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T helper cell epitopes of the human immunodeficiency virus (HIV-1) nef protein in rats and chimpanzees.

作者信息

Estaquier J, Boutillon C, Ameisen J C, Gras-Masse H, Lecocq J P, Barbier B, Dixson A, Tartar A, Capron A, Auriault C

机构信息

Centre d'Immunologie des maladies transmissibles et allergiques, Unité mixte INSERM 167-CNRS 624, Institut Pasteur Lille, France.

出版信息

Mol Immunol. 1992 Apr;29(4):489-99. doi: 10.1016/0161-5890(92)90006-j.

DOI:10.1016/0161-5890(92)90006-j
PMID:1373467
Abstract

T helper cell antigenic and immunogenic determinants of the nef protein were investigated in the rat and chimpanzee models using recombinant nef protein and five synthetic peptides selected according to their amphipathic and alpha-helicity properties. The nef protein was shown to be immunogenic with both Freund's or aluminium hydroxide adjuvants. After immunization with the nef protein the 45-69 peptide was the most antigenic in rat and monkey models. In contrast, the 98-112 peptide, that required a carrier protein to induce in vitro rat T cell recall proliferation, was able to restimulate monkey T cells in the absence of a carrier. The amino acid sequence carrying the antigenic activity of the 45-69 peptide was further investigated by synthesizing short peptides overlapping this region. The antigenic sequence was precisely located in the middle of the peptide (region 50-59). This sequence was antigenic only when N alpha-acetylated. Circular dichroism analysis of the 45-69 peptide and the in vitro activity of the N-terminus group indicate in this case the involvement of the alpha-helical propensity for antigen presentation. However, the shorter sequence 50-64, able to induce a T cell reactivity, was determined as a beta-pleated sheet structure in aqueous solution. The 45-69 peptide was not only antigenic but also immunogenic and behaved in vivo as a functional T helper cell epitope. Indeed, the priming with the peptide or the transfer of peptide specific T cells to a naive recipient, followed by immunization with the nef protein, enhanced the subsequent antibody response to the nef protein. Together, these data indicate that the 45-69 peptide appears as a candidate for the in vivo elicitation of T cell immunity to the HIV-1 nef regulatory protein.

摘要

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