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抗病毒疫苗接种引发的T细胞库受自身耐受性影响。

The T cell repertoire primed by antiviral vaccination is influenced by self-tolerance.

作者信息

Paliard X, Doe B, Walker C M

机构信息

Chiron Corporation, 4560 Horton Street, Emeryville, California, 94608, USA.

出版信息

Cell Immunol. 1998 Aug 25;188(1):73-9. doi: 10.1006/cimm.1998.1338.

Abstract

Vaccination can elicit CD8(+) cytotoxic T lymphocytes (CTL) that recognize peptides presented by class I MHC molecules. Relatively little is known, however, about the genetic factors that shape the repertoire of T cell clonotypes responding to any given epitope. We report here that H-2(b) mice immunized with a plasmid DNA vaccine or vaccinia virus encoding for HIV-1SF2p55gag elicit CD8(+) CTL against the H-2Db-restricted immunodominant epitope (pgagb). This response involved three different T cell populations based on their recognition of alloantigens: one that cross-reacted with the alloantigen H-2Ld, one that cross-reacted with H-2Kd, and one that did not cross-react with either H-2(d) or H-2(k) molecules. Using the TAP-deficient cell line T2-Ld, we showed that pgagb-specific CTL cross-react with H-2Ld and a yet unidentified self-peptide. In mice expressing H-2(b) and H-2(d) allotypes, we investigated whether tolerance to H-2(d) influenced the HIVp55gag-specific CTL repertoire as a consequence of thymic deletion of the cross-reactive CTL repertoire. In (H-2(dxb))F1 mice heterogygosity at the MHC-I level prevented maturation of some but not all TCR combinations specific for H-2Db+pgagb, illustrating the concept that self-tolerance can influence the repertoire of antiviral T cells.

摘要

接种疫苗可引发能识别由I类主要组织相容性复合体(MHC)分子呈递的肽段的CD8(+) 细胞毒性T淋巴细胞(CTL)。然而,对于塑造针对任何给定表位做出反应的T细胞克隆型库的遗传因素,我们了解得相对较少。我们在此报告,用编码HIV-1SF2p55gag的质粒DNA疫苗或痘苗病毒免疫的H-2(b) 小鼠会引发针对H-2Db限制性免疫显性表位(pgagb)的CD8(+) CTL。基于它们对同种抗原的识别,这种反应涉及三种不同的T细胞群体:一种与同种抗原H-2Ld发生交叉反应,一种与H-2Kd发生交叉反应,还有一种与H-2(d) 或H-2(k) 分子均不发生交叉反应。利用TAP缺陷细胞系T2-Ld,我们表明pgagb特异性CTL与H-2Ld和一种尚未鉴定的自身肽段发生交叉反应。在表达H-2(b) 和H-2(d) 同种异型的小鼠中,我们研究了由于交叉反应性CTL库在胸腺中的缺失,对H-2(d) 的耐受性是否会影响HIVp55gag特异性CTL库。在(H-2(dxb))F1小鼠中,MHC-I水平的杂合性阻止了一些但不是所有针对H-2Db+pgagb的TCR组合的成熟,这说明了自身耐受性可影响抗病毒T细胞库的这一概念。

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