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αβ T 细胞受体的中央 CDR3 半胱氨酸富含于 CD8αα 上皮内淋巴细胞及其胸腺前体中。

αβ T-cell receptors with a central CDR3 cysteine are enriched in CD8αα intraepithelial lymphocytes and their thymic precursors.

机构信息

Infection and Immunity Program, Monash Biomedicine Discovery Institute and Department of Biochemistry and Molecular Biology, Monash University, Melbourne, VIC, 3800, Australia.

Immunology Division, Garvan Institute of Medical Research, Sydney, NSW, 2010, Australia.

出版信息

Immunol Cell Biol. 2018 Jul;96(6):553-561. doi: 10.1111/imcb.12047. Epub 2018 May 3.

Abstract

The thymus plays a crucial role in immune tolerance by exposing developing T cells (thymocytes) to a myriad of self-antigens. Strong T-cell receptor (TCR) engagement induces tolerance in self-reactive thymocytes by stimulating apoptosis or selection into specialized T-cell lineages, including intestinal TCRαβ CD8αα intraepithelial lymphocytes (IEL). TCR-intrinsic amino acid motifs that can be used to predict whether a TCR will be strongly self-reactive remain elusive. Here, a novel TCR sequence alignment approach revealed that T-cell lineages in C57BL/6 mice had divergent usage of cysteine within two positions of the amino acid at the apex of the complementarity-determining region 3 (CDR3) of the TCRα or TCRβ chain. Compared to pre-selection thymocytes, central CDR3 cysteine usage was increased in IEL and Type A IEL precursors (IELp) and markedly decreased in Foxp3 regulatory T cells (T-reg) and naïve T cells. These findings reveal a TCR-intrinsic motif that distinguishes Type A IELp and IEL from T-reg and naïve T cells.

摘要

胸腺通过使发育中的 T 细胞(胸腺细胞)接触多种自身抗原,在免疫耐受中发挥关键作用。强烈的 T 细胞受体(TCR)结合通过刺激凋亡或选择进入专门的 T 细胞谱系,包括肠道 TCRαβ CD8αα 上皮内淋巴细胞(IEL),诱导自身反应性胸腺细胞耐受。仍然难以确定可用于预测 TCR 是否会强烈自身反应的 TCR 内在氨基酸基序。在这里,一种新的 TCR 序列比对方法表明,C57BL/6 小鼠中的 T 细胞谱系在 TCRα 或 TCRβ 链互补决定区 3(CDR3)氨基酸顶端的两个位置处的半胱氨酸使用存在差异。与预选胸腺细胞相比,中央 CDR3 半胱氨酸的使用在 IEL 和 A 型 IEL 前体(IELp)中增加,在 Foxp3 调节性 T 细胞(T-reg)和幼稚 T 细胞中显著减少。这些发现揭示了区分 A 型 IELp 和 IEL 与 T-reg 和幼稚 T 细胞的 TCR 内在基序。

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