High‐resolution KIR and HLA genotyping in three Chinese ethnic minorities reveals distinct origins

Author:

Tao Sudan1,Norman Paul J.2,You Xuan1,Kichula Katherine M.2,Dong Lina1,Chen Nanying1,He Yizhen1,Chen Chen1ORCID,Zhang Wei1,Zhu Faming1ORCID

Affiliation:

1. Blood Center of Zhejiang Province Key Laboratory of Blood Safety Research of Zhejiang Province Zhejiang Hangzhou People's Republic of China

2. Division of Biomedical Informatics and Personalized Medicine, and Department of Immunology and Microbiology University of Colorado School of Medicine Aurora Colorado USA

Abstract

Polymorphism of killer‐cell immunoglobulin‐like receptors (KIRs) and their HLA class I ligands impacts the effector activity of cytotoxic NK cell and T cell subsets. Therefore, understanding the extent and implications of KIR and HLA class I genetic polymorphism across various populations is important for immunological and medical research. In this study, we conducted a high‐resolution investigation of KIR and HLA class I diversity in three distinct Chinese ethnic minority populations. We studied the She, Yugur, and Tajik, and compared them with the Zhejiang Han population (Zhe), which represents the majority Southern Han ethnicity. Our findings revealed that the Tajik population exhibited the most diverse KIR copy number, allele, and haplotype diversity among the four populations. This diversity aligns with their proposed ancestral origin, closely resembling that of Iranian populations, with a relatively higher presence of KIR‐B genes, alleles, and haplotypes compared with the other Chinese populations. The Yugur population displayed KIR distributions similar to those of the Tibetans and Southeast Asians, whereas the She population resembled the Zhe and other East Asians, as confirmed by genetic distance analysis of KIR. Additionally, we identified 12.9% of individuals across the three minority populations as having KIR haplotypes characterized by specific gene block insertions or deletions. Genetic analysis based on HLA alleles yielded consistent results, even though there were extensive variations in HLA alleles. The observed variations in KIR interactions, such as higher numbers of 2DL1‐C2 interactions in Tajik and Yugur populations and of 2DL3‐C1 interactions in the She population, are likely shaped by demographic and evolutionary mechanisms specific to their local environments. Overall, our findings offer valuable insights into the distribution of KIR and HLA diversity among three distinct Chinese ethnic minority populations, which can inform future clinical and population studies.

Funder

National Natural Science Foundation of China

National Institute of Allergy and Infectious Diseases

Publisher

Wiley

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