Functional Validation of Doxorubicin-Induced Cardiotoxicity-Related Genes

IF 12 1区医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

Jacc: Cardiooncology Pub Date : 2024-02-01 DOI:10.1016/j.jaccao.2023.11.008

Hananeh Fonoudi PhD , Mariam Jouni PhD , Romina B. Cejas PhD , Tarek Magdy PhD , Malorie Blancard PhD , Ning Ge PhD , Disheet A. Shah PhD , Davi M. Lyra-Leite PhD , Achal Neupane PhD , Mennat Gharib BS , Zhengxin Jiang PhD , Yadav Sapkota PhD , Paul W. Burridge PhD

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Abstract

Background

Genome-wide association studies and candidate gene association studies have identified more than 180 genetic variants statistically associated with anthracycline-induced cardiotoxicity (AIC). However, the lack of functional validation has hindered the clinical translation of these findings.

Objectives

The aim of this study was to functionally validate all genes associated with AIC using human induced pluripotent stem cell–derived cardiomyocytes (hiPSC-CMs).

Methods

Through a systemic literature search, 80 genes containing variants significantly associated with AIC were identified. Additionally, 3 more genes with potential roles in AIC (GSTM1, CBR1, and ERBB2) were included. Of these, 38 genes exhibited expression in human fetal heart, adult heart, and hiPSC-CMs. Using clustered regularly interspaced short palindromic repeats/Cas9–based genome editing, each of these 38 genes was systematically knocked out in control hiPSC-CMs, and the resulting doxorubicin-induced cardiotoxicity (DIC) phenotype was assessed using hiPSC-CMs. Subsequently, functional assays were conducted for each gene knockout on the basis of hypothesized mechanistic implications in DIC.

Results

Knockout of 26 genes increased the susceptibility of hiPSC-CMs to DIC. Notable genes included efflux transporters (ABCC10, ABCC2, ABCB4, ABCC5, and ABCC9), well-established DIC-associated genes (CBR1, CBR3, and RAC2), and genome-wide association study–discovered genes (RARG and CELF4). Conversely, knockout of ATP2B1, HNMT, POR, CYBA, WDR4, and COL1A2 had no significant effect on the in vitro DIC phenotype of hiPSC-CMs. Furthermore, knockout of the uptake transporters (SLC28A3, SLC22A17, and SLC28A1) demonstrated a protective effect against DIC.

Conclusions

The present findings establish a comprehensive platform for the functional validation of DIC-associated genes, providing insights for future studies in DIC variant associations and potential mechanistic targets for the development of cardioprotective drugs.

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多柔比星诱导的心脏毒性相关基因的功能验证

背景全基因组关联研究和候选基因关联研究已发现180多个遗传变异与蒽环类药物诱导的心脏毒性（AIC）有统计学关联。本研究旨在利用人体诱导多能干细胞衍生的心肌细胞（hiPSC-CMs）对所有与 AIC 相关的基因进行功能验证。此外，还纳入了另外 3 个在 AIC 中具有潜在作用的基因（GSTM1、CBR1 和 ERBB2）。其中，38 个基因在人类胎儿心脏、成人心脏和 hiPSC-CMs 中均有表达。利用基于聚类间隔短回文重复序列/Cas9 的基因组编辑技术，在对照组 hiPSC-CMs 中系统地敲除了这 38 个基因中的每一个，并利用 hiPSC-CMs 评估了由此产生的多柔比星诱导的心脏毒性（DIC）表型。结果26个基因的敲除增加了hiPSC-CMs对DIC的易感性。值得注意的基因包括外排转运体（ABCC10、ABCC2、ABCB4、ABCC5 和 ABCC9）、成熟的 DIC 相关基因（CBR1、CBR3 和 RAC2）以及全基因组关联研究发现的基因（RARG 和 CELF4）。相反，敲除 ATP2B1、HNMT、POR、CYBA、WDR4 和 COL1A2 对 hiPSC-CMs 的体外 DIC 表型没有显著影响。结论本研究结果为 DIC 相关基因的功能验证建立了一个全面的平台，为今后研究 DIC 变异关联和开发心脏保护药物的潜在机制靶点提供了启示。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Jacc: Cardiooncology Multiple-

CiteScore

12.50

自引率

6.30%

发文量

106

期刊介绍： JACC: CardioOncology is a specialized journal that belongs to the esteemed Journal of the American College of Cardiology (JACC) family. Its purpose is to enhance cardiovascular care for cancer patients by publishing high-quality, innovative scientific research and sharing evidence-based knowledge. The journal aims to revolutionize the field of cardio-oncology and actively involve and educate professionals in both cardiovascular and oncology fields. It covers a wide range of topics including pre-clinical, translational, and clinical research, as well as best practices in cardio-oncology. Key areas of focus include understanding disease mechanisms, utilizing in vitro and in vivo models, exploring novel and traditional therapeutics (across Phase I-IV trials), studying epidemiology, employing precision medicine, and investigating primary and secondary prevention. Amyloidosis, cardiovascular risk factors, heart failure, and vascular disease are some examples of the disease states that are of particular interest to the journal. However, it welcomes research on other relevant conditions as well.

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