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首页> 外文期刊>Clinical & developmental immunology. >HSV-1 miR-H6 Inhibits HSV-1 Replication and IL-6 Expression in Human Corneal Epithelial Cells In Vitro
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HSV-1 miR-H6 Inhibits HSV-1 Replication and IL-6 Expression in Human Corneal Epithelial Cells In Vitro

机译:HSV-1 miR-H6体外抑制人角膜上皮细胞中HSV-1复制和IL-6表达

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摘要

HSV-1 infection in the cornea could lead to blindness. The infected cell polypeptide 4 (ICP4) of herpes simplex virus 1 (HSV-1) is a regulator of viral transcription that is required for productive infection. It has been previously demonstrated that miR-H6 encoded from HSV-1 genome targets ICP4 to help maintain latency. In this study, synthesized miR-H6 mimics were transfected into HSV-1-infected human cornea epithelial (HCE) cells. The inhibition of HSV-1 replication and viral ICP4 expression in miR-H6-transfected HCE was confirmed by plaque assay, immunofluorescence, and Western blot. Compared to nontransfection or mock, miR-H6 produced a low-titer HSV-1 and weak ICP4 expression. In addition, miR-H6 can decrease the interleukin 6 released into the medium, which was determined by ELISA. Taken together, the data suggests that miR-H6 targeting of ICP4 inhibits HSV-1 productive infection and decreases interleukin 6 production in HCE, and this may provide an approach to prevent HSV-1 lytic infection and inhibit corneal inflammation.
机译:角膜中的HSV-1感染可能导致失明。单纯疱疹病毒1(HSV-1)的感染细胞多肽4(ICP4)是生产性感染所需的病毒转录调节因子。先前已经证明,从HSV-1基因组编码的miR-H6靶向ICP4以帮助维持潜伏期。在这项研究中,将合成的miR-H6模拟物转染到HSV-1感染的人角膜上皮(HCE)细胞中。通过噬斑测定,免疫荧光和Western印迹证实了miR-H6转染的HCE中HSV-1复制的抑制和病毒ICP4表达的抑制。与非转染或模拟相比,miR-H6产生的低滴度HSV-1和较弱的ICP4表达。另外,miR-H6可以减少释放到培养基中的白介素6,这是通过ELISA确定的。两者合计,数据表明ICP4的miR-H6靶向抑制HCE中HSV-1的生产性感染并减少白细胞介素6的产生,这可能提供预防HSV-1裂解性感染和抑制角膜炎症的方法。

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