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人类γδ T细胞对非肽抗原的识别机制

Recognition mechanism of non-peptide antigens by human gammadelta T cells.

作者信息

Yamashita Seiji, Tanaka Yoshimasa, Harazaki Masashi, Mikami Bunzo, Minato Nagahiro

机构信息

Department of Immunology and Cell Biology, Graduate School of Biostudies and Department of Pediatrics, Kyoto University, Kyoto 606-8501, Japan.

出版信息

Int Immunol. 2003 Nov;15(11):1301-7. doi: 10.1093/intimm/dxg129.

Abstract

The majority of gammadelta T cells in adult human blood exhibit Vgamma2/Vdelta2-TCR and specifically respond to various kinds of non-peptide antigens. In this study, we comparatively analyzed the CDR3 repertoires of Vgamma2-gamma and Vdelta2-delta chain genes in the adult and cord blood. It was confirmed that the vast majority of adult gammadelta T cells exhibited Vgamma2-gamma chains bearing a Jgamma1.2 segment with no or short N-region and Vdelta2-delta chains with a conserved hydrophobic residue (leucine, valine or isoleucine) at position 97 encoded by N-region of Vdelta/Jdelta junction (deltaL97). The cord blood cells stimulated with pyrophosphomonoester antigen in vitro showed preferential expansion of the gammadelta T cells expressing Vgamma2- and Vdelta2-TCR chains with these structural features as compared with those stimulated with a polyclonal mitogen phytohemagglutinin. TCR gene transfer studies indicated that alanine substitution of lysine at position 108 in Jgamma1.2 (gammaK108) or deltaL97 abrogated the responsiveness of Vgamma2/Vdelta2-TCR to all kinds of the non-peptide antigens without affecting the response to anti-CD3 antibody. Furthermore, alanine substitution of arginine at position 51 in Vdelta2 segment (deltaR51) adjacent to gammaK108 in the Vgamma2/Vdelta2-gammadelta TCR also abolished the antigen responsiveness. These results strongly suggested that a hydrophobic and two cationic residues (deltaL97, gammaK108 and deltaR51) clustered in a particular topology at the surface edge of the pocket structure of Vgamma2/Vdelta2-gammadelta TCR played essential roles in the recognition of non-peptide antigens.

摘要

成人血液中的大多数γδ T细胞表达Vγ2/Vδ2-TCR,并对各种非肽抗原产生特异性反应。在本研究中,我们比较分析了成人和脐血中Vγ2-γ和Vδ2-δ链基因的CDR3库。结果证实,绝大多数成人γδ T细胞表达的Vγ2-γ链带有Jγ1.2片段,无N区或N区较短,Vδ2-δ链在Vδ/Jδ连接处N区编码的第97位有一个保守的疏水残基(亮氨酸、缬氨酸或异亮氨酸)(δL97)。与用多克隆有丝分裂原植物血凝素刺激的细胞相比,体外经焦磷酸单酯抗原刺激的脐血细胞显示,表达具有这些结构特征的Vγ2-和Vδ2-TCR链的γδ T细胞优先扩增。TCR基因转移研究表明,Jγ1.2中第108位赖氨酸(γK108)或δL97的丙氨酸替代消除了Vγ2/Vδ2-TCR对各种非肽抗原的反应性,而不影响对抗CD3抗体的反应。此外,Vγ2/Vδ2-γδ TCR中与γK108相邻的Vδ2片段第51位精氨酸(δR51)的丙氨酸替代也消除了抗原反应性。这些结果强烈表明,Vγ2/Vδ2-γδ TCR口袋结构表面边缘以特定拓扑聚集的一个疏水残基和两个阳离子残基(δL97、γK108和δR51)在非肽抗原的识别中起关键作用。

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