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Nef和Gag合成肽引发小鼠和灵长类动物对1型艾滋病毒抗原的抗体反应。

Nef and Gag synthetic peptide priming of antibody responses to HIV type 1 antigens in mice and primates.

作者信息

Vaslin B, Claverie J M, Benveniste O, Barre-Sinoussi F C, Dormont D

机构信息

Centre de Recherches du Service de Santé des Armées, Laboratoire de Neuropathologie Expérimentale et Neurovirologie, Fontenay-aux-Roses, France.

出版信息

AIDS Res Hum Retroviruses. 1994 Oct;10(10):1241-50. doi: 10.1089/aid.1994.10.1241.

DOI:10.1089/aid.1994.10.1241
PMID:7531460
Abstract

T epitope mapping in human immunodeficiency virus proteins provides a useful tool for AIDS vaccine design. We have previously shown that four peptides selected from the Gag polyprotein of HIV-1 were able to prime mice for in vitro lymphoproliferative responses. These responses were shown to be MHC restricted, and a pool of these peptides was able to prime mice for a subsequent humoral response to HIV-1 Gag proteins. Here we show that two of these Gag peptides are able to prime the anti-HIV-1 IgG response to heat-inactivated HIV-1 in B10Sc.Cr mice. Furthermore, we extended this study in the nonhuman primate model, and show efficient priming of the IgG response to heat-inactivated HIV-1 using the pool of four Gag peptides in baboons. Further mapping of "nonself" peptides is extended to the HIV-1 Nef protein. Three potential Nef T epitopes located at positions 137-145, 98-107, and 81-95 are also shown to prime the IgG response to HIV-1 in the mouse model, although T cell proliferation to recall peptides in vitro was not detectable. Although they have not yet been defined as major helper T epitopes in humans, using classic in vitro stimulation assays, the fact that most of them are able to prime IgG responses in animals without detectable in vitro proliferative responses does not rule out their functional helper capacity in humans.

摘要

人类免疫缺陷病毒蛋白中的T细胞表位图谱分析为艾滋病疫苗设计提供了一个有用的工具。我们之前已经表明,从HIV-1的Gag多蛋白中挑选出的四种肽能够使小鼠产生体外淋巴细胞增殖反应。这些反应显示为MHC限制性的,并且这些肽的一个组合能够使小鼠对HIV-1 Gag蛋白产生后续的体液反应。在此我们表明,这些Gag肽中的两种能够使B10Sc.Cr小鼠对热灭活的HIV-1产生抗HIV-1 IgG反应。此外,我们在非人类灵长类动物模型中扩展了这项研究,并表明在狒狒中使用四种Gag肽的组合能有效地引发对热灭活HIV-1的IgG反应。“非自身”肽的进一步图谱分析扩展到了HIV-1 Nef蛋白。位于137 - 145、98 - 107和81 - 95位的三个潜在Nef T细胞表位在小鼠模型中也显示能引发对HIV-1的IgG反应,尽管在体外未检测到对回忆肽的T细胞增殖。尽管它们尚未被确定为人类中的主要辅助性T细胞表位,但使用经典的体外刺激试验,它们中的大多数能够在动物中引发IgG反应而在体外未检测到增殖反应这一事实并不排除它们在人类中的功能性辅助能力。

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