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Endocytic and exocytic regulation of CD4 expression and function.CD4表达与功能的内吞和外排调节
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Physicochemical dissociation of CD4-mediated syncytium formation and shedding of human immunodeficiency virus type 1 gp120.CD4介导的1型人类免疫缺陷病毒gp120合胞体形成及脱落的物理化学解离
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CD4内吞作用在人类免疫缺陷病毒感染中的作用。

Role of CD4 endocytosis in human immunodeficiency virus infection.

作者信息

Pelchen-Matthews A, Clapham P, Marsh M

机构信息

Medical Research Council Laboratory for Molecular Cell Biology, University College London, United Kingdom.

出版信息

J Virol. 1995 Dec;69(12):8164-8. doi: 10.1128/JVI.69.12.8164-8168.1995.

DOI:10.1128/JVI.69.12.8164-8168.1995
PMID:7494343
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC189775/
Abstract

We have analyzed the role of CD4 endocytosis in human immunodeficiency virus (HIV) entry by measuring the infection of HeLa cells expressing various CD4 constructs with endocytosis rates of between 0.2 and 30%/min in a quantitative infectious focus assay. For a number of laboratory-adapted HIV-1 and HIV-2 strains, the highest levels of infection were found on cells with very limited CD4 endocytosis, while cells with efficient CD4 uptake were only poorly infectable, suggesting that CD4 internalization is not required for HIV entry. This was confirmed in a modified assay involving prebinding of HIV-1LAI to HeLa-CD4 cells at 4 degrees C, synchronized virus entry during warming to 37 degrees C, and neutralization of virions remaining at the cell surface with anti-V3 loop antibodies. Warming cells in hypertonic medium inhibited CD4 endocytosis but did not affect the rate or the extent of infection. These studies confirm that HIV infection does not require endocytosis and that laboratory-adapted virus strains can enter HeLa-CD4 cells by fusion at the plasma membrane.

摘要

我们通过在定量感染灶测定法中测量表达各种内吞率在0.2%至30%/分钟之间的CD4构建体的HeLa细胞的感染情况,分析了CD4内吞作用在人类免疫缺陷病毒(HIV)进入过程中的作用。对于一些实验室适应的HIV-1和HIV-2毒株,在CD4内吞作用非常有限的细胞上发现了最高水平的感染,而具有高效CD4摄取能力的细胞则很难被感染,这表明HIV进入不需要CD4内化。在一项改良实验中得到了证实,该实验包括在4℃下将HIV-1LAI预结合到HeLa-CD4细胞上,在升温至37℃期间同步病毒进入,并使用抗V3环抗体中和残留在细胞表面的病毒粒子。在高渗培养基中加热细胞可抑制CD4内吞作用,但不影响感染率或感染程度。这些研究证实,HIV感染不需要内吞作用,并且实验室适应的病毒毒株可以通过在质膜处融合进入HeLa-CD4细胞。