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细胞膜中神经酰胺的富集诱导CD81内化并抑制丙型肝炎病毒进入。

Ceramide enrichment of the plasma membrane induces CD81 internalization and inhibits hepatitis C virus entry.

作者信息

Voisset Cécile, Lavie Muriel, Helle François, Op De Beeck Anne, Bilheu Angéline, Bertrand-Michel Justine, Tercé François, Cocquerel Laurence, Wychowski Czeslaw, Vu-Dac Ngoc, Dubuisson Jean

机构信息

Institut de Biologie de Lille (UMR8161), CNRS, Université de Lille I and II and Institut Pasteur de Lille, Lille, France.

出版信息

Cell Microbiol. 2008 Mar;10(3):606-17. doi: 10.1111/j.1462-5822.2007.01070.x. Epub 2007 Nov 2.

DOI:10.1111/j.1462-5822.2007.01070.x
PMID:17979982
Abstract

Virus entry is a major step in which host-cell lipids can play an essential role. In this report, we investigated the importance of sphingolipids in hepatitis C virus (HCV) entry. For this purpose, sphingomyelin present in the plasma membrane of target cells was hydrolysed into ceramide by sphingomyelinase treatment. Interestingly, ceramide enrichment of the plasma membrane strongly inhibited HCV entry. To understand how ceramide affected HCV entry, we analysed the effect of ceramide enrichment of the plasma membrane on three cell-surface molecules identified as entry factors for HCV: CD81 tetraspanin, scavenger receptor BI and Claudin-1. These proteins, which we found to be mainly associated with detergent-soluble membranes in Huh-7 cells, were not relocated in detergent-resistant microdomains after sphingomyelin hydrolysis into ceramide. Importantly, ceramide enrichment of the plasma membrane led to a 50% decrease in cell-surface CD81, which was due to its ATP-independent internalization. Our results strongly suggest that the ceramide-induced internalization of CD81 is responsible for the inhibitory effect of ceramide on HCV entry. Together, these data indicate that some specific lipids of the plasma membrane are essential for HCV entry and highlight plasma membrane lipids as potential targets to block HCV entry.

摘要

病毒进入是一个关键步骤,宿主细胞脂质在其中可发挥重要作用。在本报告中,我们研究了鞘脂在丙型肝炎病毒(HCV)进入过程中的重要性。为此,通过鞘磷脂酶处理将靶细胞质膜中的鞘磷脂水解为神经酰胺。有趣的是,质膜中神经酰胺的富集强烈抑制了HCV的进入。为了解神经酰胺如何影响HCV进入,我们分析了质膜中神经酰胺富集对三种被确定为HCV进入因子的细胞表面分子的影响:CD81四跨膜蛋白、清道夫受体BI和紧密连接蛋白-1。我们发现这些蛋白质在Huh-7细胞中主要与去污剂可溶膜相关,在鞘磷脂水解为神经酰胺后,它们并未重新定位到抗去污剂微区。重要的是,质膜中神经酰胺的富集导致细胞表面CD81减少50%,这是由于其不依赖ATP的内化作用。我们的结果强烈表明,神经酰胺诱导的CD81内化是神经酰胺对HCV进入产生抑制作用的原因。总之,这些数据表明质膜中的某些特定脂质对HCV进入至关重要,并突出了质膜脂质作为阻断HCV进入的潜在靶点。

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