Targeting CCL24 in Inflammatory and Fibrotic Diseases: Rationale and Results from Three CM-101 Phase 1 Studies.

IF 4 2区 医学 Q1 PHARMACOLOGY & PHARMACY Drug Safety Pub Date : 2024-09-01 Epub Date: 2024-06-01 DOI:10.1007/s40264-024-01436-2
Adi Mor, Scott Friedman, Sharon Hashmueli, Amnon Peled, Massimo Pinzani, Matthew Frankel, Rifaat Safadi
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Abstract

Background: Overexpression of C-C motif chemokine ligand 24 (CCL24) is associated with inflammatory and fibrotic diseases, including primary sclerosing cholangitis (PSC), systemic sclerosis, metabolic dysfunction-associated steatotic liver disease (MASLD) and metabolic dysfunction-associated steatohepatitis (MASH). CM-101 is a humanized monoclonal antibody that neutralizes CCL24 to attenuate inflammation and fibrosis in preclinical models. Here we report the results from two Phase 1a studies investigating the safety and tolerability of intravenous (IV) and subcutaneous (SC) CM-101 in healthy participants, and in one Phase 1b study of IV and SC CM-101 in patients with MASLD without evidence of MASH.

Methods: In each dose group (0.75 mg/kg, 2.5 mg/kg, 5.0 mg/kg, and 10.0 mg/kg) of the single-center, double-blind, placebo-controlled Phase 1a IV study, healthy volunteers were randomized 3:1 to receive a single IV infusion of CM-101 or placebo. In another Phase 1a, single-center, double-blind placebo-controlled study, healthy volunteers were randomized 3:1 to receive a single SC injection of CM-101 5.0 mg/kg or placebo. In the multicenter, double-blind, placebo-controlled Phase 1b MASLD study, patients with MASLD without evidence of MASH were randomized 3:1 to receive the following: cohort 1, IV CM-101 2.5 mg/kg or placebo, and cohort 2, SC CM-101 5.0 mg/kg or placebo every three weeks for 12 weeks. The primary endpoints (for all these studies) were safety, tolerability, and serum pharmacokinetic parameters of CM-101.

Results: In each study, adverse events were rare and mild to moderate. The CM-101 pharmacokinetics profile was typical of a monoclonal antibody, with a terminal half-life of approximately 19 days when given IV and approximately 17 days when given as SC injection. In patients with MASLD without evidence of MASH, CM-101 was associated with decreased serum levels of inflammatory, fibrotic, and collagen turnover biomarkers.

Conclusions: In healthy volunteers and patients with MASLD without evidence of MASH, IV and SC CM-101 was well tolerated at doses ranging from 0.75 mg/kg to10.0 mg/kg and engaged its target (i.e., CCL24), indicating therapeutic potential in treating inflammatory and fibrotic diseases.

Clinical trial retrospectively registration: NCT06025851, NCT06037577, and NCT06044467. Date of registration: September 2023.

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在炎症和纤维化疾病中靶向 CCL24:三项 CM-101 1 期研究的原理和结果。
背景:C-C motif趋化因子配体 24(CCL24)的过度表达与炎症和纤维化疾病有关,包括原发性硬化性胆管炎(PSC)、系统性硬化症、代谢功能障碍相关性脂肪性肝病(MASLD)和代谢功能障碍相关性脂肪性肝炎(MASH)。CM-101 是一种人源化单克隆抗体,能中和 CCL24,从而减轻临床前模型中的炎症和纤维化。我们在此报告两项 1a 期研究的结果,这两项研究分别调查了 CM-101 在健康参与者中静脉注射(IV)和皮下注射(SC)的安全性和耐受性,以及 CM-101 在无 MASH 证据的 MASLD 患者中静脉注射和皮下注射的 1b 期研究:在单中心、双盲、安慰剂对照的1a期静脉注射研究中,每组剂量(0.75 mg/kg、2.5 mg/kg、5.0 mg/kg和10.0 mg/kg)的健康志愿者按3:1的比例随机分配,接受一次CM-101或安慰剂的静脉注射。在另一项 1a 期单中心双盲安慰剂对照研究中,健康志愿者按 3:1 的比例随机接受 5.0 毫克/千克 CM-101 或安慰剂的单次皮下注射。在多中心、双盲、安慰剂对照的 1b 期 MASLD 研究中,患有 MASLD 但无 MASH 证据的患者按 3:1 的比例随机接受以下治疗:组 1,静脉注射 CM-101 2.5 mg/kg 或安慰剂;组 2,每三周一次皮下注射 CM-101 5.0 mg/kg 或安慰剂,共注射 12 周。所有这些研究的主要终点是CM-101的安全性、耐受性和血清药代动力学参数:结果:在每项研究中,不良反应均为罕见的轻度至中度。CM-101的药代动力学特征是典型的单克隆抗体,静脉注射时半衰期约为19天,皮下注射时半衰期约为17天。在没有MASH证据的MASLD患者中,CM-101与血清中炎症、纤维化和胶原转化生物标志物水平的降低有关:结论:在健康志愿者和无MASH证据的MASLD患者中,静脉注射和皮下注射CM-101的耐受性良好,剂量从0.75 mg/kg到10.0 mg/kg不等,并能达到目标(即CCL24),这表明CM-101在治疗炎症和纤维化疾病方面具有治疗潜力:临床试验回顾注册:NCT06025851、NCT06037577 和 NCT06044467。注册日期:2023 年 9 月:注册日期:2023 年 9 月。
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来源期刊
Drug Safety
Drug Safety 医学-毒理学
CiteScore
7.60
自引率
7.10%
发文量
112
审稿时长
6-12 weeks
期刊介绍: Drug Safety is the official journal of the International Society of Pharmacovigilance. The journal includes: Overviews of contentious or emerging issues. Comprehensive narrative reviews that provide an authoritative source of information on epidemiology, clinical features, prevention and management of adverse effects of individual drugs and drug classes. In-depth benefit-risk assessment of adverse effect and efficacy data for a drug in a defined therapeutic area. Systematic reviews (with or without meta-analyses) that collate empirical evidence to answer a specific research question, using explicit, systematic methods as outlined by the PRISMA statement. Original research articles reporting the results of well-designed studies in disciplines such as pharmacoepidemiology, pharmacovigilance, pharmacology and toxicology, and pharmacogenomics. Editorials and commentaries on topical issues. Additional digital features (including animated abstracts, video abstracts, slide decks, audio slides, instructional videos, infographics, podcasts and animations) can be published with articles; these are designed to increase the visibility, readership and educational value of the journal’s content. In addition, articles published in Drug Safety Drugs may be accompanied by plain language summaries to assist readers who have some knowledge of, but not in-depth expertise in, the area to understand important medical advances.
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