Preclinical pharmacokinetics, CYP phenotyping, and tissue distribution study of novel anti-breast cancer candidate S-011-1559

药代动力学 药理学 分布(数学) 体内 乳腺癌 受体 脾脏 白蛋白 内分泌学 人血清白蛋白 癌症 化学 内科学 生物 医学 生物化学 数学 生物技术 数学分析
作者
Mukesh Kumar,Arpon Biswas,Mukesh Kumar,Anjali Mishra,Abhijit Deb Choudhury,Sristi Agrawal,Sachin Nashik Sanap,Amol Chhatrapati Bisen,Ashok Kumar Sharma,Gautam Panda,Rabi Sankar Bhatta
出处
期刊:Xenobiotica [Taylor & Francis]
卷期号:52 (5): 476-487 被引量:9
标识
DOI:10.1080/00498254.2022.2101033
摘要

S-011-1559 is a tyrosine-derived novel benzoxazine CDRI molecule targeted to the oestrogen-related receptor (ER-α/β) modulator in breast cancer. To explore the pharmacokinetics of S-011-1559, a selective and sensitive bioanalytical method using LC-MS/MS was established and validated in different biological matrices of female rats.Blood-to-plasma ratio and plasma protein binding (PPB) of S-011-1559 were found to be <1 and >97% in both rats and humans, respectively. The human serum albumin (HSA) and alpha-1-acid glycoprotein (AAG) binding was found in the range of > 68 to 45% and >14% respectively. Half-life and intrinsic clearance by microsomal stability study were found to be 28.83 min and 0.05 mL/min/mg in rats, 78.35 min and 0.036 mL/min/mg in humans, respectively. The IC50 value of S-011-1559 against CYP isoforms was revealed to moderately inhibit CYP2D6 by a reversible non-competitive mechanism.Tissue distribution of S-011-1559 on single intravenous injection at 2 mg/kg was found in the order of C lungs > C mammary gland > C spleen > C heart > C kidney > C liver > C brain.The data from the present study provides crucial information about S-011-1559 for further development as a novel potential drug candidate in modulating ER-α/β receptors of lung and breast neoplasia.
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