Uncovering Genetic Variation in Systemic Lupus Erythematosus Risk Variants in Indigenous Peruvians.

IF 2.9 Q2 RHEUMATOLOGY
Cristina M Lanata, Richard F Oppong, Mary K Horton, Victor Borda, Manuel F Ugarte-Gil, Joanne Nititham, Eduardo Tarazona-Santos, Timothy D O'Connor, Heinner Guio, Lindsey A Criswell
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Abstract

Objective: Systemic lupus erythematosus (SLE) results in worse clinical outcomes among individuals of Amerindian descent. The genetic basis for this is uncertain, and there is a significant lack of genetic research focused on Amerindian ancestry populations. This study aims to compare the frequencies of SLE risk variants and polygenic risk scores between Indigenous Peruvians and global populations with diverse ancestral backgrounds.

Methods: We studied 670 individuals from the Peruvian Genome Project, 2,068 individuals from the 1000 Genomes Project Phase 3 release, and 47 patients with SLE from Lima, Peru. Ancestry was inferred using admixture and RFMix. Data were imputed with the TOPMed Imputation server and annotated to hg38. We compared the frequencies of 199 SLE-associated risk variants among study participants. We also calculated SLE genetic risk scores and fixation index (FST) statistics.

Results: All 199 SLE risk single-nucleotide polymorphisms had highly significant differences in frequencies across Peruvian and other continental populations (P values <0.001). Indigenous Peruvian patients have higher polygenic risk for SLE compared to European, African, South Asian, and East Asian patients. FST analysis of SLE risk variants revealed the largest FST between Peruvian patients and African patients (mean FST 0.12), and the smallest between Peruvian patients and East Asian patients (mean FST 0.09).

Conclusion: SLE-associated variants are common among Indigenous Peruvian patients, with varying frequencies across subpopulations. This underscores the need for ongoing genetic studies in Indigenous populations, potentially explaining SLE heterogeneity.

揭示秘鲁原住民系统性红斑狼疮风险变异的遗传变异。
目的:系统性红斑狼疮(SLE)在美洲印第安人后裔中导致较差的临床结果。这种情况的遗传基础是不确定的,而且对美洲印第安人祖先群体的遗传研究明显缺乏。本研究旨在比较具有不同祖先背景的秘鲁原住民和全球人群的SLE风险变异频率和多基因风险评分。方法:我们研究了来自秘鲁基因组计划的670名个体,来自1000基因组计划3期发布的2068名个体,以及来自秘鲁利马的47名SLE患者。使用admix和RFMix推断祖先。数据通过TOPMed Imputation服务器进行输入,并标注到hg38。我们比较了研究参与者中199种与睡眠不足相关的风险变异的频率。我们还计算了SLE遗传风险评分和固定指数(FST)统计。结果:所有199个SLE风险单核苷酸多态性在秘鲁和其他大陆人群中有高度显著的频率差异(P值)。结论:SLE相关变异在秘鲁土著患者中很常见,不同亚群的频率不同。这强调了在土著人群中进行遗传研究的必要性,这可能解释SLE的异质性。
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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来源期刊
CiteScore
5.80
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