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Co-evolution of KIR2DL3 with HLA-C in a human population retaining minimal essential diversity of KIR and HLA class I ligands

机译:在人类中KIR2DL3与HLA-C的共同进化保留了KIR和HLA I类配体的基本必需多样性

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摘要

Natural killer (NK) cells contribute to immunity and reproduction. Guiding these functions, and NK cell education, are killer cell Ig-like receptors (KIR), NK cell receptors that recognize HLA class I. In most human populations, these highly polymorphic receptors and ligands combine with extraordinary diversity. To assess how much of this diversity is necessary, we studied KIR and HLA class I at high resolution in the Yucpa, a small South Amerindian population that survived an approximate 15,000-year history of population bottleneck and epidemic infection, including recent viral hepatitis. The Yucpa retain the three major HLA epitopes recognized by KIR. Through balancing selection on a few divergent haplotypes the Yucpa maintain much of the KIR variation found worldwide. HLA-C*07, the strongest educator of C1-specific NK cells, has reached unusually high frequency in the Yucpa. Concomitantly, weaker variants of the C1 receptor, KIR2DL3, were selected and have largely replaced the form of KIR2DL3 brought by the original migrants from Asia. HLA-C1 and KIR2DL3 homozygosity has previously been correlated with resistance to viral hepatitis. Selection of weaker forms of KIR2DL3 in the Yucpa can be seen as compensation for the high frequency of the potent HLA-C*07 ligand. This study provides an estimate of the minimal KIR-HLA system essential for long-term survival of a human population. That it contains all functional elements of KIR diversity worldwide, attests to the competitive advantage it provides, not only for surviving epidemic infections, but also for rebuilding populations once infection has passed.
机译:天然杀伤(NK)细胞有助于免疫和繁殖。指导这些功能和NK细胞教育的是杀伤细胞Ig样受体(KIR),它们是识别HLA I类的NK细胞受体。在大多数人群中,这些高度多态的受体和配体具有非凡的多样性。为了评估这种多样性的必要性,我们在尤帕(Yucpa)进行了高分辨率的KIR和HLA I类研究,这是一个小的南美人口,在人口瓶颈和流行病感染(包括最近的病毒性肝炎)中已有大约15,000年的历史。丝兰保留了KIR识别的三个主要HLA表位。通过平衡几种不同单倍型的选择,Yucpa保持了全世界发现的大部分KIR变异。 HLA-C * 07,最强的C1特异性NK细胞教育者,在丝兰达到了异常高的频率。随之而来的是,选择了C1受体的较弱变异体KIR2DL3,这些变异体已大大替代了亚洲原始移民带来的KIR2DL3形式。 HLA-C1和KIR2DL3纯合子以前与抗病毒性肝炎有关。在丝兰中选择较弱形式的KIR2DL3可以视为对有效HLA-C * 07配体高频的补偿。这项研究提供了对人类长期生存必不可少的最小KIR-HLA系统的估计。它包含了全球KIR多样性的所有功能要素,证明了它提供的竞争优势,不仅对于幸存的流行性感染,而且一旦感染过去,也可以用于重建种群。

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