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首页> 外文期刊>Cellular microbiology >lncRNA HULC facilitates efficient loading of HCV-core protein onto lipid droplets and subsequent virus-particle release
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lncRNA HULC facilitates efficient loading of HCV-core protein onto lipid droplets and subsequent virus-particle release

机译:LNCRNA Hulc有效地将HCV核心蛋白加载到脂液滴和随后的病毒颗粒释放中

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The cellular lipid pool plays a central role in hepatitis C virus (HCV) life cycle, from establishing infection to virus propagation. Here, we show that a liver abundant long noncoding RNA, highly upregulated in liver carcinoma (HULC), is upregulated during HCV infection and manipulates the lipid pool to favour virus life cycle. Interestingly, HULC was found to be crucial for the increase in number of lipid droplets in infected cells. This effect was attributed to the role of HULC in lipid biogenesis. Further, we demonstrated that HULC knockdown decreases the association of HCV-core protein with lipid droplets. This exhibited a direct consequence on the release of HCV particles. The role of HULC in HCV-particle release was further substantiated by additional knockdown and mutation experiments. Additionally, we found that increased level of HULC in HCV-infected cells was a result of Retinoid X Receptor Alpha (RXRA)-mediated transcription, which seemed to be aided by HCV-core protein. Taken together, the results identify a distinct role of long noncoding RNA HULC in lipid dynamics during HCV infection, which provides new insights into the complex process of HCV propagation and pathogenesis.
机译:细胞脂池在丙型肝炎病毒(HCV)生命周期中起着核心作用,从建立感染病毒繁殖。在这里,我们表明,在HCV感染期间,在HCV感染期间上调肝癌(Hulc)中高度上调的肝脏丰富的长度,并且操纵脂池以支持病毒生命周期。有趣的是,赫尔康被发现对受感染细胞的脂液滴数增加至关重要。这种效果归因于Hulc在脂质生物发生中的作用。此外,我们证明Hulc敲低降低了HCV-核心蛋白与脂液滴的关联。这对HCV颗粒的释放表现出直接的结果。 Hulc在HCV颗粒释放中的作用进一步通过额外的敲低和突变实验来证实。另外,我们发现HCV感染细胞中的HulC水平增加是类视黄醇X受体α(RXRA)介导的转录的结果,该转录似乎由HCV核心蛋白辅助。在一起占据,结果鉴定了长的非分量RNA Hulc在HCV感染过程中脂质动力学中的不同作用,这为HCV繁殖和发病机制复杂过程提供了新的见解。

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