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南佛罗里达州不同西班牙裔人群队列中炎症性肠病的基因特征及其对疾病表达的影响

Genetic Characterization and Influence on Inflammatory Bowel Disease Expression in a Diverse Hispanic South Florida Cohort.

作者信息

Damas Oriana M, Gomez Lissette, Quintero Maria A, Rampersaud Evadnie, Slifer Susan, Beecham Gary W, Kerman David H, Deshpande Amar R, Sussman Daniel A, Abreu Maria T, McCauley Jacob L

机构信息

Division of Gastroenterology, Department of Medicine, University of Miami Miller School of Medicine, Miami, Florida, USA.

John P. Hussman Institute for Human Genomics, University of Miami Miller School of Medicine, Miami, Florida, USA.

出版信息

Clin Transl Gastroenterol. 2017 Apr 13;8(4):e87. doi: 10.1038/ctg.2017.13.

Abstract

OBJECTIVES

Hispanics represent an understudied inflammatory bowel disease (IBD) population. Prior studies examining genetic predisposition to IBD in Hispanics are limited. In this study, we examined whether European-derived IBD variants confer risk in Hispanics and their influence on IBD phenotype in Hispanics compared to non-Hispanic whites (NHW).

METHODS

Self-identified Hispanics and NHWs with IBD were included. Hispanic controls were included for our genetic analyses. We performed single-variant testing at previously identified Crohn's disease (CD) and ulcerative colitis (UC) IBD variants in Hispanic cases and controls. These risk variants were used to compute individual genetic risk scores. Genetic risk scores and phenotype associations were compared between Hispanic and NHW.

RESULTS

A total of 1,115 participants were included: 698 controls and 417 IBD patients (230 Hispanics). We found evidence of association within our Hispanic cohort at 22 IBD risk loci, with ~76% of the risk loci demonstrating over-representation of the European risk allele; these included loci corresponding to IL23R and NOD2 genes. CD genetic risk score for Hispanics (199.67) was similar to the score for NHW (200.33), P=0.51; the same was true in UC. Genetic risk scores did not predict IBD phenotype or complications in Hispanics or NHW except for a younger age of CD onset in Hispanics (P=0.04).

CONCLUSIONS

This study highlights the fundamental importance of these loci in IBD pathogenesis including in our diverse Hispanic population. Future studies looking at non-genetic mechanisms of disease are needed to explain differences in age of presentation and phenotype between Hispanics and NHW.

摘要

目的

西班牙裔是一个研究较少的炎症性肠病(IBD)群体。之前关于西班牙裔IBD遗传易感性的研究有限。在本研究中,我们探讨了源自欧洲的IBD变异在西班牙裔中是否会带来风险,以及与非西班牙裔白人(NHW)相比,它们对西班牙裔IBD表型的影响。

方法

纳入自我认定为患有IBD的西班牙裔和NHW。西班牙裔对照纳入我们的基因分析。我们在先前确定的西班牙裔IBD病例和对照的克罗恩病(CD)和溃疡性结肠炎(UC)IBD变异处进行单变异检测。这些风险变异用于计算个体遗传风险评分。比较西班牙裔和NHW之间的遗传风险评分及表型关联。

结果

共纳入1115名参与者:698名对照和417名IBD患者(230名西班牙裔)。我们在西班牙裔队列中的22个IBD风险位点发现了关联证据,约76%的风险位点显示欧洲风险等位基因过度表达;这些位点包括与IL23R和NOD2基因对应的位点。西班牙裔的CD遗传风险评分为199.67,与NHW的评分(200.33)相似,P = 0.51;UC情况相同。除西班牙裔CD发病年龄较小外(P = 0.04),遗传风险评分无法预测西班牙裔或NHW的IBD表型或并发症。

结论

本研究强调了这些位点在IBD发病机制中的根本重要性,包括在我们多样化的西班牙裔人群中。未来需要研究疾病的非遗传机制,以解释西班牙裔和NHW在发病年龄和表型上的差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6cfd/5415895/ce94d1dc7177/ctg201713f1.jpg

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