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新世界灵长类动物夜猴中杀伤细胞免疫球蛋白样受体的谱系特异性多样化。

Lineage-specific diversification of killer cell Ig-like receptors in the owl monkey, a New World primate.

作者信息

Cadavid Luis F, Lun Cheng-Man

机构信息

Department of Biology and Institute of Genetics, Universidad Nacional de Colombia, Cr. 30 # 4508, Bogotá, Distrito Capital, Colombia.

出版信息

Immunogenetics. 2009 Jan;61(1):27-41. doi: 10.1007/s00251-008-0342-y. Epub 2008 Nov 14.

DOI:10.1007/s00251-008-0342-y
PMID:19009288
Abstract

Killer cell Ig-like receptors (KIRs) modulate the cytotoxic effects of natural killer cells. In primates, the KIRs are highly diverse as a consequence of variation in gene content, alternative domain composition, and loci polymorphism. We analyzed a bacterial artificial chromosome (BAC) clone draft sequence spanning the owl monkey KIR cluster. The draft sequence had seven ordered yet unconnected contigs containing six full-length and two partial gene models, flanked by the LILRB and FcAR framework genes. Gene models were predicted to encode KIRs with inhibitory, activating, or dual functionality. Four gene models encoded three Ig domain receptors, while three others encoded molecules with four Ig domains. The additional domain resulted from an insertion in tandem of a 2,101 bp fragment containing the last 289 bp of intron 2, exon 3, and intron 3, resulting in molecules with two D0 domains. Re-screening of the owl monkey BAC library and sequencing of partial cDNAs from an owl monkey yielded five additional KIRs, four of which encoded receptors with short cytoplasmic domains with premature stop codons due to either a single nucleotide substitution or deletion or the absence of exon 8. Phylogenetic analysis by domains showed that owl monkey KIRs were monophyletic, clustering independently from other primate KIR lineages. Retroelements found in introns, however, were shared by KIRs from different primate lineages. This suggests that the owl monkey inherited a KIR cluster with a rich history of exon shuffling upon which positive selection for ligand binding operated to diversify the receptors in a lineage-specific fashion.

摘要

杀伤细胞免疫球蛋白样受体(KIRs)可调节自然杀伤细胞的细胞毒性作用。在灵长类动物中,由于基因含量、可变结构域组成和基因座多态性的差异,KIRs具有高度多样性。我们分析了一个跨越夜猴KIR基因簇的细菌人工染色体(BAC)克隆草图序列。该草图序列有7个有序但未连接的重叠群,包含6个全长和2个部分基因模型,两侧是LILRB和FcAR框架基因。预测基因模型编码具有抑制、激活或双重功能的KIRs。4个基因模型编码3个免疫球蛋白结构域受体,另外3个编码具有4个免疫球蛋白结构域的分子。额外的结构域是由于一个2101 bp片段的串联插入导致的,该片段包含内含子2的最后289 bp、外显子3和内含子3,从而产生了具有两个D0结构域的分子。对夜猴BAC文库进行重新筛选,并对一只夜猴的部分cDNA进行测序,又获得了5个KIRs,其中4个编码的受体具有短细胞质结构域,由于单个核苷酸替换、缺失或外显子8缺失而带有提前终止密码子。通过结构域进行的系统发育分析表明,夜猴KIRs是单系的,独立于其他灵长类KIR谱系聚类。然而,内含子中发现的逆转录元件在不同灵长类谱系的KIRs中是共享的。这表明夜猴继承了一个具有丰富外显子重排历史的KIR基因簇,在此基础上,针对配体结合的正选择以谱系特异性方式使受体多样化。

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