Effect of beta-chemokines on human immunodeficiency virus type 1 replication, binding, uncoating, and CCR5 receptor expression in human monocyte-derived macrophages.

Journal of human virology Pub Date : 1999-05-01

Y Jiang, P E Jolly

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Abstract

Objectives: We examined the effect and time of addition of beta-chemokines on human immunodeficiency virus type 1 (HIV-1) replication, binding, and uncoating in human macrophages and measured CCR5 receptor expression during virus binding and uncoating.

Methods: Macrophages were treated with beta-chemokines before infection, at infection, or postinfection, and virus replication was determined by p24 antigen level. Binding and uncoating of 35[S]-methionine-labeled HIV-1 was measured. CCR5 expression was determined by flow cytometry.

Results: The beta-chemokines potently inhibited virus replication. The strongest inhibition occurred when cultures were pretreated and maintained with beta-chemokines. Beta-chemokines also caused strong inhibition of viral uncoating and a considerable decrease in CCR5 expression during uncoating.

Conclusions: CCR5 receptors appear to be internalized and recycled to the cell surfaces during HIV entry. The down-regulation of CCR5 expression by beta-chemokines during virus uncoating probably accounts for the reduction in virus uncoating (entry) and hence in virus replication.

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趋化因子对人单核细胞源性巨噬细胞中人免疫缺陷病毒1型复制、结合、剥膜和CCR5受体表达的影响

目的:研究β趋化因子对人类免疫缺陷病毒1型(HIV-1)在人巨噬细胞中的复制、结合和脱壳的影响和时间，并测量病毒结合和脱壳过程中CCR5受体的表达。方法:在感染前、感染时和感染后用β趋化因子处理巨噬细胞，用p24抗原水平检测病毒复制。测定35[S]-蛋氨酸标记的HIV-1的结合和脱包。流式细胞术检测CCR5的表达。结果:趋化因子能有效抑制病毒复制。最强烈的抑制发生在培养物预处理和维持β趋化因子。趋化因子对病毒脱衣也有很强的抑制作用，在脱衣过程中CCR5的表达显著降低。结论:在HIV进入过程中，CCR5受体似乎被内化并循环到细胞表面。在病毒脱壳过程中，β趋化因子下调CCR5的表达可能是病毒脱壳(进入)减少的原因，从而导致病毒复制减少。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Journal of human virology

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