| Literature DB >> 27696525 |
Jianqiang Hu1,2, Lei Zhang3, Yang Yang4, Yanjie Guo2, Yanhong Fan2, Mingming Zhang1,2, Wanrong Man1,2, Erhe Gao5, Wei Hu4, Russel J Reiter6, Haichang Wang1,2, Dongdong Sun1,2.
Abstract
Melatonin reportedly protects against several cardiovascular diseases including ischemia/reperfusion (I/R), atherosclerosis, and hypertension. The present study investigated the effects and mechanisms of melatonin on cardiomyocyte autophagy, apoptosis, and mitochondrial injury in the context of myocardial infarction (MI). We demonstrated that melatonin significantly alleviated cardiac dysfunction after MI. Four weeks after MI, echocardiography and Masson staining indicated that melatonin notably mitigated adverse left ventricle remodeling. The mechanism may be associated with increased autophagy, reduced apoptosis, and alleviated mitochondrial dysfunction. Furthermore, melatonin significantly inhibited Mst1 phosphorylation while promoting Sirt1 expression after MI, which indicates that Mst1/Sirt1 signaling may serve as the downstream target of melatonin. We thus constructed a MI model using Mst1 transgenic (Mst1 Tg) and Mst1 knockout (Mst1-/- ) mice. The absence of Mst1 abolished the favorable effects of melatonin on cardiac injury after MI. Consistently, melatonin administration did not further increase autophagy, decrease apoptosis, or alleviate mitochondrial integrity and biogenesis in Mst1 knockout mice subjected to MI injury. These results suggest that melatonin alleviates postinfarction cardiac remodeling and dysfunction by upregulating autophagy, decreasing apoptosis, and modulating mitochondrial integrity and biogenesis. The attributed mechanism involved, at least in part, Mst1/Sirt1 signaling.Entities:
Keywords: autophagy; mammalian Ste20-like kinase 1; melatonin; myocardial infarction; silent information regulator 1
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Year: 2016 PMID: 27696525 DOI: 10.1111/jpi.12368
Source DB: PubMed Journal: J Pineal Res ISSN: 0742-3098 Impact factor: 13.007