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一种传染性胃肠炎冠状病毒核蛋白表位引发辅助性T细胞,这些细胞在体外与针对三种主要病毒结构蛋白的抗体合成过程中协同作用。

A transmissible gastroenteritis coronavirus nucleoprotein epitope elicits T helper cells that collaborate in the in vitro antibody synthesis to the three major structural viral proteins.

作者信息

Antón I M, Suñé C, Meloen R H, Borrás-Cuesta F, Enjuanes L

机构信息

Department of Molecular and Cell Biology, Campus Universidad Autónoma de Madrid, Canto Blanco, Spain.

出版信息

Virology. 1995 Oct 1;212(2):746-51. doi: 10.1006/viro.1995.1535.

Abstract

Four strong T cell epitopes have been identified studying the blastogenic response of lymphocytes from haplotype-defined transmissible gastroenteritis virus (TGEV) immune miniswine to sixty-one 15-mer synthetic peptides. Three of these epitopes are located on the nucleoprotein (N46, amino acids 46 to 60; N272, amino acids 272 to 286; and N321, amino acids 321 to 335), and one on the membrane protein (M196, amino acids 196 to 210). N321 peptide induced the highest T cell response and was recognized by immune miniswine lymphocytes with haplotypes dd, aa, and cc. T lymphocytes from peptide N321-immune miniswine reconstituted the in vitro synthesis of TGEV-specific antibodies by complementing CD4- TGEV-immune cells. This response was directed at least against the three major structural proteins. The synthesized antibodies specific for S protein preferentially recognized discontinuous epitopes and neutralized TGEV infectivity. These results show that peptide N321 defines a functional T helper epitope eliciting T cells capable of collaborating with B cells specific for different proteins of TGEV.

摘要

通过研究来自单倍型定义的传染性胃肠炎病毒(TGEV)免疫小型猪的淋巴细胞对61种15肽合成肽的增殖反应,已鉴定出4个强T细胞表位。其中3个表位位于核蛋白上(N46,氨基酸46至60;N272,氨基酸272至286;以及N321,氨基酸321至335),1个位于膜蛋白上(M196,氨基酸196至210)。N321肽诱导的T细胞反应最强,且被单倍型为dd、aa和cc的免疫小型猪淋巴细胞识别。来自N321肽免疫小型猪的T淋巴细胞通过补充CD4 - TGEV免疫细胞,在体外重建了TGEV特异性抗体的合成。这种反应至少针对三种主要结构蛋白。针对S蛋白合成的抗体优先识别不连续表位并中和TGEV的感染性。这些结果表明,肽N321定义了一个功能性T辅助表位,可引发能够与针对TGEV不同蛋白的B细胞协作的T细胞。

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