Emerging research highlights the transformative potential of
m6A RNA modification in the diagnosis and treatment of
cardiovascular diseases (CVDs). As the most abundant internal modification of
eukaryotic RNA, m6A is pivotal in regulating
gene expression,
RNA metabolism, and
cellular processes. Understanding its role in CVDs could revolutionize therapeutic strategies, offering new pathways to manage conditions like
coronary artery disease (CAD),
heart failure (HF),
pulmonary hypertension (PH), and
arrhythmias (AH).
The mechanism of
m6A modification involves the dynamic interaction between
methyltransferases (writers),
demethylases (erasers), and
m6A-binding proteins (readers). These molecular players regulate the addition and removal of m6A marks on RNA, influencing processes such as
mRNA stability,
translation efficiency, and
gene transcription. In the context of cardiovascular health, dysregulation of m6A has been linked to
vascular inflammation,
endothelial dysfunction, and
cardiac remodeling.
One of the most promising aspects of m6A research lies in its role in
coronary artery disease. Elevated m6A levels have been associated with
chronic inflammation,
atherosclerotic plaque formation, and
vascular smooth muscle cell proliferation. m6A-modifying enzymes like
METTL3 and
METTL14 influence the expression of genes involved in
lipid metabolism and
vascular integrity, potentially offering new targets for
atherosclerosis treatment. Additionally,
FTO-mediated demethylation of m6A-modified RNA has been linked to the regulation of
adipogenesis, highlighting its relevance in managing
metabolic risk factors associated with CAD.
In the case of
heart failure, m6A modification affects
myocardial cell apoptosis,
calcium homeostasis, and
ventricular remodeling. Upregulated m6A levels can impair
cardiomyocyte function and exacerbate
ventricular hypertrophy. Conversely,
downregulation of m6A methyltransferases may enhance
cardiac repair mechanisms, offering potential for
regenerative therapies. The interaction between m6A and cardiac-specific RNAs like
MHRT and
SERCA2a underscores its influence on
contractile function and
cardiac remodeling.
Pulmonary hypertension also demonstrates a significant relationship with m6A, particularly in regulating
smooth muscle cell proliferation and
vascular remodeling. Modulating m6A marks on key transcripts like
FOXO1 and
MAGE-D1 may reduce
pulmonary artery pressure and improve
vascular resistance, presenting a potential strategy for
PH management.
In the realm of
arrhythmias, m6A regulation of
calcium signaling pathways and
autonomic nerve activity can affect
cardiac electrical stability. Dysregulated m6A modifications have been observed in conditions like
atrial fibrillation, where they impact
ion channel expression and
sympathetic hyperactivity. Targeting m6A-related pathways could help
stabilize cardiac rhythm and reduce
arrhythmic risk.
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Reference
Hongjiao Liu, Tao Song, Yan Huang, The mechanism of m6A modification in cardiovascular diseases: A systematic review, Genes & Diseases, Volume 13, Issue 1, 2026, 101672,
https://doi.org/10.1016/j.gendis.2025.101672
Funding
National Natural Science Foundation of China 82100331
Natural Science Foundation of Hubei Province, China 2023AFB797
Natural Science Foundation of Hubei Province, China 2023AFB806
Knowledge Innovation Program of Wuhan-Shuguang Project (China) (2022020801020484
Fundamental Research Funds for the Central Universities of China 2042019kf0058