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一种流感病毒血凝素的合成十肽能引发具有与对完整病毒应答时相同精细识别特异性的辅助性T细胞。

A synthetic decapeptide of influenza virus hemagglutinin elicits helper T cells with the same fine recognition specificities as occur in response to whole virus.

作者信息

Hackett C J, Hurwitz J L, Dietzschold B, Gerhard W

出版信息

J Immunol. 1985 Aug;135(2):1391-4.

PMID:2409149
Abstract

The immunogenicity of an isolated murine helper T cell determinant was studied. Mice were immunized with a synthetic peptide corresponding to amino acid residues 111-120 of the influenza PR8 hemagglutinin (HA) heavy chain, a region previously identified as a major target of the helper T cell response to the HA molecule in virus-primed BALB/c mice. Lymph node T cells from these mice were fused with BW 5147 cells to produce T hybrids for clonal analysis of their recognition specificities. Three T cell hybridoma clones, obtained from two different mice, responded to the immunizing peptide when presented by syngeneic antigen-presenting cells. All of these clones responded also to antigen provided as intact wild-type PR8 virus. The fine specificity of the peptide-induced T cell hybridomas, in response to a panel of mutant and variant influenza viruses, was indistinguishable from the fine specificities of T cells to the corresponding region of the HA1 chain of the HA molecule which had been generated by priming of mice with intact wild-type virus. These results suggest that an immunogenic determinant is contained within the 111-120 sequence that is able to elicit anti-influenza virus T cells with a similar repertoire to those elicited by immunization with whole virus.

摘要

对分离出的小鼠辅助性T细胞决定簇的免疫原性进行了研究。用一种合成肽免疫小鼠,该合成肽对应于流感PR8血凝素(HA)重链的氨基酸残基111 - 120,此区域先前被确定为在病毒致敏的BALB/c小鼠中辅助性T细胞对HA分子反应的主要靶点。将这些小鼠的淋巴结T细胞与BW 5147细胞融合以产生T杂交瘤,用于克隆分析其识别特异性。从两只不同的小鼠获得的三个T细胞杂交瘤克隆,在同基因抗原呈递细胞呈递时对免疫肽有反应。所有这些克隆对完整的野生型PR8病毒提供的抗原也有反应。肽诱导的T细胞杂交瘤对一组突变和变异流感病毒的精细特异性,与用完整野生型病毒致敏小鼠产生的T细胞对HA分子HA1链相应区域的精细特异性没有区别。这些结果表明,111 - 120序列中包含一个免疫原性决定簇,该决定簇能够引发抗流感病毒T细胞,其库与用全病毒免疫引发的T细胞库相似。

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