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在低细胞表面CCR5密度下,对vicriviroc耐药的HIV-1通过抑制剂-CCR5复合物的低效进入。

Inefficient entry of vicriviroc-resistant HIV-1 via the inhibitor-CCR5 complex at low cell surface CCR5 densities.

作者信息

Pugach Pavel, Ray Neelanjana, Klasse Per Johan, Ketas Thomas J, Michael Elizabeth, Doms Robert W, Lee Benhur, Moore John P

机构信息

Department of Microbiology and Immunology, Weill Medical College of Cornell University, New York, NY, USA.

出版信息

Virology. 2009 May 10;387(2):296-302. doi: 10.1016/j.virol.2009.02.044. Epub 2009 Mar 20.

DOI:10.1016/j.virol.2009.02.044
PMID:19303620
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2674391/
Abstract

HIV-1 variants resistant to small molecule CCR5 inhibitors such as vicriviroc (VVC) have modified Env complexes that can use both the inhibitor-bound and -free forms of the CCR5 co-receptor to enter target cells. However, entry via the inhibitor-CCR5 complex is inefficient in some, but not all, cell types, particularly cell lines engineered to express CCR5. We investigated the effect of increasing CCR5 expression, and hence the density of the inhibitor-CCR5 complex when a saturating inhibitor (VVC) concentration was present, by using 293-Affinofile cells, in which CCR5 expression is up-regulated by the transcriptional activator, ponasterone. When CCR5 expression was low, the resistant virus entered the target cells to a lesser extent when VVC was present than absent. However, at a higher CCR5 level, there was much less entry inhibition at a constant, saturating VVC concentration. We conclude that the relative decrease in entry of a VVC-resistant virus in some cell types results from its less efficient use of the VVC-CCR5 complex, and that increasing the CCR5 expression level can compensate for this inefficiency.

摘要

对小分子CCR5抑制剂(如维克维罗克,VVC)耐药的HIV-1变体具有修饰的Env复合物,该复合物可利用CCR5共受体的抑制剂结合形式和游离形式进入靶细胞。然而,通过抑制剂-CCR5复合物进入在某些但并非所有细胞类型中效率低下,特别是经基因工程改造以表达CCR5的细胞系。我们利用293-Affinofile细胞研究了增加CCR5表达的影响,因此在存在饱和抑制剂(VVC)浓度时增加了抑制剂-CCR5复合物的密度,在293-Affinofile细胞中,转录激活剂ponasterone可上调CCR5表达。当CCR5表达较低时,与不存在VVC时相比,存在VVC时耐药病毒进入靶细胞的程度较小。然而,在较高的CCR5水平下,在恒定的饱和VVC浓度下,进入抑制作用要小得多。我们得出结论,在某些细胞类型中,VVC耐药病毒进入的相对减少是由于其对VVC-CCR5复合物的利用效率较低,并且增加CCR5表达水平可以弥补这种低效率。

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