Modeling Drug-induced Mitochondrial Toxicity with Human Primary Cardiomyocytes

Overview

Journal Sci China Life Sci

Specialties Biology
Science

Date 2023 Oct 20

PMID 37864082

Authors

Xiaoli Tang

Hong Liu

Rongjia Rao

Yafei Huang

Mengqi Dong

Miaomiao Xu

Shanshan Feng

Xun Shi

Li Wang

Zengwu Wang

Bingying Zhou

Affiliations

Soon will be listed here.

Abstract

Mitochondrial toxicity induced by therapeutic drugs is a major contributor for cardiotoxicity, posing a serious threat to pharmaceutical industries and patients' lives. However, mitochondrial toxicity testing is not incorporated into routine cardiac safety screening procedures. To accurately model native human cardiomyocytes, we comprehensively evaluated mitochondrial responses of adult human primary cardiomyocytes (hPCMs) to a nucleoside analog, remdesivir (RDV). Comparison of their response to human pluripotent stem cell-derived cardiomyocytes revealed that the latter utilized a mitophagy-based mitochondrial recovery response that was absent in hPCMs. Accordingly, action potential duration was elongated in hPCMs, reflecting clinical incidences of RDV-induced QT prolongation. In a screen for mitochondrial protectants, we identified mitochondrial ROS as a primary mediator of RDV-induced cardiotoxicity. Our study demonstrates the utility of hPCMs in the detection of clinically relevant cardiac toxicities, and offers a framework for hPCM-based high-throughput screening of cardioprotective agents.

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