The evolution of strategies to minimise the risk of human drug-induced liver injury (DILI) in drug discovery and development

被引:57
|
作者
Walker, Paul A. [1 ]
Ryder, Stephanie [1 ]
Lavado, Andrea [1 ]
Dilworth, Clive [1 ,2 ]
Riley, Robert J. [1 ]
机构
[1] Cyprotex Discovery Ltd, 24 Mereside,Alderley Pk, Macclesfield SK10 4TG, Cheshire, England
[2] Alderley Pk Accelerator, Alderley Pk, Macclesfield SK10 4TG, Cheshire, England
来源
ARCHIVES OF TOXICOLOGY | 2020年 / 94卷 / 08期
关键词
Hepatotoxicity; Spheroid; HCI; DILI; Cmax; tot; u; Strategies; CRYOPRESERVED HUMAN HEPATOCYTES; SALT EXPORT PUMP; IN-VITRO; HEPARG CELLS; MULTIPARAMETRIC ASSAY; HUMAN HEPATOTOXICITY; HEPG2; CELLS; TOXICITY; METABOLISM; PREDICTION;
D O I
10.1007/s00204-020-02763-w
中图分类号
R99 [毒物学(毒理学)];
学科分类号
100405 ;
摘要
Early identification of toxicity associated with new chemical entities (NCEs) is critical in preventing late-stage drug development attrition. Liver injury remains a leading cause of drug failures in clinical trials and post-approval withdrawals reflecting the poor translation between traditional preclinical animal models and human clinical outcomes. For this reason, preclinical strategies have evolved over recent years to incorporate more sophisticated human in vitro cell-based models with multi-parametric endpoints. This review aims to highlight the evolution of the strategies adopted to improve human hepatotoxicity prediction in drug discovery and compares/contrasts these with recent activities in our lab. The key role of human exposure and hepatic drug uptake transporters (e.g. OATPs, OAT2) is also elaborated.
引用
收藏
页码:2559 / 2585
页数:27
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