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体外和体内临床前药代动力学特征研究表明,阿非卡肽是一种小分子心肌肌球蛋白抑制剂。

In vitro and in vivo preclinical pharmacokinetic characterization of aficamten, a small molecule cardiac myosin inhibitor.

机构信息

Department of Drug Metabolism and Pharmacokinetics, Cytokinetics, Inc, South San Francisco, California, USA.

Department of Medicinal Chemistry, Cytokinetics, Inc, South San Francisco, California, USA.

出版信息

Xenobiotica. 2024 Sep;54(9):686-700. doi: 10.1080/00498254.2024.2389407. Epub 2024 Aug 9.

DOI:10.1080/00498254.2024.2389407
PMID:39102472
Abstract

Aficamten, a small molecule selective inhibitor of cardiac myosin, was characterised in preclinical and studies.Protein binding in human plasma was 10.4% unbound and ranged from 1.6% to 24.9% unbound across species. Blood-to-plasma ratios ranged from 0.69 to 1.14 across species. Aficamten hepatic clearance in human was predicted to be low from observed high metabolic stability in human liver microsomes. Aficamten demonstrated high permeability in Caco-2 cell monolayers.Aficamten clearance was low across species at 8.8, 2.1, 3.3, and 11 mL/min/kg in mouse, rat, dog, and monkey, respectively. The volume of distribution was low-to-high ranging from 0.53 in rat to 11 L/kg in dog. Oral bioavailability ranged from 41% in monkey to 98% in mouse.Aficamten was metabolised to eight metabolites with hydroxylated metabolites M1a and M1b predominating. CYP phenotyping indicated multiple CYPs (2C8, 2C9, 2D6, and 3A4) contributing to the metabolism of aficamten.Human clearance (1.1 mL/min/kg) and volume of distribution (6.5 L/kg) were predicted using 4-species allometry employing 'rule-of-exponents'. A predicted 69 hour half-life is consistent with observed half-life in human Phase-1.No CYP-based drug-drug interaction liability as a precipitant was predicted for aficamten.

摘要

阿非卡肽是一种心脏肌球蛋白的小分子选择性抑制剂,在临床前和临床研究中得到了研究。人血浆中的蛋白结合率为 10.4%未结合,在各物种中范围为 1.6%至 24.9%未结合。血对血浆的比值在各物种中范围为 0.69 至 1.14。阿非卡肽在人肝微粒体中表现出高代谢稳定性,因此预测其在人体内的肝清除率较低。阿非卡肽在 Caco-2 细胞单层中表现出高渗透性。阿非卡肽在各物种中的清除率均较低,在小鼠、大鼠、狗和猴子中分别为 8.8、2.1、3.3 和 11 毫升/分钟/千克。分布容积从大鼠的 0.53 到狗的 11 升/千克,范围为低至高。口服生物利用度从猴子的 41%到老鼠的 98%不等。阿非卡肽被代谢为八种代谢物,其中羟基化代谢物 M1a 和 M1b 占主导地位。CYP 表型分析表明,多种 CYP(2C8、2C9、2D6 和 3A4)参与了阿非卡肽的代谢。使用 4 种物种的比例分配法,根据预测人清除率(1.1 毫升/分钟/千克)和分布容积(6.5 升/千克)。预测的 69 小时半衰期与人体 I 期观察到的半衰期一致。阿非卡肽没有预测到基于 CYP 的药物相互作用的药物相互作用风险。

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