miR-486 improves fibrotic activity in myocardial infarction by targeting SRSF3/p21-Mediated cardiac myofibroblast senescence.
Hongyi ChenLuocheng LvRuoxu LiangWeimin GuoZhaofu LiaoYilin ChenKuikui ZhuRuijin HuangHui ZhaoQin PuZiqiang YuanZhaohua ZengXin ZhengShanshan FengXu-Feng QiDong-Qing CaiPublished in: Journal of cellular and molecular medicine (2022)
The regulation of fibrotic activities is key to improving pathological remodelling post-myocardial infarction (MI). Currently, in the clinic, safe and curative therapies for cardiac fibrosis and improvement of the pathological fibrotic environment, scar formation and pathological remodelling post-MI are lacking. Previous studies have shown that miR-486 is involved in the regulation of fibrosis. However, it is still unclear how miR-486 functions in post-MI regeneration. Here, we first demonstrated that miR-486 targeting SRSF3/p21 mediates the senescence of cardiac myofibroblasts to improve their fibrotic activity, which benefits the regeneration of MI by limiting scar size and post-MI remodelling. miR-486-targeted silencing has high potential as a novel target to improve fibrotic activity, cardiac fibrosis and pathological remodelling.
Keyphrases
- cell proliferation
- long non coding rna
- left ventricular
- long noncoding rna
- systemic sclerosis
- idiopathic pulmonary fibrosis
- stem cells
- heart failure
- dna damage
- cancer therapy
- endothelial cells
- primary care
- stress induced
- oxidative stress
- prognostic factors
- risk assessment
- transforming growth factor
- human health
- case control