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由肽/主要组织相容性复合体配体中的局灶性结构改变所刺激的差异性胸腺选择结果。

Differential thymic selection outcomes stimulated by focal structural alteration in peptide/major histocompatibility complex ligands.

作者信息

Ghendler Y, Teng M K, Liu J H, Witte T, Liu J, Kim K S, Kern P, Chang H C, Wang J H, Reinherz E L

机构信息

Laboratory of Immunobiology, Dana-Farber Cancer Institute and Department of Medicine, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Aug 18;95(17):10061-6. doi: 10.1073/pnas.95.17.10061.

Abstract

The T lineage repertoire is shaped by T cell receptor (TCR)-dependent positive and negative thymic selection processes. Using TCR-transgenic (N15tg) beta2-microglobulin-deficient (beta2m-/-) RAG-2(-/-) H-2(b) mice specific for the VSV8 (RGYVYQGL) octapeptide bound to Kb, we identified a single weak agonist peptide variant V4L (L4) inducing phenotypic and functional T cell maturation. The cognate VSV8 peptide, in contrast, triggers negative selection. The crystal structure of L4/Kb was determined and refined to 2.1 A for comparison with the VSV8/Kb structure at similar resolution. Aside from changes on the p4 side chain of L4 and the resulting alteration of the exposed Kb Lys-66 side chain, these two structures are essentially identical. Hence, a given TCR recognizes subtle distinctions between highly related ligands, resulting in dramatically different selection outcomes. Based on these finding and the recent structural elucidation of the N15-VSV8/Kb complex, moreover, it appears that the germ-line Valpha repertoire contributes in a significant way to positive selection.

摘要

T细胞谱系由依赖T细胞受体(TCR)的胸腺阳性和阴性选择过程塑造。利用对与Kb结合的VSV8(RGYVYQGL)八肽具有特异性的TCR转基因(N15tg)β2-微球蛋白缺陷(β2m-/-)RAG-2(-/-)H-2(b)小鼠,我们鉴定出一种单一的弱激动剂肽变体V4L(L4),它可诱导T细胞表型和功能成熟。相比之下,同源的VSV8肽会引发阴性选择。测定并将L4/Kb的晶体结构精修至2.1 Å,以便与相似分辨率下的VSV8/Kb结构进行比较。除了L4的p4侧链上的变化以及由此导致的暴露的Kb Lys-66侧链的改变外,这两种结构基本相同。因此,给定的TCR能够识别高度相关配体之间的细微差异,从而导致截然不同的选择结果。此外,基于这些发现以及最近对N15-VSV8/Kb复合物的结构解析,种系Vα谱系似乎对阳性选择有重要贡献。

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