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HIV-1对单核吞噬细胞的嗜性可由CD4结合域之外的gp120区域决定。

HIV-1 tropism for mononuclear phagocytes can be determined by regions of gp120 outside the CD4-binding domain.

作者信息

O'Brien W A, Koyanagi Y, Namazie A, Zhao J Q, Diagne A, Idler K, Zack J A, Chen I S

机构信息

Department of Medicine, West Los Angeles Veteran's Administration Medical Center, UCLA School of Medicine, 90073.

出版信息

Nature. 1990 Nov 1;348(6296):69-73. doi: 10.1038/348069a0.

DOI:10.1038/348069a0
PMID:2172833
Abstract

Cells of the mononuclear phagocyte system are the predominant cell producing HIV-1 in most tissues including the central nervous system (CNS), spinal cord, lung and skin; infection is associated with dementia, neuropathy, pneumonitis, and dermatitis respectively. Different HIV-1 isolates vary markedly in their ability to infect mononuclear phagocytes productively. Here we describe molecular clones of a CNS-derived isolate, HIV-1(JR-FL), which can replicate efficiently in mononuclear phagocytes. Analysis by polymerase chain reaction of early events after infection indicates that the early phase of viral replication before reverse transcription determines tropism. Genetic mapping of the macrophage-tropic phenotype by construction of recombinant viruses indicates that mononuclear phagocyte infectivity can be determined by a 157-amino-acid region of the gp 120 glycoprotein of HIV-1(JR-FL). Significantly, this region is upstream from the previously defined CD4-binding domain. We propose that at least one determinant for mononuclear phagocyte tropism involves target cell interactions with regions of gp120 distinct from the CD4-binding domain.

摘要

在包括中枢神经系统(CNS)、脊髓、肺和皮肤在内的大多数组织中,单核吞噬细胞系统的细胞是产生HIV-1的主要细胞;感染分别与痴呆、神经病变、肺炎和皮炎相关。不同的HIV-1分离株在有效感染单核吞噬细胞的能力上有显著差异。在此,我们描述了一种源自CNS的分离株HIV-1(JR-FL)的分子克隆,其能够在单核吞噬细胞中高效复制。通过聚合酶链反应对感染后早期事件进行分析表明,逆转录之前的病毒复制早期阶段决定了嗜性。通过构建重组病毒对巨噬细胞嗜性表型进行基因定位表明,单核吞噬细胞感染性可由HIV-1(JR-FL)的gp120糖蛋白的一个157个氨基酸的区域决定。重要的是,该区域位于先前定义的CD4结合域的上游。我们提出,单核吞噬细胞嗜性的至少一个决定因素涉及靶细胞与gp120中不同于CD4结合域的区域的相互作用。

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