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RAET1E/ULBP4 外显子 4 和 3' 非翻译区遗传结构的特征揭示了更多的多样性和等位基因多态性。

Characterisation of RAET1E/ULBP4 exon 4 and 3' untranslated region genetic architecture reveals further diversity and allelic polymorphism.

机构信息

Anthony Nolan Research Institute, Royal Free Hospital, London, UK.

UCL Cancer Institute, Royal Free Campus, London, UK.

出版信息

HLA. 2024 Apr;103(4):e15457. doi: 10.1111/tan.15457.

DOI:10.1111/tan.15457
PMID:38575368
Abstract

NKG2D is a natural killer cell activating receptor recognising ligands on infected or tumorigenic cells, leading to their cytolysis. There are eight known genes encoding NKG2D ligands: MICA, MICB and ULBP1-6. MICA and MICB are highly polymorphic and well characterised, whilst ULBP ligands are less polymorphic and the functional implication of their diversity is not well understood. Using International HLA and Immunogenetics Workshop (IHIW) cell line DNA, we previously characterised alleles of the RAET1E gene (encoding ULBP4 proteins), including the 5' UTR promoter region and exons 1-3. We found 11 promoter haplotypes associating with alleles based on exons 1-3, revealing 19 alleles overall. The current study extends this analysis using 87 individual DNA samples from IHIW cell lines or cord blood to include RAET1E exon 4 and the 3' UTR, as polymorphism in these regions have not been previously investigated. We found two novel exon 4 polymorphisms encoding amino acid substitutions altering the transmembrane domain. An amino acid substitution at residue 233 was unique to the RAET1E*008 allele whereas the substitution at residue 237 was shared between groups of alleles. Additionally, four haplotypes were found based on 3' UTR sequences, which were unique to certain alleles or shared with allele groups based on exons 1-4 polymorphisms. Furthermore, putative microRNAs were identified that may interact with these polymorphic sites, repressing transcription and potentially affecting expression levels.

摘要

NKG2D 是一种自然杀伤细胞激活受体,可识别受感染或癌变细胞上的配体,导致其细胞溶解。有八个已知的编码 NKG2D 配体的基因:MICA、MICB 和 ULBP1-6。MICA 和 MICB 高度多态性且特征明显,而 ULBP 配体的多态性较低,其多样性的功能意义尚不清楚。使用国际 HLA 和免疫遗传学研讨会 (IHIW) 细胞系 DNA,我们之前对 RAET1E 基因(编码 ULBP4 蛋白)的等位基因进行了特征描述,包括 5'UTR 启动子区域和外显子 1-3。我们根据外显子 1-3 发现了与等位基因相关的 11 个启动子单倍型,总共发现了 19 个等位基因。本研究使用来自 IHIW 细胞系或脐带血的 87 个个体 DNA 样本扩展了这一分析,包括 RAET1E 外显子 4 和 3'UTR,因为这些区域的多态性尚未被研究过。我们发现了两个新的外显子 4 多态性,编码改变跨膜结构域的氨基酸取代。残基 233 处的氨基酸取代仅存在于 RAET1E*008 等位基因中,而残基 237 的取代则存在于等位基因组之间。此外,根据 3'UTR 序列发现了四个单倍型,它们是某些等位基因所特有的,或者是根据外显子 1-4 多态性与等位基因组共享的。此外,还鉴定了可能与这些多态性位点相互作用的潜在 microRNAs,抑制转录并可能影响表达水平。

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