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MicroRNA-381 protects myocardial cell function in children and mice with viral myocarditis via targeting cyclooxygenase-2 expression

机译:MicroRNA-381通过靶向环氧化酶-2表达,保护儿童和小鼠的心肌细胞功能免受病毒性心肌炎

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摘要

The present study aimed to determine the expression of cyclooxygenase (COX)-2 and microRNA (miRNA/miR)-381 in the blood of children with viral myocarditis (VM), and investigate the association between COX-2 and miR-381 in the occurrence and development of the disease using a mouse model. A total of 26 children with VM (15 boys and 11 girls) were included in the present study. Peripheral blood was collected from all children. The mouse model of VM was constructed by coxsackievirus B3 (CVB3) infection. Peripheral blood and myocardial tissues were collected from all mice for analysis. Reverse transcription-quantitative polymerase chain reaction was used to determine the expression of COX-2 mRNA and miR-381 in serum and myocardial tissues. ELISA was used to measure the content of COX-2 protein in serum from humans and mice, and western blotting was employed to determine the expression of COX-2 protein in myocardial tissues from mice. Contents of creatine kinase (CK-MB) and lactate dehydrogenase (LDH) were evaluated using an automatic biochemical analyzer. A dual luciferase assay was conducted to identify interactions between COX-2 mRNA and miR-381. Children with VM had increased COX-2 levels and decreased miR-381 expression in peripheral blood, compared with those who had recovered from VM. CVB3 infection resulted in damage in the myocardium of mice, and elevated CK-MB and LDH contents. VM model mice exhibited increased COX-2 levels and decreased miR-381 expression in peripheral blood and myocardial tissues compared with normal mice. miR-381 binds to the 3'-untranslated seed regions of both human and mouse COX-2 mRNA to regulate their expression. The present study demonstrated that children with VM have decreased miR-381 expression and elevated COX-2 expression in peripheral blood. miR-381 may inhibit myocardial cell damage caused by CVB3 infection and protect myocardial cell function by targeting COX-2 expression.
机译:本研究旨在确定有病毒心肌炎(VM)的儿童血液中环氧氧酶(COX)-2和microRNA(miRNA / miR)-381的表达,并研究COX-2和MIR-381之间的关联使用小鼠模型的发生和发展疾病。本研究共纳入共有26名带VM(15名男孩和11名女孩)的儿童。从所有孩子收集外周血。 VM的小鼠模型由CoxSackeivirus B3(CVB3)感染构成。从所有小鼠中收集外周血和心肌组织进行分析。逆转录定量聚合酶链反应用于确定血清和心肌组织中COX-2 mRNA和miR-381的表达。 ELISA用于测量来自人和小鼠的血清中COX-2蛋白的含量,并且使用Western印迹以确定小鼠心肌组织中COX-2蛋白的表达。使用自动化生物化学分析仪评价肌酸激酶(CK-MB)和乳酸脱氢酶(LDH)的含量。进行双荧光素酶测定以鉴定COX-2 mRNA和miR-381之间的相互作用。与从VM恢复的人相比,患有VM的儿童增加了COX-2水平并降低了外周血中的miR-381表达。 CVB3感染导致小鼠心肌损伤,升高的CK-MB和LDH内容物。与正常小鼠相比,VM模型小鼠表现出增加的COX-2水平并降低了外周血和心肌组织中的miR-381表达。 miR-381与人和小鼠Cox-2 mRNA的3'-未翻译的种子区域结合,以调节其表达。本研究表明,VM的儿童在外周血中升高了miR-381表达和升高的COX-2表达。 miR-381可以通过靶向COX-2表达来抑制由CVB3感染和保护心肌细胞功能引起的心肌细胞损伤。

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  • 作者单位

    Huazhong Univ Sci &

    Technol Tongji Med Coll Wuhan Childrens Hosp Cardiol Dept Wuhan 430015;

    Huazhong Univ Sci &

    Technol Tongji Med Coll Wuhan Childrens Hosp Cardiol Dept Wuhan 430015;

    Hubei Univ Med Taihe Hosp Dept Pediat 32 Peoples South Rd Shiyan 442000 Hubei Peoples R China;

    Hubei Univ Med Taihe Hosp Dept Pediat 32 Peoples South Rd Shiyan 442000 Hubei Peoples R China;

    Hubei Univ Med Taihe Hosp Dept Pediat 32 Peoples South Rd Shiyan 442000 Hubei Peoples R China;

    Hubei Univ Med Taihe Hosp Dept Pediat 32 Peoples South Rd Shiyan 442000 Hubei Peoples R China;

    Hubei Univ Med Taihe Hosp Dept Pediat 32 Peoples South Rd Shiyan 442000 Hubei Peoples R China;

    Huazhong Univ Sci &

    Technol Tongji Med Coll Wuhan Childrens Hosp Cardiol Dept Wuhan 430015;

    Hubei Univ Med Taihe Hosp Dept Pediat 32 Peoples South Rd Shiyan 442000 Hubei Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 治疗学;
  • 关键词

    viral myocarditis; cyclooxygenase-2; miR-381;

    机译:病毒心肌炎;环氧酶-2;mir-381;

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