Dimethyl fumarate induces cardiac developmental toxicity in zebrafish via down-regulation of oxidative stress

Dimethyl fumarate induces cardiac developmental toxicity in zebrafish via down-regulation of oxidative stress

Dimethyl fumarate (DMF) is an immunosuppressant commonly used to treat multiple sclerosis and other autoimmune diseases. Despite known side effects such as lymphopenia, the effect of DMF on cardiac development remains unclear. To assess this, we used zebrafish to evaluate the cardiac developmental t...

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Veröffentlicht in:Toxicology (Amsterdam) 2024-03, Vol.503, p.153735-153735, Article 153735
Hauptverfasser: Wan, Mengqi, Liu, Jiejun, Yang, Dou, Xiao, Zhonghao, Li, Xue, Liu, Jieping, Huang, Ling, Liu, Fasheng, Zhang, Shouhua, Tao, Qiang, Xiao, Juhua, Cao, Zigang
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Apoptosis
Cardiotoxicity
Dimethyl fumarate
Oxidative stress
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container_start_page 153735
container_title Toxicology (Amsterdam)
container_volume 503
creator Wan, Mengqi
Liu, Jiejun
Yang, Dou
Xiao, Zhonghao
Li, Xue
Liu, Jieping
Huang, Ling
Liu, Fasheng
Zhang, Shouhua
Tao, Qiang
Xiao, Juhua
Cao, Zigang
description Dimethyl fumarate (DMF) is an immunosuppressant commonly used to treat multiple sclerosis and other autoimmune diseases. Despite known side effects such as lymphopenia, the effect of DMF on cardiac development remains unclear. To assess this, we used zebrafish to evaluate the cardiac developmental toxicity of DMF. Our study showed that DMF reduced the survival rate of zebrafish embryos, with those exposed to 1, 1.3, and 1.6 mg/L exhibiting heart rate reduction, shortened body length, delayed yolk sac absorption, pericardial edema, increased distance from sinus venous to bulbus arteriosus, and separation of cardiomyocytes and endocardial cells at 72 hpf. Heart development-related genes showed disorder, apoptosis-related genes were up-regulated, and the oxidative stress response was down-regulated. Treatment with cysteamine ameliorated the heart development defects. Our study demonstrates that DMF induces cardiac developmental toxicity in zebrafish, possibly by down-regulating oxidative stress responses. This study provides a certain research basis for further study of DMF-induced cardiac developmental toxicity, and provides some experimental evidence for future clinical application and study of DMF.
doi_str_mv 10.1016/j.tox.2024.153735
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subjects Apoptosis
Cardiotoxicity
Dimethyl fumarate
Oxidative stress
title Dimethyl fumarate induces cardiac developmental toxicity in zebrafish via down-regulation of oxidative stress
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