联合基因型和祖先分析确定了与非裔美国人特应性皮炎相关的新基因位点。

IF 3.3 Q2 GENETICS & HEREDITY
HGG Advances Pub Date : 2024-10-10 Epub Date: 2024-09-07 DOI:10.1016/j.xhgg.2024.100350
Yadu Gautam, Latha Satish, Stephen Ramirez, Brittany Grashel, Jocelyn M Biagini, Lisa J Martin, Marc E Rothenberg, Gurjit K Khurana Hershey, Tesfaye B Mersha
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引用次数: 0

摘要

特应性皮炎(AD)是一种慢性瘙痒性皮肤炎症。遗传研究发现了与该病相关的多种风险因素;然而,大多数研究都来自欧洲和东亚人群。非裔美国人(AA)的混血基因组可能为发现与AD易感性相关的祖先特异性位点提供了机会。在本文中,我们利用来自非裔美国人群体的 710 例 AD 病例和 1015 例非 AD 对照,对祖先和基因型效应进行了联合分析,然后利用差异基因表达分析对 AD 进行了验证。联合分析确定了两个新的AD易感基因位点,即基因ANGPT1(8q23.1)中的rs2195989和基因间区域LURAP1L-MPDZ(9p23)中的rs62538818。混血图谱(AM)结果显示了潜在的基因组膨胀,我们实施了基因组控制,并确定了五个具有欧洲血统效应的祖源位点。AM 信号中变异的多组学功能优先排序优先考虑了 SLAIN2、RNF39 和 FOXA2 等位点。在 AA 群体中,GWAS 发现了与 AD 明显相关的变异,包括 SGK1(rs113357522,OR = 2.81)、EFR3A(rs16904552,OR = 1.725)和 MMP14(rs911912,OR = 1.791)。GWAS变异在AA人群中很常见,但在欧洲人群中却很罕见,这表明AD的风险具有非洲血统特异性。四个基因(ANGPT1、LURAP1L、EFR3A 和 SGK1)通过 AD 和健康皮肤的 qPCR 得到了进一步验证。这项研究强调了对混血人群进行基因研究的重要性,以及当地血统和基因型-血统联合效应对确定AD风险位点的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Joint genotype and ancestry analysis identify novel loci associated with atopic dermatitis in African American population.

Atopic dermatitis (AD) is a chronic itchy inflammatory disease of the skin. Genetic studies have identified multiple risk factors linked to the disease; however, most of the studies have been derived from European and East Asian populations. The admixed African American (AA) genome may provide an opportunity to discovery ancestry-specific loci involved in AD susceptibility. Herein, we present joint analysis of ancestry and genotype effects followed by validation using differential gene expression analysis on AD using 726 AD-affected individuals and 999 non-AD control individuals from the AA population, genotyped using Multi-Ethnic Global Array (MEGA) followed by imputation using the Consortium on Asthma among African Ancestry Populations in the Americas (CAAPA) reference panel. The joint analysis identified two novel AD-susceptibility loci, rs2195989 in gene ANGPT1 (8q23.1) and rs62538818 in the intergenic region between genes LURAP1L and MPDZ (9p23). Admixture mapping (AM) results showed potential genomic inflation, and we implemented genomic control and identified five ancestry-of-origin loci with European ancestry effects. The multi-omics functional prioritization of variants in AM signals prioritized the loci SLAIN2, RNF39, and FOXA2. Genome-wide association study (GWAS) identified variants significantly associated with AD in the AA population, including SGK1 (rs113357522, odds ratio [OR] = 2.81), EFR3A (rs16904552, OR = 1.725), and MMP14 (rs911912, OR = 1.791). GWAS variants were common in the AA but rare in the European population, which suggests an African-ancestry-specific risk of AD. Four genes (ANGPT1, LURAP1L, EFR3A, and SGK1) were further validated using qPCR from AD and healthy skin. This study highlighted the importance of genetic studies on admixed populations, as well as local ancestry and genotype-ancestry joint effects to identify risk loci for AD.

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来源期刊
HGG Advances
HGG Advances Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
4.30
自引率
4.50%
发文量
69
审稿时长
14 weeks
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