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Hepatitis C virus modulates human monocyte-derived dendritic cells.

机译:丙型肝炎病毒可调节人单核细胞衍生的树突状细胞。

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This study is to examine the monocyte-derived dendritic cell (DC) response to hepatitis C virus (HCV) in a cell culture system. Adherence-derived DCs were incubated with various titres of JFH-1 (HCV genotype 2a), generated from transfected Huh 7.5 cells or co-incubated with Newcastle disease virus (NDV). Infection and the type 1 interferon (IFN) response were assessed by real-time reverse transcriptase-polymerase chain reaction, morphology by light microscopy and immunophenotype by flow cytometry. Our data demonstrated no viral replication or particle release from DC after HCV infection. Morphologically, monocytes showed a tendency to shift to immature DCs when cultured with HCV, when compared with control monocytes. This shift was confirmed by flow cytometry and appeared to be related to viral titres. There was also an increase in immature DC numbers. HCV infection induced IFNbeta expression in DCs, and the amount seemed to be inversely correlated with viral titres indicating that HCV has the capacity to negatively regulate such cells. However, IFNalpha does not appear to be affected by direct contact with the virus. A strong IFNbeta signal induced by NDV in DC was substantially diminished by HCV. HCV negatively affects the maturation of DCs and suppresses the type 1 IFN response of DC. Our results suggest a mechanism of viral evasion of host immunity.
机译:这项研究旨在检查细胞培养系统中单核细胞衍生的树突状细胞(DC)对丙型肝炎病毒(HCV)的反应。将粘附来源的DC与各种滴度的JFH-1(HCV基因型2a)温育,该抗体由转染的Huh 7.5细胞产生或与新城疫病毒(NDV)共温育。通过实时逆转录酶-聚合酶链反应,光学显微镜的形态学和流式细胞术的免疫表型评估感染和1型干扰素(IFN)反应。我们的数据表明,HCV感染后无病毒复制或DC释放颗粒。从形态上讲,与对照单核细胞相比,当用HCV培养时,单核细胞表现出向未成熟DC转移的趋势。这种改变通过流式细胞术证实,并且似乎与病毒滴度有关。未成熟DC数也增加了。 HCV感染可诱导DC中IFNbeta的表达,其量似乎与病毒滴度成反比,表明HCV具有负调控此类细胞的能力。但是,IFNalpha似乎不受与病毒直接接触的影响。 HCV大大减弱了NDV在DC中诱导的强IFNbeta信号。 HCV对DC的成熟产生负面影响,并抑制DC的1型IFN反应。我们的结果表明病毒逃逸宿主免疫的机制。

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