首页> 外文期刊>The American Journal of Human Genetics >Introgression of Neandertal- and Denisovan-like Haplotypes Contributes to Adaptive Variation in Human Toll-like Receptors
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Introgression of Neandertal- and Denisovan-like Haplotypes Contributes to Adaptive Variation in Human Toll-like Receptors

机译:尼安德特人和Denisovan样单元型的渗入有助于人类通行费样受体的适应性变异。

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Pathogens and the diseases they cause have been among the most important selective forces experienced by humans during their evolutionary history. Although adaptive alleles generally arise by mutation, introgression can also be a valuable source of beneficial alleles. Archaic humans, who lived in Europe and Western Asia for more than 200,000 years, were probably well adapted to this environment and its local pathogens. It is therefore conceivable that modern humans entering Europe and Western Asia who admixed with them obtained a substantial immune advantage from the introgression of archaic alleles. Here we document a cluster of three Toll-like receptors (TLR6-TLR1-TLR10) in modem humans that carries three distinct archaic haplotypes, indicating repeated introgression from archaic humans. Two of these haplotypes are most similar to the Neandertal genome, and the third haplotype is most similar to the Denisovan genome. The Toll-like receptors are key components of innate immunity and provide an important first line of immune defense against bacteria, fungi, and parasites. The unusually high allele frequencies and unexpected levels of population differentiation indicate that there has been local positive selection on multiple haplotypes at this locus. We show that the introgressed alleles have clear functional effects in modern humans; archaic-like alleles underlie differences in the expression of the TLR genes and are associated with reduced microbial resistance and increased allergic disease in large cohorts. This provides strong evidence for recurrent adaptive introgression at the TLR6-TLR1-TLR10 locus, resulting in differences in disease phenotypes in modem humans.
机译:病原体及其引起的疾病一直是人类进化史上经历的最重要的选择力。尽管适应性等位基因通常通过突变产生,但基因渗入也可以是有益等位基因的宝贵来源。在欧洲和西亚生活了20万多年的古人类很可能已经适应了这种环境及其本地病原体。因此可以想象,进入欧洲和西亚并与之混合的现代人类从古体等位基因的渗入中获得了巨大的免疫优势。在这里,我们记录了现代人类中三个Toll样受体(TLR6-TLR1-TLR10)的簇,该簇带有三种不同的古单体型,表明古人类反复渗入。这些单倍型中的两个与尼安德特人基因组最相似,第三个单倍型与Denisovan基因组最相似。 Toll样受体是先天免疫的关键组成部分,为抵抗细菌,真菌和寄生虫提供了重要的第一线免疫防御。异常高的等位基因频率和出乎意料的种群分化水平表明,在该基因座的多个单倍型上存在局部阳性选择。我们表明,渗入的等位基因在现代人类中具有明显的功能作用;古代样等位基因是TLR基因表达差异的基础,并且与微生物抗药性降低和大型人群的过敏性疾病增加有关。这为TLR6-TLR1-TLR10基因座的反复适应性基因渗入提供了有力的证据,从而导致现代人类疾病表型的差异。

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