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Impact of genomic polymorphisms on the repertoire of human MHC class I-associated peptides

机译:基因组多态性对人类MHC I类相关肽库的影响

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For decades, the global impact of genomic polymorphisms on the repertoire of peptides presented by major histocompatibility complex (MHC) has remained a matter of speculation. Here we present a novel approach that enables high-throughput discovery of polymorphic MHC class I-associated peptides (MIPs), which play a major role in allorecognition. On the basis of comprehensive analyses of the genomic landscape of MIPs eluted from B lymphoblasts of two MHC-identical siblings, we show that 0.5% of non-synonymous single nucleotide variations are represented in the MIP repertoire. The 34 polymorphic MIPs found in our subjects are encoded by bi-allelic loci with dominant and recessive alleles. Our analyses show that, at the population level, 12% of the MIP-coding exome is polymorphic. Our method provides fundamental insights into the relationship between the genomic self and the immune self and accelerates the discovery of polymorphic MIPs (also known as minor histocompatibility antigens).RI Perreault, Claude/A-7220-2008OI Perreault, Claude/0000-0001-9453-7383
机译:几十年来,基因组多态性对主要组织相容性复合物(MHC)呈现的肽库的全球影响仍然是一个推测的问题。在这里,我们提出了一种新颖的方法,可以高通量发现多态性MHC I类相关肽(MIP),其在同种异体认知中起主要作用。在对两个相同的MHC兄弟姐妹的B淋巴母细胞洗脱的MIP的基因组图谱进行全面分析的基础上,我们显示MIP谱中有0.5%的非同义单核苷酸变异。在我们的受试者中发现的34个多态性MIP由具有等位基因和隐性等位基因的双等位基因基因座编码。我们的分析表明,在人群水平上,MIP编码外显子组中有12%是多态的。我们的方法为基因组自身与免疫自身之间的关系提供了基本的见识,并加速了多态性MIP(也称为次要组织相容性抗原)的发现.RI Perreault,Claude / A-7220-2008OI Perreault,Claude / 0000-0001- 9453-7383

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