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人血浆载脂蛋白H与人免疫缺陷病毒1型和2型蛋白结合。

Human plasmatic apolipoprotein H binds human immunodeficiency virus type 1 and type 2 proteins.

作者信息

Stefas E, Rucheton M, Graafland H, Moynier M, Sompeyrac C, Bahraoui E M, Veas F

机构信息

OSRTOM, UR41, Montpellier, France.

出版信息

AIDS Res Hum Retroviruses. 1997 Jan 1;13(1):97-104. doi: 10.1089/aid.1997.13.97.

Abstract

Apolipoprotein H (apo H), isolated from human plasma albumin solution, was shown to capture HIV-1-related antigens from antigen-positive sera (HIV-1 AG+) of AIDS patients, by using HIV-1-specific polyclonal antibodies. In an enzyme-linked immunosorbent assay and ligand blot and dot assays, apo H was able to bind recombinant retroviral HIV antigens, especially Gag proteins p18 of HIV-1, p26 of HIV-2, and Env gp160 of HIV-1. Binding was shown to be pH and NaCl dependent, with an optimum at acidic pH and low ionic strength. Specificity was demonstrated by saturation of this binding and inhibition either by homologous competition or by specific antisera. Binding was also observed in cell line-harvested viral proteins. The mechanism of this apo H-polyspecific binding is discussed in relation to conformational changes due to the influence of lipids or detergents.

摘要

从人血浆白蛋白溶液中分离出的载脂蛋白H(apo H),通过使用HIV-1特异性多克隆抗体,被证明能够从艾滋病患者的抗原阳性血清(HIV-1 AG+)中捕获HIV-1相关抗原。在酶联免疫吸附测定、配体印迹和斑点测定中,apo H能够结合重组逆转录病毒HIV抗原,特别是HIV-1的Gag蛋白p18、HIV-2的p26以及HIV-1的Env gp160。结果表明,结合作用依赖于pH值和氯化钠,在酸性pH值和低离子强度条件下达到最佳。通过这种结合的饱和以及同源竞争或特异性抗血清的抑制作用证明了其特异性。在细胞系收获的病毒蛋白中也观察到了结合现象。本文讨论了这种apo H多特异性结合的机制与脂质或去污剂影响导致的构象变化之间的关系。

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