Examination of eQTL Polymorphisms Associated with Increased Risk of Progressive Complicated Sarcoidosis in European and African Descent Subjects.

Nancy G Casanova, Sara M Camp, Manuel L Gonzalez-Garay, Ken Batai, Lori Garman, Courtney G Montgomery, Nathan Ellis, Rick Kittles, Christian Bime, Amy P Hsu, Steven Holland, Yves A Lussier, Jason Karnes, Nadera Sweiss, Lisa A Maier, Laura Koth, David R Moller, Naftali Kaminski, Joe G N Garcia
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Abstract

Background: A limited pool of SNPs are linked to the development and severity of sarcoidosis, a systemic granulomatous inflammatory disease. By integrating genome-wide association studies (GWAS) data and expression quantitative trait loci (eQTL) single nuclear polymorphisms (SNPs), we aimed to identify novel sarcoidosis SNPs potentially influencing the development of complicated sarcoidosis.

Methods: A GWAS (Affymetrix 6.0) involving 209 African-American (AA) and 193 European-American (EA, 75 and 51 complicated cases respectively) and publicly-available GWAS controls (GAIN) was utilized. Annotation of multi-tissue eQTL SNPs present on the GWAS created a pool of ~46,000 eQTL SNPs examined for association with sarcoidosis risk and severity (Logistic Model, Plink). The most significant EA/AA eQTL SNPs were genotyped in a sarcoidosis validation cohort (n=1034) and cross-validated in two independent GWAS cohorts.

Results: No single GWAS SNP achieved significance (p<1x10-8), however, analysis of the eQTL/GWAS SNP pool yielded 621 eQTL SNPs (p<10-4) associated with 730 genes that highlighted innate immunity, MHC Class II, and allograft rejection pathways with multiple SNPs validated in an independent sarcoidosis cohort (105 SNPs analyzed) (NOTCH4, IL27RA, BTNL2, ANXA11, HLA-DRB1). These studies confirm significant association of eQTL/GWAS SNPs in EAs and AAs with sarcoidosis risk and severity (complicated sarcoidosis) involving HLA region and innate immunity.

Conclusion: Despite the challenge of deciphering the genetic basis for sarcoidosis risk/severity, these results suggest that integrated eQTL/GWAS approaches may identify novel variants/genes and support the contribution of dysregulated innate immune responses to sarcoidosis severity.

研究欧洲和非洲裔受试者中与进展性并发肉样瘤病风险增加相关的 eQTL 多态性。
背景:肉样瘤病是一种全身性肉芽肿性炎症性疾病,与肉样瘤病的发病和严重程度有关的 SNPs 数量有限。通过整合全基因组关联研究(GWAS)数据和表达定量性状位点(eQTL)单核多态性(SNPs),我们旨在确定可能影响复杂性肉样瘤病发展的新型肉样瘤病SNPs:我们利用了一项涉及 209 例非洲裔美国人(AA)和 193 例欧洲裔美国人(EA,分别为 75 例和 51 例复杂病例)的 GWAS(Affymetrix 6.0)以及公开的 GWAS 对照(GAIN)。对出现在 GWAS 上的多组织 eQTL SNP 进行注释后,建立了一个约有 46,000 个 eQTL SNP 的基因库,研究其与肉样瘤病风险和严重程度的关系(逻辑模型,Plink)。最重要的 EA/AA eQTL SNP 在肉样瘤病验证队列(n=1034)中进行了基因分型,并在两个独立的 GWAS 队列中进行了交叉验证:结果:没有一个 GWAS SNP 达到显著性(p结论:尽管破译肉样瘤病风险/严重程度的遗传基础是一项挑战,但这些结果表明,综合 eQTL/GWAS 方法可能会发现新的变体/基因,并支持先天性免疫反应失调对肉样瘤病严重程度的贡献。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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