Safety, Pharmacokinetics, and Pharmacodynamics of a First-in-Class ClC-1 Inhibitor to Enhance Muscle Excitability: Phase I Randomized Controlled Trial.

IF 6.3 2区医学 Q1 PHARMACOLOGY & PHARMACY

Clinical Pharmacology & Therapeutics Pub Date : 2024-12-09 DOI:10.1002/cpt.3516

Titia Q Ruijs, Catherine M K E de Cuba, Jules A A C Heuberger, John Hutchison, Jane Bold, Thomas S Grønnebæk, Klaus G Jensen, Eva Chin, Jorge A Quiroz, Thomas K Petersen, Peter Flagstad, Marieke L de Kam, Michiel J van Esdonk, Erica Klaassen, Robert J Doll, Ingrid W Koopmans, Annika A de Goede, Linda B S Aulin, Thomas H Pedersen, Geert Jan Groeneveld

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引用次数: 0

Abstract

NMD670 is a first-in-class inhibitor of skeletal muscle-specific chloride channel ClC-1, developed to improve muscle weakness and fatigue in neuromuscular diseases. Preclinical studies show that ClC-1 inhibition enhances muscle excitability, improving muscle contractility and strength. We describe the first-in-human, randomized, double-blind, placebo-controlled study, which evaluated the safety, pharmacokinetics, and pharmacodynamics of single and multiple doses of NMD670 in healthy male and female subjects. Single-ascending doses (50-1,600 mg) were administered in a (partial) cross-over design; multiple-ascending doses (200-600 mg q.d.; 400 mg b.i.d.) were administered in a parallel design. Differences in pharmacokinetics between males/females and fed/fasted states were evaluated. Pharmacodynamic effects were evaluated using muscle velocity recovery cycles (MVRC) and analyzed using mixed-effects modeling. NMD670 was generally safe and well-tolerated in healthy subjects, with the only dose-related adverse event being myotonia occurring at the highest dose levels tested (single dose of 1,200, and 1,600 mg). Moreover, NMD670 significantly increased the following MVRC parameters after a single dose of 1,200 mg compared with placebo: early supernormality (estimated difference (ED) 2.04; 95% confidence interval (CI) 0.379, 3.70; P = 0.0242); early supernormality after 5 conditioning stimuli (ED 2.51; 95%CI 0.599, 4.41; P = 0.0177); supernormality at 20 ms (ED 2.78; 95%CI 1.377, 4.181; P = 0.0021). Importantly, the results of this study indicate pharmacological target engagement at well-tolerated dose levels in healthy subjects; firstly, because myotonia was an expected exaggerated on-target pharmacological effect, and secondly, because the effects on MVRC indicate increased muscle cell excitability. This study in healthy subjects indicates proof-of-mechanism and provides a solid base for translation to patients with neuromuscular diseases.

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一种一流的ClC-1抑制剂增强肌肉兴奋性的安全性、药代动力学和药效学：I期随机对照试验。

NMD670是骨骼肌特异性氯离子通道ClC-1的一流抑制剂，用于改善神经肌肉疾病患者的肌肉无力和疲劳。临床前研究表明，抑制ClC-1可增强肌肉兴奋性，改善肌肉收缩力和力量。我们描述了第一个人体、随机、双盲、安慰剂对照研究，该研究评估了健康男性和女性受试者单剂量和多剂量NMD670的安全性、药代动力学和药效学。单次递增剂量（50-1,600 mg）采用（部分）交叉设计；多次递增剂量(每日200-600毫克；400 mg b.i.d)，采用平行设计。评估了男性/女性和进食/禁食状态之间的药代动力学差异。使用肌肉速度恢复周期（MVRC）评估药效学效果，并使用混合效应模型进行分析。在健康受试者中，NMD670总体上是安全的，耐受性良好，唯一与剂量相关的不良事件是在测试的最高剂量水平（单剂量为1200毫克和1600毫克）下发生的肌强直。此外，与安慰剂相比，单次给药1200 mg后，NMD670显著增加了以下MVRC参数：早期异常(估计差异（ED） 2.04；95%置信区间（CI） 0.379, 3.70；p = 0.0242)；5次条件刺激后早期异常(ED 2.51；95%ci 0.599, 4.41；p = 0.0177)；20 ms异常(ED 2.78；95%ci 1.377, 4.181；p = 0.0021)。重要的是，这项研究的结果表明，在健康受试者耐受良好的剂量水平下，药物靶点参与；首先，因为肌强直是一种预期的夸张的靶标药理作用，其次，因为对MVRC的影响表明肌肉细胞兴奋性增加。这项健康受试者的研究表明了机制的证明，并为神经肌肉疾病患者的翻译提供了坚实的基础。

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

Clinical Pharmacology & Therapeutics 医学-药学

CiteScore

12.70

自引率

7.50%

发文量

290

审稿时长

2 months

期刊介绍： Clinical Pharmacology & Therapeutics (CPT) is the authoritative cross-disciplinary journal in experimental and clinical medicine devoted to publishing advances in the nature, action, efficacy, and evaluation of therapeutics. CPT welcomes original Articles in the emerging areas of translational, predictive and personalized medicine; new therapeutic modalities including gene and cell therapies; pharmacogenomics, proteomics and metabolomics; bioinformation and applied systems biology complementing areas of pharmacokinetics and pharmacodynamics, human investigation and clinical trials, pharmacovigilence, pharmacoepidemiology, pharmacometrics, and population pharmacology.