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首页> 外文期刊>Immunogenetics >Comparative genomics indicates the mammalian CD33rSiglec locus evolved by an ancient large-scale inverse duplication and suggests all Siglecs share a common ancestral region
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Comparative genomics indicates the mammalian CD33rSiglec locus evolved by an ancient large-scale inverse duplication and suggests all Siglecs share a common ancestral region

机译:比较基因组学表明哺乳动物CD33rSiglec基因座是由古代大规模逆向复制进化而来的,表明所有Siglecs都拥有一个共同的祖先区域

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The CD33-related sialic acid binding Ig-like lectins (CD33rSiglecs) are predominantly inhibitory receptors expressed on leukocytes. They are distinguishable from conserved Siglecs, such as Sialoadhesin and MAG, by their rapid evolution. A comparison of the CD33rSiglec gene cluster in different mammalian species showed that it can be divided into subclusters, A and B. The two subclusters, inverted in relation to each other, each encode a set of CD33rSiglec genes arranged head-to-tail. Two regions of strong correspondence provided evidence for a large-scale inverse duplication, encompassing the framework CEACAM-18 (CE18) and ATPBD3 (ATB3) genes that seeded the mammalian CD33rSiglec cluster. Phylogenetic analysis was consistent with the predicted inversion. Rodents appear to have undergone wholesale loss of CD33rSiglec genes after the inverse duplication. In contrast, CD33rSiglecs expanded in primates and many are now pseudogenes with features consistent with activating receptors. In contrast to mammals, the fish CD33rSiglecs clusters show no evidence of an inverse duplication. They display greater variation in cluster size and structure than mammals. The close arrangement of other Siglecs and CD33rSiglecs in fish is consistent with a common ancestral region for Siglecs. Expansion of mammalian CD33rSiglecs appears to have followed a large inverse duplication of a smaller primordial cluster over 180 million years ago, prior to eutherian/marsupial divergence. Inverse duplications in general could potentially have a stabilizing effect in maintaining the size and structure of large gene clusters, facilitating the rapid evolution of immune gene families.
机译:CD33相关的唾液酸结合Ig样凝集素(CD33rSiglecs)主要是在白细胞上表达的抑制性受体。它们的快速进化与保守的Siglecs(例如Sialoadhesin和MAG)区分开。对不同哺乳动物物种中的CD33rSiglec基因簇的比较显示,它可以分为亚簇A和B。两个彼此相对颠倒的亚簇各自编码一组CD33rSiglec基因,这些CD33rSiglec基因从头到尾排列。两个高度对应的区域为大规模反向重复提供了证据,其中包括植入哺乳动物CD33rSiglec簇的框架CEACAM-18(CE18)和ATPBD3(ATB3)基因。系统发育分析与预测的反演是一致的。反向复制后,啮齿类动物似乎已经完全丧失了CD33rSiglec基因。相反,CD33rSiglecs在灵长类动物中扩增,许多现在是假基因,其特征与激活受体一致。与哺乳动物相反,鱼的CD33rSiglecs簇没有显示出反向重复的证据。它们在簇的大小和结构上显示出比哺乳动物更大的变异。鱼中其他Siglecs和CD33rSiglecs的紧密排列与Siglecs的祖先区域一致。哺乳动物CD33rSiglecs的扩张似乎是在1亿8千万年前,在一个以太子/有袋动物发散之前,一个较小的原始基团发生了大的反向复制。一般而言,反向重复可能在保持大型基因簇的大小和结构方面具有稳定作用,从而促进免疫基因家族的快速进化。

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