Cardiomyocyte‐derived HMGB1 takes a protective role in CVB3‐induced viral myocarditis via inhibiting cardiac apoptosis

Cardiomyocyte‐derived HMGB1 takes a protective role in CVB3‐induced viral myocarditis via inhibiting cardiac apoptosis

Coxsackievirus B3 (CVB3)‐induced viral myocarditis (VMC) is characterized by immune cell infiltration and myocardial damage. High mobility group box 1 (HMGB1) is a highly conserved nuclear DNA‐binding protein that participates in DNA replication, transcriptional regulation, repair response and infla...

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Published in:Immunology and cell biology Vol. 101; no. 8; pp. 735 - 745
Main Authors: Sun, Tianle, Dong, Chunsheng, Xiong, Sidong
Format: Journal Article
Language:English
Published: United States Blackwell Science Ltd 01-09-2023
Subjects:
Apoptosis
cardiomyocyte
Cardiomyocytes
coxsackievirus B3
Cre recombinase
Cytosol
DNA biosynthesis
DNA repair
Gene regulation
Heart diseases
high mobility group box 1
High mobility group proteins
HMGB1 protein
Localization
Myocarditis
p53 Protein
p53 translocationviral myocarditis
high mobility group box 1
coxsackievirus B3
cardiomyocyte
p53 translocationviral myocarditis
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Summary:Coxsackievirus B3 (CVB3)‐induced viral myocarditis (VMC) is characterized by immune cell infiltration and myocardial damage. High mobility group box 1 (HMGB1) is a highly conserved nuclear DNA‐binding protein that participates in DNA replication, transcriptional regulation, repair response and inflammatory response in different disease models. To investigate the exact function of HMGB1 in CVB3‐induced VMC, we crossed Hmgb1‐floxed (Hmgb1f/f) mice with mice carrying a suitable Cre recombinase transgenic strain to achieve conditional inactivation of the Hmgb1 gene in a cardiomyocyte‐specific manner and to establish myocarditis. In this study, we found that cardiomyocyte‐specific Hmgb1‐deficient (Hmgb1f/fTgCre/+) mice exhibited exacerbated myocardial injury. Hmgb1‐deficient cardiomyocytes may promote early apoptosis via the p53‐mediated Bax mitochondrial pathway, as evidenced by the higher localization of p53 protein in the cytosol of Hmgb1‐deficient cardiomyocytes upon CVB3 infection. Moreover, cardiomyocyte Hmgb1‐deficient mice are more susceptible to cardiac dysfunction after infection. This study provides new insights into HMGB1 in VMC pathogenesis and a strategy for appropriate blocking of HMGB1 in the clinical treatment of VMC. In this study, we found that cardiomyocyte‐specific Hmgb1‐deficient mice exhibited exacerbated myocardial injury. Hmgb1‐deficient cardiomyocytes may promote early apoptosis via the p53‐mediated Bax mitochondrial pathway, as evidenced by the higher localization of p53 protein in the cytosol of Hmgb1‐deficient cardiomyocytes upon CVB3 infection.
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ISSN:0818-9641
1440-1711
DOI:10.1111/imcb.12660