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The evolution of vertebrate antigen receptors: A phylogenetic approach

机译:脊椎动物抗原受体的进化:系统发育方法

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Classical T cells, those with alpha beta T-cell receptors (TCRs), are an important component of the dominant paradigm for self-nonself immune recognition in vertebrates. alpha beta T cells recognize foreign peptide antigens when they are bound to MHC molecules on the surfaces of antigen-presenting cells, gamma delta T cells bear a similar receptor, and it is often assumed that these T cells also require specialized antigen-presenting molecules for immune recognition, which we term "indirect antigen recognition." B-cell receptors, or immunoglobulins, bind directly to antigens without the help of a specialized antigen-presenting molecule. Phylogenetically, it has been assumed that T-cell receptors and the genes that encode them are a monophyletic group, and that "indirect" antigen recognition evolved before the split into two types of TCR. Recently, however, it has been proposed that gamma delta-TCRs bind directly to antigens, as do immunoglobulins (Ig's). This calls into question the null hypothesis that indirect antigen recognition is a common characteristic of TCRs and, by extension, the hypothesis that all TCR gene sequences form a monophyletic group. To determine whether alternative explanations for antigen recognition and other historical relationships among TCR genes might be possible, we performed phylogenetic analyses on amino acid sequences of the constant and variable regions which encode the basic subunits of TCR and Ig molecules. We used both maximum-parsimony and genetic distance-based methods and could find no strong support for the hypothesis of TCR monophyly. Analyses of the constant region suggest that TCR gamma or delta sequences are the most ancient, implying that the ancestral immune cell was like a modern gamma delta T cell. From this gamma delta-like ancestor arose alpha beta T cells and B cells, implying that indirect antigen recognition is indeed a derived property of alpha beta-TCRs. Analyses of the variable regions are complicated by strong selection on antigen-binding sequences, but imply that direct antigen binding is the ancestral condition.
机译:经典 T 细胞,即具有 α β T 细胞受体 (TCR) 的细胞,是脊椎动物自我非自我免疫识别主导范式的重要组成部分。α-β T细胞在与抗原呈递细胞表面的MHC分子结合时识别外来肽抗原,γδT细胞携带类似的受体,通常认为这些T细胞也需要专门的抗原呈递分子进行免疫识别,我们称之为“间接抗原识别”。B细胞受体或免疫球蛋白直接与抗原结合,无需借助专门的抗原呈递分子。从系统发育学上讲,人们认为T细胞受体和编码它们的基因是一个单系群,并且“间接”抗原识别在分裂成两种类型的TCR之前就进化了。然而,最近有人提出 γ delta-TCR 直接与抗原结合,免疫球蛋白 (Ig) 也是如此。这质疑了间接抗原识别是 TCR 的共同特征的零假设,以及所有 TCR 基因序列形成单系群的假设。为了确定抗原识别和 TCR 基因之间的其他历史关系的替代解释是否可能,我们对编码 TCR 和 Ig 分子基本亚基的恒定和可变区域的氨基酸序列进行了系统发育分析。我们同时使用了最大简约和基于遗传距离的方法,并且没有发现对 TCR 单系假设的有力支持。对恒定区域的分析表明,TCR γ 或 delta 序列是最古老的,这意味着祖先免疫细胞类似于现代的 γ δ T 细胞。从这个γδ样祖先中产生了αβT细胞和B细胞,这意味着间接抗原识别确实是αβ-TCR的衍生特性。由于抗原结合序列的强选择,对可变区域的分析很复杂,但暗示直接抗原结合是祖先条件。

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