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首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >Does intra-individual major histocompatibility complex diversity keep a golden mean
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Does intra-individual major histocompatibility complex diversity keep a golden mean

机译:个体内主要组织相容性复合体多样性是否保持中庸

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摘要

An adaptive immune response is usually initiated only if a major histocompatibility complex (MHC) molecule presents pathogen-derived peptides to T-cells. Every MHC molecule can present only peptides that match its peptide-binding groove. Thus, it seems advantageous for an individual to express many different MHC molecules to be able to resist many different pathogens. However, although MHC genes are the most polymorphic genes of vertebrates, each individual has only a very small subset of the diversity at the population level. This is an evolutionary paradox. We provide an overview of the current data on infection studies and mate-choice experiments and conclude that overall evidence suggests that intermediate intra-individual MHC diversity is optimal. Selective forces that may set an upper limit to intra-individual MHC diversity are discussed. An updated mathematical model based on recent findings on T-cell selection can predict the natural range of intra-individual MHC diversity. Thus, the aim of our review is to evaluate whether the number of MHC alleles usually present in individuals may be optimal to balance the advantages of presenting an increased range of peptides versus the disadvantages of an increased loss of T-cells.
机译:通常,只有在主要的组织相容性复合体(MHC)分子将病原体衍生的肽呈递给T细胞时,才启动适应性免疫反应。每个MHC分子只能呈现与其肽结合槽匹配的肽。因此,对于个体而言,表达许多不同的MHC分子以能够抵抗许多不同的病原体似乎是有利的。但是,尽管MHC基因是脊椎动物的多态性最高的基因,但每个个体在种群水平上仅具有非常小的多样性子集。这是一个进化悖论。我们提供了有关感染研究和择偶实验的最新数据的概述,并得出结论,总体证据表明,中间个体内MHC多样性是最佳的。讨论了可能为个体内MHC多样性设置上限的选择力。基于最近在T细胞选择上的发现的更新的数学模型可以预测个体MHC多样性的自然范围。因此,我们综述的目的是评估通常存在于个体中的MHC等位基因的数量是否可以最佳地平衡呈现更大范围肽段的优势与增加T细胞损失的劣势。

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