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首页> 外文期刊>Gene therapy >Ultrasound-targeted microbubble destruction-mediated microRNA-21 transfection regulated PDCD4/NF-kappa B/TNF-alpha pathway to prevent coronary microembolization-induced cardiac dysfunction
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Ultrasound-targeted microbubble destruction-mediated microRNA-21 transfection regulated PDCD4/NF-kappa B/TNF-alpha pathway to prevent coronary microembolization-induced cardiac dysfunction

机译:超声靶向微泡破坏介导的microRNA-21转染调节PDCD4 /NF-κB/TNF-α通路,以预防冠状动脉微栓塞引起的心脏功能障碍

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摘要

The programmed cell death 4uclear factor-kappa B/tumor necrosis factor a (PDCD4/NF-kappa B/TNF-alpha) signaling pathway has an important role in coronary microembolization (CME)-induced inflammation. microRNA-21 protects myocardium mainly via regulation of its target gene PDCD4. Therefore, in this study we investigated the effect of ultrasound-guided microbubblemediated microRNA-21 transfection on cardiac function in CME pig model and determined the potential mechanisms involved. The pig CME model was established by microcatheter-mediated injection of microembolization beads into the left anterior descending artery. The CME with microRNA transfection group was injected with plasmid-microbubble mixture through the marginal ear vein 4 days before CME treatment, along with ultrasound to the myocardium. Cardiac function indices were examined by cardiac ultrasound; infarct area was measured by hematoxylin-eosin and hematoxylin-basic Fuchsin-picric acid staining of tissue pathological sections; green fluorescent protein-labeled gene expression levels were evaluated by fluorescent microscopy in frozen sections; myocardial PDCD4 and TNF-alpha mRNA levels were measured by fluorescent quantitative PCR and protein levels were measured by western blotting; and NF-kappa B activity was tested by electrophoretic mobility shift assay. Compared with the CME group, the CME with ultrasound-mediated microRNA transfection group demonstrated improved CME-induced cardiac dysfunction (P<0.05). Compared with the CME group, the CME with ultrasound-mediated microRNA transfection group showed significantly lower PDCD4 expression and NF-kappa B activity (Po0.05). Ultrasound microbubblemediated microRNA-21 transfection effectively improved CME-induced cardiac dysfunction via inhibition of PDCD4/NF-kappa B/TNF-alpha signal transduction pathway.
机译:程序性细胞死亡4 /核因子-κB/肿瘤坏死因子a(PDCD4 /NF-κB/TNF-α)信号通路在冠状动脉微栓塞(CME)诱导的炎症中具有重要作用。 microRNA-21主要通过调节其靶基因PDCD4保护心肌。因此,在这项研究中,我们研究了超声引导的微泡介导的microRNA-21转染对CME猪模型心脏功能的影响,并确定了潜在的机制。猪CME模型是通过微导管介导的微栓塞珠注入左前降支动脉而建立的。在进行CME治疗前4天,通过microRNA转染的CME组通过耳缘静脉注射质粒-微泡混合物,并超声注射至心肌。心脏超声检查心脏功能指标;通过苏木精-曙红和苏木精碱性品红-苦味酸染色对组织病理切片进行测定;在冷冻切片中通过荧光显微镜评估绿色荧光蛋白标记的基因表达水平;荧光定量PCR检测心肌PDCD4和TNF-αmRNA水平,蛋白质印迹法检测蛋白质水平。电泳迁移率变化法检测NF-κB的活性。与CME组相比,超声介导的microRNA转染组的CME改善了CME引起的心脏功能障碍(P <0.05)。与CME组相比,超声介导的microRNA转染组的CME显示PDCD4表达和NF-κB活性明显降低(Po0.05)。超声微泡介导的microRNA-21转染通过抑制PDCD4 /NF-κB/TNF-α信号转导途径有效改善了CME诱导的心脏功能障碍。

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