[Viral myocarditis serum exosome-derived miR-320 promotes the apoptosis of mouse cardiomyocytes by inhibiting AKT/mTOR pathway and targeting phosphatidylinositol 3-kinase regulatory subunit 1 (Pik3r1)].

Xin Zhang, Xueqin Li, Liangyu Zhu, Guoquan Yin, Yuan Zhang, Kun Lyu
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Abstract

Objective To investigate the effect of viral myocarditis serum exosomal miR-320 on apoptosis of cardiomyocytes and its mechanism. Methods The model of viral myocarditis mice was established by intraperitoneal injection of Coxsackie virus B3. Serum exosomes were extracted by serum exosome extraction kit and co-cultured with cardiomyocytes. The uptake of exosomes by cardiomyocytes was detected by laser confocal microscopy. Cardiomyocytes were transfected with miR-320 inhibitor or mimic, and the expression level of miR-320 was detected by real-time quantitative PCR. Flow cytometry was used to detect cardiomyocyte apoptosis rate, and the expression levels of B cell lymphoma 2 (Bcl2) and Bcl2-related X protein (BAX) were tested by Western blot analysis. The prediction of miR-320 target genes and GO and KEGG enrichment analysis were tested by online database. The relationship between miR-320 and its target gene phosphoinositide-3-kinase regulatory subunit 1(Pik3r1) was examined by luciferase reporter gene. The effect of miR-320 on AKT/mTOR pathway protein was detected by Western blot analysis. Results Viral myocarditis serum exosomes promoted cardiomyocyte apoptosis, and increased the level of BAX while the level of Bcl2 was decreased. miR-320 was significantly up-regulated in myocardial tissue of viral myocarditis mice, and both pri-miR-320 and mature of miR-320 were up-regulated greatly in cardiomyocytes. The level of miR-320 in cardiomyocytes treated with viral myocarditis serum exosomes was significantly up-regulated, while transfection of miR-320 inhibitor counteracted miR-320 overexpression and reduced apoptosis rate caused by exosomes. Pik3r1 is the target gene of miR-320, and its overexpression reversed cardiomyocyte apoptosis induced by miR-320 up-regulation. The overexpression of miR-320 inhibited AKT/mTOR pathway activation. Conclusion Viral myocarditis serum exosome-derived miR-320 promotes apoptosis of mouse cardiomyocytes by inhibiting AKT/mTOR pathway by targeting Pik3r1.

[病毒性心肌炎血清外泌体来源的miR-320通过抑制AKT/mTOR通路并靶向磷脂酰肌醇3-激酶调控亚基1 (Pik3r1)促进小鼠心肌细胞凋亡]。
目的探讨病毒性心肌炎血清外泌体miR-320对心肌细胞凋亡的影响及其机制。方法腹腔注射柯萨奇B3病毒建立病毒性心肌炎小鼠模型。用血清外泌体提取试剂盒提取血清外泌体,并与心肌细胞共培养。用激光共聚焦显微镜检测心肌细胞对外泌体的摄取。用miR-320抑制剂或模拟物转染心肌细胞,通过实时定量PCR检测miR-320的表达水平。流式细胞术检测心肌细胞凋亡率,Western blot检测B细胞淋巴瘤2 (Bcl2)及Bcl2相关X蛋白(BAX)的表达水平。通过在线数据库对miR-320靶基因预测及GO和KEGG富集分析进行检验。通过荧光素酶报告基因检测miR-320与其靶基因磷酸肌醇-3激酶调控亚基1(Pik3r1)的关系。Western blot检测miR-320对AKT/mTOR通路蛋白的影响。结果病毒性心肌炎血清外泌体促进心肌细胞凋亡,BAX水平升高,Bcl2水平降低。病毒性心肌炎小鼠心肌组织中miR-320显著上调,心肌细胞中miR-320的pre -miR-320和成熟miR-320均显著上调。经病毒性心肌炎血清外泌体处理的心肌细胞中miR-320水平显著上调,转染miR-320抑制剂可抵消miR-320过表达,降低外泌体引起的凋亡率。Pik3r1是miR-320的靶基因,其过表达逆转了miR-320上调诱导的心肌细胞凋亡。过表达miR-320抑制AKT/mTOR通路的激活。结论病毒性心肌炎血清外泌体来源的miR-320通过靶向Pik3r1抑制AKT/mTOR通路促进小鼠心肌细胞凋亡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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