Activation of the TCR complex by peptide-MHC and superantigens.

Q2 Medicine Experientia supplementum (2012) Pub Date : 2014-01-01 DOI:10.1007/978-3-0348-0726-5_2

Christine Louis-Dit-Sully, Britta Blumenthal, Marlena Duchniewicz, Katharina Beck-Garcia, Gina J Fiala, Esmeralda Beck-García, Markus Mukenhirn, Susana Minguet, Wolfgang W A Schamel

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引用次数: 6

Abstract

Drug hypersensitivity reactions are immune mediated, with T lymphocytes being stimulated by the drugs via their T-cell antigen receptor (TCR). In the nonpathogenic state, the TCR is activated by foreign peptides presented by major histocompatibility complex molecules (pMHC). Foreign pMHC binds with sufficient affinity to TCRαβ and thereby elicits phosphorylation of the cytoplasmic tails of the TCRαβ-associated CD3 subunits. The process is called TCR triggering. In this review, we discuss the current models of TCR triggering and which drug properties are crucial for TCR stimulation. The underlying molecular mechanisms mostly include pMHC-induced exposure of the CD3 cytoplasmic tails or alterations of the kinase-phosphatase equilibrium in the vicinity of CD3. In this review, we also discuss triggering of the TCR by small chemical compounds in context of these general mechanisms.

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肽- mhc和超抗原激活TCR复合体。

药物超敏反应是免疫介导的，药物通过T细胞抗原受体(TCR)刺激T淋巴细胞。在非致病性状态下，TCR被主要组织相容性复合体分子(pMHC)呈递的外源肽激活。外源pMHC与TCRαβ具有足够的亲和力，从而引起TCRαβ相关CD3亚基的细胞质尾部磷酸化。这个过程被称为TCR触发。在这篇综述中，我们讨论了目前的TCR触发模型以及哪些药物特性对TCR刺激至关重要。潜在的分子机制主要包括pmhc诱导的CD3细胞质尾部暴露或CD3附近激酶-磷酸酶平衡的改变。在这篇综述中，我们还讨论了在这些一般机制的背景下，小化合物触发TCR。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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