disease progression through 12 months as measured by the R4DNPCCSS versus placebo.

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一项为期12个月的双盲随机试验显示阿利莫洛尔治疗尼曼-匹克病C型（NPC）的疗效：呈现一个重新定义的4域NPC临床严重程度量表

在这项为期12个月、随机、双盲、安慰剂对照的2/3期NPC-002研究（NCT02612129）中，通过5域NPC临床严重程度量表（5DNPCCSS）测量，与安慰剂相比，阿利莫洛尔显著降低了年度疾病进展。阿利莫洛莫在美国被批准联合米卢司他治疗尼曼-匹克病C型（NPC）。本文介绍了重建的4域NPCCSS （R4DNPCCSS）作为NPC-002的事后主要终点，讨论了其有效性，并给出了事后主要分析的结果。方法为了更准确地评估一组异质性患者在12个月时间内的病程变化，从5DNPCCSS中去除认知域，恢复Swallow域以反映疾病进展的线性。吞咽域的重新评分是基于临床鼻咽癌和吞咽专家的定性访谈研究（N = 12），得出R4DNPCCSS。为了补充先前的验证分析，我们通过结构分析和收敛效度分析收集了支持R4DNPCCSS整体效度和信度的数据。基于5DNPCCSS评分从基线到12个月变化的NPC-002预先指定的主要疗效终点分析与R4DNPCCSS重复。结果结构效度分析表明，R4DNPCCSS域评分与临床总体印象严重程度量表（CGI-S）和NPC临床数据库（NPC-cdb）评分具有较高的一致性。R4DNPCCSS域与共济失调评定量表（SARA）、9孔peg测试（9-HPT）和视频透视吞咽研究（VFSS）性能测试中相应项目的强相关性证实了收敛效度。NPC-002事后初步分析显示，阿利莫洛尔（N = 34）组R4DNPCCSS评分的平均标准误差（SE）变化为0.35(0.40)，而安慰剂（N = 16）组为2.05(0.54)，阿利莫洛尔优于安慰剂的治疗效果为- 1.70 （p = 0.0155）。在米卢司他亚组分析中，阿利莫洛尔（N = 22）组R4DNPCCSS评分的平均（SE）变化为- 0.23(1.02)，而安慰剂（N = 12）组为1.92(3.37)，代表治疗效果为- 2.21 （p = 0.0077）。结论R4DNPCCSS是一种有效可靠的疾病进展测量方法，其结果与预先指定的5DNPCCSS终点一致。与安慰剂相比，通过R4DNPCCSS测量，阿利莫洛尔在12个月内显著减缓了疾病进展。

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

Molecular Genetics and Metabolism Reports Biochemistry, Genetics and Molecular Biology-Endocrinology

CiteScore

4.00

自引率

5.30%

发文量

105

审稿时长

33 days

期刊介绍： Molecular Genetics and Metabolism Reports is an open access journal that publishes molecular and metabolic reports describing investigations that use the tools of biochemistry and molecular biology for studies of normal and diseased states. In addition to original research articles, sequence reports, brief communication reports and letters to the editor are considered.