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本文引用的文献

1
Tetherin inhibits HIV-1 release by directly tethering virions to cells.tetherin通过将病毒粒子直接拴系到细胞上来抑制HIV-1释放。
Cell. 2009 Oct 30;139(3):499-511. doi: 10.1016/j.cell.2009.08.039.
2
The formation of cysteine-linked dimers of BST-2/tetherin is important for inhibition of HIV-1 virus release but not for sensitivity to Vpu.BST-2/栓系蛋白的半胱氨酸连接二聚体的形成对于抑制HIV-1病毒释放很重要,但对Vpu的敏感性而言并非如此。
Retrovirology. 2009 Sep 8;6:80. doi: 10.1186/1742-4690-6-80.
3
HIV-1 Vpu neutralizes the antiviral factor Tetherin/BST-2 by binding it and directing its beta-TrCP2-dependent degradation.HIV-1 Vpu通过与抗病毒因子Tetherin/BST-2结合并引导其依赖β-TrCP2的降解来中和该因子。
PLoS Pathog. 2009 Sep;5(9):e1000574. doi: 10.1371/journal.ppat.1000574. Epub 2009 Sep 4.
4
The cell biology of HIV-1 virion genesis.人类免疫缺陷病毒1型病毒体产生的细胞生物学
Cell Host Microbe. 2009 Jun 18;5(6):550-8. doi: 10.1016/j.chom.2009.05.015.
5
Vpu directs the degradation of the human immunodeficiency virus restriction factor BST-2/Tetherin via a {beta}TrCP-dependent mechanism.Vpu通过一种依赖βTrCP的机制指导人类免疫缺陷病毒限制因子BST-2/拴系蛋白的降解。
J Virol. 2009 Aug;83(16):7931-47. doi: 10.1128/JVI.00242-09. Epub 2009 Jun 10.
6
Nef proteins from simian immunodeficiency viruses are tetherin antagonists.来自猿猴免疫缺陷病毒的Nef蛋白是束缚素拮抗剂。
Cell Host Microbe. 2009 Jul 23;6(1):54-67. doi: 10.1016/j.chom.2009.05.008. Epub 2009 Jun 4.
7
Vpu antagonizes BST-2-mediated restriction of HIV-1 release via beta-TrCP and endo-lysosomal trafficking.Vpu通过β-TrCP和内吞溶酶体运输拮抗BST-2介导的HIV-1释放限制。
PLoS Pathog. 2009 May;5(5):e1000450. doi: 10.1371/journal.ppat.1000450. Epub 2009 May 29.
8
Mutation of a single residue renders human tetherin resistant to HIV-1 Vpu-mediated depletion.单个残基的突变使人类束缚素对HIV-1 Vpu介导的耗竭具有抗性。
PLoS Pathog. 2009 May;5(5):e1000443. doi: 10.1371/journal.ppat.1000443. Epub 2009 May 22.
9
Species-specific activity of SIV Nef and HIV-1 Vpu in overcoming restriction by tetherin/BST2.猴免疫缺陷病毒Nef和人免疫缺陷病毒1型Vpu在克服由束缚素/BST2介导的限制作用中的种属特异性活性
PLoS Pathog. 2009 May;5(5):e1000429. doi: 10.1371/journal.ppat.1000429. Epub 2009 May 15.
10
HM1.24 is internalized from lipid rafts by clathrin-mediated endocytosis through interaction with alpha-adaptin.HM1.24通过与α-衔接蛋白相互作用,经网格蛋白介导的内吞作用从脂筏内化。
J Biol Chem. 2009 Jun 5;284(23):15927-41. doi: 10.1074/jbc.M109.005124. Epub 2009 Apr 8.

CD317/tetherin 在 HIV-1 包膜中富集,并在病毒感染后从质膜下调。

CD317/tetherin is enriched in the HIV-1 envelope and downregulated from the plasma membrane upon virus infection.

机构信息

Department of Infectious Diseases, Virology, University of Heidelberg, Im Neuenheimer Feld 324, 69120 Heidelberg, Germany.

出版信息

J Virol. 2010 May;84(9):4646-58. doi: 10.1128/JVI.02421-09. Epub 2010 Feb 10.

DOI:10.1128/JVI.02421-09
PMID:20147389
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2863769/
Abstract

CD317/Bst-2/tetherin is a host factor that restricts the release of human immunodeficiency virus type 1 (HIV-1) by trapping virions at the plasma membrane of certain producer cells. It is antagonized by the HIV-1 accessory protein Vpu. Previous light microscopy studies localized CD317 to the plasma membrane and the endosomal compartment and showed Vpu induced downregulation. In the present study, we performed quantitative immunoelectron microscopy of CD317 in cells producing wild-type or Vpu-defective HIV-1 and in control cells. Double-labeling experiments revealed that CD317 localizes to the plasma membrane, to early and recycling endosomes, and to the trans-Golgi network. CD317 largely relocated to endosomes upon HIV-1 infection, and this effect was partly counteracted by Vpu. Unexpectedly, CD317 was enriched in the membrane of viral buds and cell-associated and cell-free viruses compared to the respective plasma membrane, and this enrichment was independent of Vpu. These results suggest that the tethering activity of CD317 critically depends on its density at the cell surface and appears to be less affected by its density in the virion membrane.

摘要

CD317/Bst-2/ tetherin 是一种宿主因子,通过将病毒粒子困在某些产生细胞的质膜上来限制人类免疫缺陷病毒 1 型 (HIV-1) 的释放。它被 HIV-1 辅助蛋白 Vpu 拮抗。先前的光学显微镜研究将 CD317 定位在质膜和内体区室,并显示 Vpu 诱导的下调。在本研究中,我们对产生野生型或 Vpu 缺陷型 HIV-1 的细胞和对照细胞中的 CD317 进行了定量免疫电子显微镜研究。双标记实验表明,CD317 定位于质膜、早期和再循环内体以及高尔基网络。HIV-1 感染后,CD317 大量重定位到内体,Vpu 部分拮抗了这一效应。出乎意料的是,与相应的质膜相比,CD317 在病毒芽和细胞相关及无细胞病毒的膜中富集,这种富集与 Vpu 无关。这些结果表明,CD317 的 tethering 活性严重依赖于其在细胞表面的密度,并且似乎不太受其在病毒膜中的密度影响。