Prediction of hepatotoxicity for drugs using human pluripotent stem cell-derived hepatocytes

被引:20
|
作者
Kim, Jong Hyun [1 ]
Wang, Min [2 ]
Lee, Jaehun [3 ]
Park, Han-Jin [4 ]
Han, Chungseong [1 ]
Hong, Hee Su [1 ]
Kim, Jeong Seong [1 ]
An, Geun Ho [1 ]
Park, Kijung [1 ]
Park, Hee-Kyung [5 ,6 ]
Zhu, Shi Feng [7 ]
Sun, Xiao-Bo [2 ]
Kim, Jong-Hoon [3 ]
Woo, Dong-Hun [1 ]
机构
[1] NEXEL Co Ltd, Lab Stem Cells, 9th Floor,21 Wangsan Ro, Seoul 02580, South Korea
[2] CAMS, Inst Med Plant Dev IMPLAD, PUMC, 151 North Rd Malianwa, Beijing 100093, Peoples R China
[3] Korea Univ, Coll Life Sci & Biotechnol, Dept Biotechnol, Lab Stem Cells & Tissue Regenerat, Sci Campus,145 Anam Ro, Seoul 02841, South Korea
[4] Korea Inst Toxicol, Predict Model Res Ctr, Daejeon 34114, South Korea
[5] Seoul Natl Univ, Dept Oral Med & Oral Diag, Sch Dent, Yunkeun Dong 28, Seoul 03080, South Korea
[6] Seoul Natl Univ, Dent Res Inst, Yunkeun Dong 28, Seoul 03080, South Korea
[7] Yanbian Univ, Sch Continuing Educ, 977 Gongyuan Str, Yanji 133002, Jilin, Peoples R China
关键词
Drug screening; Hepatocytes; Human embryonic stem cells; Toxicity test; METABOLIZING-ENZYMES; SIGNALING PATHWAYS; GENE-EXPRESSION; LIVER-INJURY; RECEPTOR; RAT; ACID; PXR; TROGLITAZONE; SENSITIVITY;
D O I
10.1007/s10565-017-9392-y
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Drug-induced liver toxicity is a main reason for withdrawals of new drugs in late clinical phases and post-launch of the drugs. Thus, hepatotoxicity screening of drug candidates in pre-clinical stage is important for reducing drug attrition rates during the clinical development process. Here, we show commercially available hepatocytes that could be used for early toxicity evaluation of drug candidates. From our hepatic differentiation technology, we obtained highly pure (>= 98%) hepatocytes from human embryonic stem cells (hESCs) having mature phenotypes and similar gene expression profiles with those of primary human tissues. Furthermore, we optimized 96-well culture condition of hESC-derived hepatocytes suitable for toxicity tests in vitro. To this end, we demonstrated the efficacy of our optimized hepatocyte model for predicting hepatotoxicity against the Chinese herbal medicines and showed that toxicity patterns from our hepatocyte model was similar to those of human primary cultured hepatocytes. We conclude that toxicity test using our hepatocyte model could be a good alternative cell source for pre-clinical study to predict potential hepatotoxicity in drug discovery industries.
引用
收藏
页码:51 / 64
页数:14
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