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结构域洗牌一直是形成新的类人猿杀伤细胞免疫球蛋白样受体的主要机制。

Domain shuffling has been the main mechanism forming new hominoid killer cell Ig-like receptors.

作者信息

Rajalingam Raja, Parham Peter, Abi-Rached Laurent

机构信息

Department of Structural Biology, Stanford University, 299 Campus Drive West, Stanford, CA 94305, USA.

出版信息

J Immunol. 2004 Jan 1;172(1):356-69. doi: 10.4049/jimmunol.172.1.356.

Abstract

The killer cell Ig-like receptor (KIR) gene family encodes MHC class I-specific receptors, which regulate NK cell responses and are also expressed on subpopulations of T cells. KIR haplotypes vary in gene content, which, in combination with allelic polymorphism, extensively diversifies the KIR genotype both within and between human populations. Species comparison indicates that formation of new KIR genes and loss of old ones are frequent events, so that few genes are conserved even between closely related species. In this regard, the hominoids define a time frame that is particularly informative for understanding the processes of KIR evolution and its potential impact on killer cell biology. KIR cDNA were characterized from PBMC of three gorillas, and genomic DNA were characterized for six additional individuals. Eleven gorilla KIR genes were defined. With attainment of these data, a set of 75 KIR sequences representing five hominoid species was assembled, which also included rhesus monkey, cattle, and rodent KIR. Searching this data set for recombination events, and phylogenetic analysis using Bayesian methods, demonstrated that new KIR were usually the result of recombination between loci in which complete protein domains were shuffled. Further phylogenetic analysis of the KIR sequences after removal of confounding recombined segments showed that only two KIR genes, KIR2DL4 and KIR2DL5, have been preserved throughout hominoid evolution, and one of them, KIR2DL4, is also common to rhesus monkey and hominoids. Other KIR genes represent recombinant forms present in a minority of species, often only one, as exemplified by 8 of the 11 gorilla KIR genes.

摘要

杀伤细胞免疫球蛋白样受体(KIR)基因家族编码MHC I类特异性受体,该受体调节自然杀伤细胞(NK细胞)反应,也在T细胞亚群上表达。KIR单倍型的基因组成各不相同,再加上等位基因多态性,使得人类群体内部和群体之间的KIR基因型广泛多样化。物种比较表明,新KIR基因的形成和旧KIR基因的丢失是常见事件,因此即使在亲缘关系密切的物种之间,也只有少数基因是保守的。在这方面,类人猿定义了一个特别有助于理解KIR进化过程及其对杀伤细胞生物学潜在影响的时间框架。从三只大猩猩的外周血单核细胞(PBMC)中鉴定出KIR cDNA,并对另外六只个体的基因组DNA进行了鉴定。确定了11个大猩猩KIR基因。获得这些数据后,组装了一组代表五个类人猿物种(还包括恒河猴、牛和啮齿动物的KIR)的75个KIR序列。在该数据集中搜索重组事件,并使用贝叶斯方法进行系统发育分析,结果表明新的KIR通常是完整蛋白质结构域被改组的基因座之间重组的结果。去除混杂的重组片段后对KIR序列进行的进一步系统发育分析表明,在整个类人猿进化过程中仅保留了两个KIR基因,即KIR2DL4和KIR2DL5,其中一个KIR基因KIR2DL4在恒河猴和类人猿中也很常见。其他KIR基因代表少数物种(通常只有一个物种)中存在的重组形式,11个大猩猩KIR基因中的8个就是例证。

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