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HLA-G全基因扩增揭示了HLA-G 3'非翻译区与编码序列之间的连锁不平衡。

HLA-G whole gene amplification reveals linkage disequilibrium between the HLA-G 3'UTR and coding sequence.

作者信息

Drabbels Jos J M, Welleweerd Robert, van Rooy Inge, Johnsen Guro M, Staff Anne Cathrine, Haasnoot Geert W, Westerink Nienke, Claas Frans H J, Rozemuller Erik, Eikmans Michael

机构信息

Department of Immunohematology, Leiden University Medical Center, Leiden, The Netherlands.

GenDx, Utrecht, The Netherlands.

出版信息

HLA. 2020 Aug;96(2):179-185. doi: 10.1111/tan.13909. Epub 2020 May 17.

Abstract

Polymorphic sites in the HLA-G gene may influence expression and function of the protein. Knowledge of the association between high-resolution HLA-G alleles and 3-prime untranslated (3'UTR) haplotypes is useful for studies on the role of HLA-G in transplantation, pregnancy, and cancer. We developed a next generation sequencing (NGS)-based typing assay enabling full phasing over the whole HLA-G gene sequence with inclusion of the 3'UTR region. DNA from 171 mother-child pairs (342 samples) was studied for: (a) HLA-G allele information by the NGSgo-AmpX HLA-G assay, (b) 3'UTR haplotype information by an in-house developed sequence-based typing method of a 699/713 base pair region in the 3'UTR, and (c) the full phase HLA-G gene sequence, by combining primers from both assays. The mother to child inheritance allowed internal verification of newly identified alleles and of association between coding and UTR regions. The NGSgo workflow compatible with Illumina platforms was employed. Data was interpreted using NGSengine software. In 99.4% of all alleles analyzed, the extended typing was consistent with the separate allele and 3'UTR typing methods. After repeated analysis of four samples that showed discrepancy, consistency reached 100%. A high-linkage disequilibrium between IPD-IMGT/HLA Database-defined HLA-G alleles and the extended 3'UTR region was identified (D' = 0.994, P < .0001). Strong associations were found particularly between HLA-G01:04 and UTR-3, between HLA-G01:01:03 and UTR-7, and between HLA-G*01:03:01 and UTR-5 (for all: r = 1). Six novel HLA-G alleles and three novel 3'UTR haplotype variants were identified, of which three and one, respectively, were verified in the offspring.

摘要

HLA - G基因中的多态性位点可能会影响该蛋白的表达和功能。了解高分辨率HLA - G等位基因与3'非翻译区(3'UTR)单倍型之间的关联,对于研究HLA - G在移植、妊娠和癌症中的作用很有帮助。我们开发了一种基于下一代测序(NGS)的分型检测方法,能够对整个HLA - G基因序列进行完全定相,包括3'UTR区域。对171对母婴(342个样本)的DNA进行了研究,内容包括:(a)通过NGSgo - AmpX HLA - G检测获得HLA - G等位基因信息;(b)通过内部开发的基于序列的分型方法,对3'UTR中699/713碱基对区域进行3'UTR单倍型信息分析;(c)通过结合两种检测方法的引物获得完整定相的HLA - G基因序列。母婴遗传关系允许对新鉴定的等位基因以及编码区和UTR区之间的关联进行内部验证。采用了与Illumina平台兼容的NGSgo工作流程。使用NGSengine软件对数据进行解读。在所有分析的等位基因中,99.4%的扩展分型结果与单独的等位基因分型和3'UTR分型方法一致。对显示有差异的4个样本进行重复分析后,一致性达到了100%。在IPD - IMGT/HLA数据库定义的HLA - G等位基因与扩展的3'UTR区域之间发现了高度连锁不平衡(D' = 0.994,P < 0.0001)。尤其在HLA - G01:04与UTR - 3之间、HLA - G01:01:03与UTR - 7之间以及HLA - G*01:03:01与UTR - 5之间发现了强关联(所有情况:r = 1)。鉴定出6个新的HLA - G等位基因和3个新的3'UTR单倍型变体,其中分别有3个和1个在子代中得到验证。

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