Determining MHC restriction of T-cell responses.

Mark Larché
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引用次数: 6

Abstract

T-cell receptors (TcR) recognize short linear peptides (9-15 amino acid long), which have been processed by an 'antigen-presenting cell' and complexed to products of the major histocompatibility complex (MHC). Peptides of the appropriate shape and charge are able to bind within the groove of the MHC molecule and it is this complex which is recognized by the TcR. The MHC molecules are highly polymorphic, but each individual will only express one maternal and one paternal allele of HLA Class 1 molecule A, B, and C and HLA Class II DR, DP, and DQ. As a result of TcR specificity and MHC restriction, a clone of T cells will bear a specific receptor which has a very limited repertoire of targets (peptide-MHC complexes). When sufficient numbers of TcR are engaged on a T-cell surface, a cascade of signal transduction events is initiated which results in cellular activation. When investigating the immune response, it may be advantageous to be able to identify which MHC molecules bind a particular peptide well and give rise to a vigorous T-cell response. Such information may be useful in generating effective vaccines. In this chapter, we provide examples of Epstein-Barr virus-transformed lymphoid cell lines and fibroblast cell lines to determine MHC restriction elements.

测定MHC对t细胞反应的限制。
t细胞受体(TcR)识别短的线性肽(9-15个氨基酸长),这些肽已被“抗原呈递细胞”处理并与主要组织相容性复合体(MHC)的产物络合。具有适当形状和电荷的多肽能够在MHC分子的凹槽内结合,正是这种复合体被TcR识别。MHC分子具有高度多态性,但每个个体只表达HLA 1类分子A、B、C和HLA II类分子DR、DP、DQ的一个母系和一个父系等位基因。由于TcR特异性和MHC的限制,T细胞的克隆将携带一个特异性受体,其靶标库(肽-MHC复合物)非常有限。当t细胞表面有足够数量的TcR参与时,一系列信号转导事件被启动,导致细胞活化。在研究免疫反应时,能够识别哪些MHC分子与特定肽结合良好并引起强烈的t细胞反应可能是有利的。这些信息可能有助于生产有效的疫苗。在本章中,我们提供了Epstein-Barr病毒转化淋巴样细胞系和成纤维细胞系的例子,以确定MHC限制因子。
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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