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阳离子脂质体增强1型人类免疫缺陷病毒感染:CD4、血清及脂质体与细胞相互作用的作用

Enhancement of human immunodeficiency virus type 1 infection by cationic liposomes: the role of CD4, serum and liposome-cell interactions.

作者信息

Konopka K, Stamatatos L, Larsen C E, Davis B R, Düzgüneş N

机构信息

Cancer Research Institute, University of California, San Francisco 94143-0128.

出版信息

J Gen Virol. 1991 Nov;72 ( Pt 11):2685-96. doi: 10.1099/0022-1317-72-11-2685.

Abstract

We have reported previously the enhancement of the infectivity of human immunodeficiency virus type 1 (HIV-1) by liposomes composed of the cationic lipid N-[2,3-(dioleyloxy) propyl]-N,N,N-trimethylammonium chloride (DOTMA). To determine the mechanism by which this process occurs, we have investigated the role of CD4, serum concentration and liposome-cell interactions in the DOTMA-mediated stimulation of HIV-1 infection of A3.01 cells. Serum alone significantly inhibited the binding and infectivity of HIV-1, but DOTMA-mediated enhancement of infectivity was more pronounced in the presence of serum than in its absence. HIV-1 binding to cells was increased in the presence of DOTMA liposomes, DEAE-dextran and polybrene, all of which also enhanced infectivity to a similar extent at comparable concentrations. Fluorescence dequenching measurements indicated that DOTMA liposomes fused with HIV-1, but not with cell membranes, in the presence of serum. The enhancing effect of DOTMA liposomes on HIV-1 infectivity was CD4-dependent, and appeared to involve virus-liposome fusion and liposome binding to the cell surface. DOTMA liposomes did not mediate infection of the CD4-K562 and Raji cell lines.

摘要

我们之前曾报道过,由阳离子脂质N-[2,3-(二油酰氧基)丙基]-N,N,N-三甲基氯化铵(DOTMA)组成的脂质体可增强1型人类免疫缺陷病毒(HIV-1)的感染性。为了确定这一过程发生的机制,我们研究了CD4、血清浓度和脂质体-细胞相互作用在DOTMA介导的A3.01细胞HIV-1感染刺激中的作用。单独的血清可显著抑制HIV-1的结合和感染性,但在有血清存在时,DOTMA介导的感染性增强比无血清时更明显。在DOTMA脂质体、DEAE-葡聚糖和聚凝胺存在的情况下,HIV-1与细胞的结合增加,在可比浓度下,所有这些物质也能在相似程度上增强感染性。荧光猝灭测量表明,在血清存在的情况下,DOTMA脂质体与HIV-1融合,但不与细胞膜融合。DOTMA脂质体对HIV-1感染性的增强作用依赖于CD4,并且似乎涉及病毒-脂质体融合以及脂质体与细胞表面的结合。DOTMA脂质体不介导CD4-K562和Raji细胞系的感染。

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