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352783名芬兰人的自然杀伤(NK)细胞杀伤细胞免疫球蛋白样受体(KIR)基因含量变异与疾病的关联

Disease associations of natural killer (NK) cell KIR gene content variation in 352,783 Finns.

作者信息

Ritari Jarmo, Koskela Satu, Hyvärinen Kati, Ollila Hanna, Partanen Jukka

机构信息

Research and Development, Finnish Red Cross Blood Service, Helsinki, Finland.

Research and Development, Finnish Red Cross Blood Service, Helsinki, Finland; Blood Service Biobank, Finnish Red Cross Blood Service, Vantaa, Finland.

出版信息

Hum Immunol. 2024 Nov;85(6):111177. doi: 10.1016/j.humimm.2024.111177. Epub 2024 Nov 14.

DOI:10.1016/j.humimm.2024.111177
PMID:39546901
Abstract

Allelic, gene presence/absence, and gene-copy number variations in the KIR genes encoding Natural Killer (NK) cell surface receptors have been reported to be associated in case-control studies with infectious and autoimmune diseases, and relapse after stem cell transplantation. To understand more comprehensively the role of KIR gene presence/absence variation and HLA-KIR interactions in disease susceptibility, we imputed from genome SNP data the presence and absence of 10 KIR genes in the FinnGen cohort. The cohort consists of 352,783 Finns with extensive phenotypes from the national health registries. We tested associations between 762 FinnGen phenotypes and presence/absence variation based on imputation of KIR genes using 5,900 SNPs located in the KIR genomic segment. Our results provide a platform to query HLA-KIR associations in a large population cohort. We found 13 phenotype - KIR gene or KIR - HLA C combination associations with false discovery rate < 0.05. These results differ from the very high number of associations between HLA alleles and diseases reported earlier in the FinnGen cohort. Five of the 13 significant associations included malignant phenotypes, e.g., melanoma, thyroid gland neoplasm, and haematopoietic malignancy, supporting the essential role of NK cells in controlling malignancy.

摘要

据报道,在病例对照研究中,编码自然杀伤(NK)细胞表面受体的杀伤细胞免疫球蛋白样受体(KIR)基因中的等位基因、基因存在/缺失以及基因拷贝数变异与感染性疾病、自身免疫性疾病和干细胞移植后的复发有关。为了更全面地了解KIR基因存在/缺失变异和HLA-KIR相互作用在疾病易感性中的作用,我们从基因组SNP数据中推断出芬兰基因队列中10个KIR基因的存在与否。该队列由352,783名芬兰人组成,他们具有来自国家健康登记处的广泛表型。我们使用位于KIR基因组片段中的5900个SNP,基于KIR基因的推断,测试了762种芬兰基因表型与存在/缺失变异之间的关联。我们的结果提供了一个在大型人群队列中查询HLA-KIR关联的平台。我们发现了13种表型-KIR基因或KIR-HLA C组合关联,错误发现率<0.05。这些结果与芬兰基因队列中早期报道的HLA等位基因与疾病之间大量的关联不同。13个显著关联中的5个包括恶性表型,如黑色素瘤、甲状腺肿瘤和血液系统恶性肿瘤,支持了NK细胞在控制恶性肿瘤中的重要作用。

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