首页> 美国卫生研究院文献>Journal of Virology >The envelope gp120 gene of human immunodeficiency virus type 1 determines the rate of CD4-positive T-cell depletion in SCID mice engrafted with human peripheral blood leukocytes.
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The envelope gp120 gene of human immunodeficiency virus type 1 determines the rate of CD4-positive T-cell depletion in SCID mice engrafted with human peripheral blood leukocytes.

机译:1型人类免疫缺陷病毒的包膜gp120基因决定了植入人外周血白细胞的SCID小鼠中CD4阳性T细胞的耗竭率。

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摘要

We have used envelope recombinant viruses generated between two molecular clones of human immunodeficiency virus type 1 (HIV-1), T-cell-tropic HIV-1SF2 and macrophage-tropic HIV-1SF162, to assess pathogenic potential in the human peripheral blood leukocyte-reconstituted severe combined immune deficiency mouse model. Recombinant HIV-1SF2 viruses expressing the envelope gp120 gene of HIV-ISF162 caused as rapid a CD4+ T-cell depletion as did HIV-1SF162. The reciprocal HIV-1SF162 recombinant virus with the HIV-1SF2 envelope caused slower CD4+ T-cell loss. Although changing the V3 loop sequence of HIV-1SF162 to that of HIV-1SF2 did not change the rate of CD4+ T-cell depletion, replacing the V3 of HIV-1SF2 with the sequence of HIV-1SF162 resulted in virus that was poorly infectious in vivo but not in vitro. These studies suggest that the envelope gene determines properties important for pathogenesis in vivo as well as for cell tropism in vitro. HIV-1 infection in vivo may have more stringent requirements for envelope conformation.
机译:我们已使用在人类免疫缺陷病毒1型(HIV-1)的两个分子克隆(嗜T细胞的HIV-1SF2和嗜巨噬细胞的HIV-1SF162)之间产生的包膜重组病毒来评估人类外周血白细胞-重组严重的联合免疫缺陷小鼠模型。表达HIV-ISF162的包膜gp120基因的重组HIV-1SF2病毒与HIV-1SF162一样迅速引起CD4 + T细胞耗竭。具有HIV-1SF2包膜的互惠HIV-1SF162重组病毒引起较慢的CD4 + T细胞丢失。尽管将HIV-1SF162的V3环序列更改为HIV-1SF2的环序列不会改变CD4 + T细胞的耗竭率,但用HIV-1SF162的序列替换HIV-1SF2的V3导致病毒在体内但非体外。这些研究表明,包膜基因决定了对于体内发病机理以及体外细胞嗜性重要的特性。体内HIV-1感染可能对包膜构象有更严格的要求。

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