一株利用CCR5的1型原发性人类免疫缺陷病毒分离株对不依赖CD4复制的适应性
Adaptation of a CCR5-using, primary human immunodeficiency virus type 1 isolate for CD4-independent replication.
作者信息
Kolchinsky P, Mirzabekov T, Farzan M, Kiprilov E, Cayabyab M, Mooney L J, Choe H, Sodroski J
机构信息
Department of Cancer, Dana-Farber Cancer Institute, Children's Hospital, Harvard Medical School, Boston, Massachusetts 02115, USA.
出版信息
J Virol. 1999 Oct;73(10):8120-6. doi: 10.1128/JVI.73.10.8120-8126.1999.
Abstract
The gp120 envelope glycoprotein of the human immunodeficiency virus type 1 (HIV-1) promotes virus entry by sequentially binding CD4 and chemokine receptors on the target cell. Primary, clinical HIV-1 isolates require interaction with CD4 to allow gp120 to bind the CCR5 chemokine receptor efficiently. We adapted a primary HIV-1 isolate, ADA, to replicate in CD4-negative canine cells expressing human CCR5. The gp120 changes responsible for the adaptation were limited to alteration of glycosylation addition sites in the V2 loop-V1-V2 stem. The gp120 glycoproteins of the adapted viruses bound CCR5 directly, without prior interaction with CD4. Thus, a major function of CD4 binding in the entry of primary HIV-1 isolates can be bypassed by changes in the gp120 V1-V2 elements, which allow the envelope glycoproteins to assume a conformation competent for CCR5 binding.
摘要
人类免疫缺陷病毒1型(HIV-1)的包膜糖蛋白gp120通过依次结合靶细胞上的CD4和趋化因子受体来促进病毒进入。原发性临床HIV-1分离株需要与CD4相互作用,以使gp120能够有效地结合CCR5趋化因子受体。我们对一株原发性HIV-1分离株ADA进行改造,使其能在表达人CCR5的CD4阴性犬类细胞中复制。导致这种改造的gp120变化仅限于V2环-V1-V2茎中糖基化添加位点的改变。改造后的病毒的gp120糖蛋白可直接结合CCR5,无需事先与CD4相互作用。因此,gp120 V1-V2元件的变化可以绕过原发性HIV-1分离株进入过程中CD4结合的主要功能,这些变化使包膜糖蛋白能够呈现出适合与CCR5结合的构象。
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