miRâ335 promotes stress granule formation to inhibit apoptosis by targeting ROCK2 in acute ischemic stroke.
[No authors listed]
摘要
Under harmful environmental conditions, stress granules (SGs), macromolecular aggregates that are associated with cell survival and death, are produced in the eukaryotic cytoplasm. However, whether and how microRNAs (miRNAs/miRs) modulate SG formation induced by acute ischemic stroke has not been investigated. In the present study, a rat model of middle cerebral artery occlusion (MCAO) was utilized and miRNA array proï¬ling and reverse transcriptionâquantitative polymerase chain reaction were performed. The results revealed that miRâ335 was downregulated during acute ischemic stroke, which was concomitant with reduced SG formation, enhanced apoptosis levels and increased Rho associated protein kinase 2 (ROCK2) expression. In the MCAO rat and serumâfree cell models, miRâ335 treatment upregulated SG formation, alleviated the ischemiaâinduced infarction, and decreased ROCK2 protein expression and apoptosis levels. By contrast, when compared with miRâ335 treatment, the inhibition of miRâ335 resulted in reduced SG formation and higher ROCK2 expression and apoptosis levels. Target prediction analysis and luciferase 3'âuntranslated region reporter assay identiï¬ed ROCK2 as the direct target of miRâ335. Furthermore, ROCK2 silencing enhanced SG formation and attenuated the level of apoptosis in the serumâfree cell model. In addition, ROCK2 silencing markedly inhibited the effect of miRâ335 on SG formation and apoptosis levels. Unexpectedly, the phosphorylation of Tâcell intracellular antigenâ1 was significantly inhibited by miRâ335 in the MCAO rat model, which provides a reasonable explanation for the promotional effect of miRâ335 on SG formation by specifically targeting ROCK2. In conclusion, these results demonstrate that miRâ335 promotes SG formation and inhibits apoptosis by reducing ROCK2 expression in acute ischemic stroke, which provides a possible therapeutic target for brain injury.
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基因功能
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原始数据
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文献解读
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