衣壳
药代动力学
病毒学
药理学
药物代谢
药品
候选药物
乙型肝炎病毒
病毒
新陈代谢
化学
医学
生物
生物化学
作者
Ming Li,Xingguo Yan,Li Zhang,Xinchang Liu,Yayi Liu,Qian Wang,Jing Li
出处
期刊:Xenobiotica
[Taylor & Francis]
日期:2024-07-26
卷期号:54 (9): 701-710
标识
DOI:10.1080/00498254.2024.2381223
摘要
Pibothiadine (PBD; HEC121120) is a novel hepatitis B virus capsid assembly modulator based on GLS4 (morphothiadine) and has inhibitory activities against resistant strains.To assess the overall preclinical drug metabolism and pharmacokinetics (DMPK) properties of PBD, in vivo pharmacokinetics studies in rats and dogs have been performed along with a series of in vitro metabolism assays.The oral bioavailability of PBD in rats and dogs might be related to its medium permeability in Caco-2 cells and largely be impacted by the pH-dependent solubility. PBD was highly distributed to the liver where the local exposure was 16.4 fold of the system exposure. PBD showed relatively low metabolic rate in recombinant human cytochrome P450 enzymes, whereas low to moderate in vitro clearance in liver microsomes and low (dog) to moderate (rat) in vivo clearance. Furthermore, β-oxidation and dehydrogenation were proposed as the primary metabolic pathways of PBD in rats.Compared to GLS4, the higher systemic exposure of PBD might be attributed to its improved oral absorption and metabolic stability. In addition, the enhanced liver/plasma exposure ratio could further increase the local exposure around the target. These improved DMPK properties might indicate better development of PBD in the clinical phase.
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