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构象对HIV-1 gp120中和抗体反应的重要性。

Importance of conformation on the neutralizing antibody response to HIV-1 gp120.

作者信息

Steimer K S, Haigwood N L

机构信息

Chiron Corporation, Emeryville, California 94608-2916.

出版信息

Biotechnol Ther. 1991;2(1-2):63-89.

PMID:1726963
Abstract

We have investigated the role of conformation of HIV-1 gp120 on its potential efficacy as a subunit vaccine. The questions that we set out to answer were: 1) Are there neutralizing antibodies directed to conformational epitopes in gp120? 2) If so, what is the spectrum of virus isolates neutralized by these antibodies? 3) Is a conformationally correct gp120 subunit more effective in the induction of neutralizing antibodies than a denatured subunit? 4) Does native gp120 subunit vaccination induce a broader neutralizing response than a gp120 antigen that cannot display conformational epitopes? To address these questions, we characterized the gp120-specific antibody response of HIV-1-infected humans and of experimental animals immunized with recombinant native and nonnative gp120 subunits. Two versions of recombinant gp120 produced from the HIV-SF2 isolate of HIV-1 were employed in these studies: 1) a nonglycosylated, denatured version produced in genetically engineered yeast, which we presume is capable of presenting only linear determinants, and 2) a fully glycosylated, native version, produced in genetically engineered mammalian cells, that is capable of displaying linear as well as conformational epitopes. Antibodies directed exclusively to conformational epitopes in gp120 were purified from pooled HIV antibody-positive human sera using these two versions of HIV-SF2 gp120. These antibodies exhibited neutralizing activity, and this activity was effective in the neutralization of a different, broader spectrum of HIV-1 isolates than that of antibodies to linear determinants in gp120 purified from the same serum pool. When these two versions of HIV-SF2 gp120 were used as subunit immunogens in baboons, clear differences in their abilities to elicit neutralizing antibodies were observed. The native version was more effective in the induction of neutralizing antibodies effective against HIV-SF2, the homologous virus isolate. The isolate specificity of the neutralizing response to these two versions of HIV-SF2 gp120 also differed. The nonglycosylated version induced neutralizing antibodies that were effective against only the isolate, or closely related isolates, from which the antigen was derived. In contrast, the native version induced a neutralizing response that was effective against a broad panel of HIV-1 isolates, including at least one isolate that one would not expect to be neutralized by antibodies to the PND of HIV-SF2 gp120.

摘要

我们研究了HIV-1 gp120的构象对其作为亚单位疫苗潜在效力的作用。我们着手回答的问题是:1)是否存在针对gp120中构象表位的中和抗体?2)如果存在,这些抗体中和的病毒分离株谱是怎样的?3)构象正确的gp120亚单位在诱导中和抗体方面是否比变性亚单位更有效?4)天然gp120亚单位疫苗接种诱导的中和反应是否比不能展示构象表位的gp120抗原更广泛?为解决这些问题,我们对感染HIV-1的人类以及用重组天然和非天然gp120亚单位免疫的实验动物的gp120特异性抗体反应进行了表征。这些研究中使用了由HIV-1的HIV-SF2分离株产生的两种重组gp120:1)在基因工程酵母中产生的非糖基化、变性版本,我们推测其仅能呈现线性决定簇;2)在基因工程哺乳动物细胞中产生的完全糖基化、天然版本,其能够展示线性以及构象表位。使用这两种版本的HIV-SF2 gp120从合并的HIV抗体阳性人血清中纯化出仅针对gp120中构象表位的抗体。这些抗体表现出中和活性,并且与从同一血清库中纯化的针对gp120中线性决定簇的抗体相比,这种活性在中和不同的、更广泛的HIV-1分离株谱方面更有效。当将这两种版本的HIV-SF2 gp120用作狒狒的亚单位免疫原时,观察到它们在引发中和抗体能力方面存在明显差异。天然版本在诱导针对同源病毒分离株HIV-SF2的有效中和抗体方面更有效。对这两种版本的HIV-SF2 gp120的中和反应的分离株特异性也有所不同。非糖基化版本诱导的中和抗体仅对其抗原来源的分离株或密切相关的分离株有效。相比之下,天然版本诱导的中和反应对广泛的HIV-1分离株有效,包括至少一种人们不会预期被针对HIV-SF2 gp120的PND的抗体中和的分离株。

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