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首页> 外文期刊>Human Molecular Genetics >Mechanisms of copy number variation and hybrid gene formation in the KIR immune gene complex.
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Mechanisms of copy number variation and hybrid gene formation in the KIR immune gene complex.

机译:KIR免疫基因复合体中拷贝数变异和杂种基因形成的机制。

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The fine-scale structure of the majority of copy number variation (CNV) regions remains unknown. The killer immunoglobulin receptor (KIR) gene complex exhibits significant CNV. The evolutionary plasticity of the KIRs and their broad biomedical relevance makes it important to understand how these immune receptors evolve. In this paper, we describe haplotype re-arrangement creating novel loci at the KIR complex. We completely sequenced, after fosmid cloning, two rare contracted haplotypes. Evidence of frequent hybrid KIR genes in samples from many populations suggested that re-arrangements may be frequent and selectively advantageous. We propose mechanisms for formation of novel hybrid KIR genes, facilitated by protrusive non-B DNA structures at transposon recombination sites. The heightened propensity to generate novel hybrid KIR receptors may provide a proactive evolutionary measure, to militate against pathogen evasion or subversion. We propose that CNV in KIR is an evolutionary strategy, which KIR typing for disease association must take into account.
机译:大多数拷贝数变异(CNV)区域的精细结构仍然未知。杀手免疫球蛋白受体(KIR)基因复合物表现出显着的CNV。 KIRs的进化可塑性及其广泛的生物医学相关性使得了解这些免疫受体如何进化非常重要。在本文中,我们描述了在KIR复合体上创建新基因座的单倍型重排。 fosmid克隆后,我们对两个罕见的收缩单倍型进行了完全测序。来自许多人群的样品中频繁杂交的KIR基因的证据表明,重排可能是频繁的,并且选择性地有利。我们提出了在转座子重组位点由突出的非B DNA结构促进的新型杂种KIR基因形成的机制。产生新的杂合KIR受体的倾向可能会提供一种积极的进化措施,以防止病原体逃避或颠覆。我们提出,KIR中的CNV是一种进化策略,必须将KIR类型用于疾病关联。

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