Characterization of AST-001 non-clinical pharmacokinetics: A novel selective AKR1C3-activated prodrug in mice, rats, and cynomolgus monkeys

IF 1.7 4区 医学 Q3 PHARMACOLOGY & PHARMACY
Teng Meng, Donald Jung, Xiao-Hong Cai, Zhao-Qiang Lu, Ji-Bing Yu, Tian-Yang Qi, Fan-Ying Meng, Mei-Zhen Ruan, Jian-Xin Duan
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Abstract

AST-001 is a chemically synthesized inactive nitrogen mustard prodrug that is selectively cleaved to a cytotoxic aziridine (AST-2660) via aldo-keto reductase family 1 member C3 (AKR1C3). The purpose of this study was to investigate the pharmacokinetics and tissue distribution of the prodrug, AST-001, and its active metabolite, AST-2660, in mice, rats, and monkeys. After single and once daily intravenous bolus doses of 1.5, 4.5, and 13.5 mg/kg AST-001 to Sprague-Dawley rats and once daily 1 h intravenous infusions of 0.5, 1.5, and 4.5 mg/kg AST-001 to cynomolgus monkeys, AST-001 exhibited dose-dependent pharmacokinetics and reached peak plasma levels at the end of the infusion. No significant accumulation and gender differences were observed after 7 days of repeated dosing. In rats, the half-life of AST-001 was dose independent and ranged from 4.89 to 5.75 h. In cynomolgus monkeys, the half-life of AST-001 was from 1.66 to 5.56 h and increased with dose. In tissue distribution studies conducted in Sprague-Dawley rats and in liver cancer PDX models in female athymic nude mice implanted with LI6643 or LI6280 HepG2-GFP tumor fragments, AST-001 was extensively distributed to selected tissues. Following a single intravenous dose, AST-001 was not excreted primarily as the prodrug, AST-001 or the metabolite AST-2660 in the urine, feces, and bile. A comprehensive analysis of the preclinical data and inter-species allometric scaling were used to estimate the pharmacokinetic parameters of AST-001 in humans and led to the recommendation of a starting dose of 5 mg/m2 in the first-in-human dose escalation study.

Abstract Image

AST-001 非临床药代动力学特征:一种新型选择性 AKR1C3 激活原药在小鼠、大鼠和猕猴体内的作用。
AST-001 是一种化学合成的非活性氮芥原药,可通过醛酮还原酶家族 1 成员 C3(AKR1C3)选择性地裂解为具有细胞毒性的氮丙啶(AST-2660)。本研究旨在探讨原药 AST-001 及其活性代谢物 AST-2660 在小鼠、大鼠和猴子体内的药代动力学和组织分布。对 Sprague-Dawley 大鼠单次和每天一次静脉注射 1.5、4.5 和 13.5 毫克/千克 AST-001,以及对猴每天一次静脉注射 0.5、1.5 和 4.5 毫克/千克 AST-001,AST-001 均表现出剂量依赖性药代动力学,并在输注结束时达到血浆峰值水平。重复给药 7 天后,未观察到明显的蓄积和性别差异。在大鼠体内,AST-001 的半衰期与剂量无关,从 4.89 到 5.75 小时不等;在猴体内,AST-001 的半衰期从 1.66 到 5.56 小时不等,并随剂量增加而延长。在Sprague-Dawley大鼠和植入LI6643或LI6280 HepG2-GFP肿瘤片段的雌性无胸腺裸鼠肝癌PDX模型的组织分布研究中,AST-001广泛分布于选定的组织。单次静脉注射后,AST-001 主要以原药 AST-001 或代谢物 AST-2660 的形式从尿液、粪便和胆汁中排出。通过对临床前数据的综合分析和种间异速比,我们估算出了AST-001在人体中的药代动力学参数,并建议在首次人体剂量递增研究中将起始剂量定为5毫克/平方米。
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来源期刊
CiteScore
3.60
自引率
0.00%
发文量
35
审稿时长
6-12 weeks
期刊介绍: Biopharmaceutics & Drug Dispositionpublishes original review articles, short communications, and reports in biopharmaceutics, drug disposition, pharmacokinetics and pharmacodynamics, especially those that have a direct relation to the drug discovery/development and the therapeutic use of drugs. These includes: - animal and human pharmacological studies that focus on therapeutic response. pharmacodynamics, and toxicity related to plasma and tissue concentrations of drugs and their metabolites, - in vitro and in vivo drug absorption, distribution, metabolism, transport, and excretion studies that facilitate investigations related to the use of drugs in man - studies on membrane transport and enzymes, including their regulation and the impact of pharmacogenomics on drug absorption and disposition, - simulation and modeling in drug discovery and development - theoretical treatises - includes themed issues and reviews and exclude manuscripts on - bioavailability studies reporting only on simple PK parameters such as Cmax, tmax and t1/2 without mechanistic interpretation - analytical methods
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