全基因组关联研究揭示了西班牙裔社区健康研究/拉丁裔研究(HCHS/SOL)中脂肪酸和生物活性氧脂代谢产物的共同和独特的遗传结构。

IF 3.3 Q2 GENETICS & HEREDITY
HGG Advances Pub Date : 2025-01-09 Epub Date: 2024-12-06 DOI:10.1016/j.xhgg.2024.100390
Carolina G Downie, Heather M Highland, Mona Alotaibi, Barrett M Welch, Annie Green Howard, Susan Cheng, Nick Miller, Mohit Jain, Robert C Kaplan, Adam G Lilly, Tao Long, Tamar Sofer, Bharat Thyagarajan, Bing Yu, Kari E North, Christy L Avery
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引用次数: 0

摘要

生物活性脂肪酸衍生的氧化脂分子在介导炎症和氧化应激中起着关键作用。脂肪酸和氧化脂的循环水平受环境和遗传因素的影响;表征生物活性脂质的遗传结构可以对潜在生物学产生新的见解。我们在11,584名西班牙裔社区健康研究/拉丁裔研究(HCHS/SOL)参与者中进行了81种脂肪酸和氧脂素的全基因组关联研究(GWAS),研究基线时测量了遗传和脂质组学数据(58.6%为女性,平均年龄= 46.1岁(标准差13.8))。此外,考虑到中心性肥胖对炎症的影响,我们使用两自由度关节测试检查了与腰围的相互作用。81种氧脂类和脂肪酸中有33种具有显著的遗传性(遗传率范围为0 ~ 32.7%)。40个(49.4%)氧化脂类和脂肪酸至少有一个全基因组显著变异(p< 6.94E-11),导致19个独立的遗传位点。6个位点(先导变异次要等位基因频率[MAF]范围:0.08-0.50),包括编码去饱和酶FADS和编码OATP1B1转运蛋白SLCO1B1,显示出与两种或多种脂肪酸和氧化脂类相关。在其中的几个位点上,有证据表明,顶部变异在脂肪酸和氧化脂类之间存在共定位。其余位点仅与一种氧脂素或脂肪酸相关,包括几个CYP位点。在二自由度测试中,我们还在CARS2附近发现了一个额外的罕见变异(MAF = 0.002)。我们的分析揭示了脂肪酸和氧化脂素的共同和独特的遗传结构,提供了对遗传因素的见解,并激励了表征这些化合物并阐明其在疾病中的作用的工作。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Genome-wide association study reveals shared and distinct genetic architecture of fatty acids and oxylipins in the Hispanic Community Health Study/Study of Latinos.

Bioactive fatty acid-derived oxylipin molecules play key roles mediating inflammation and oxidative stress. Circulating levels of fatty acids and oxylipins are influenced by environmental and genetic factors; characterizing the genetic architecture of bioactive lipids could yield new insights into underlying biology. We performed a genome-wide association study (GWAS) of 81 fatty acids and oxylipins in 11,584 Hispanic Community Health Study/Study of Latinos (HCHS/SOL) participants with genetic and lipidomic data measured at study baseline (58.6% female, mean age = 46.1 years (standard deviation 13.8)). Additionally, given the effects of central obesity on inflammation, we examined interactions with waist circumference using two-degree-of-freedom joint tests. Thirty-three of the 81 oxylipins and fatty acids were significantly heritable (heritability range: 0-32.7%). Forty (49.4%) oxylipins and fatty acids had at least one genome-wide significant (p < 6.94E-11) variant resulting in 19 independent genetic loci. Six loci (lead variant minor allele frequency [MAF] range: 0.08-0.50), including desaturase-encoding FADS and OATP1B1 transporter protein-encoding SLCO1B1, exhibited associations with two or more fatty acids and oxylipins. At several of these loci, there was evidence of colocalization of the top variant across fatty acids and oxylipins. The remaining loci were only associated with one oxylipin or fatty acid and included several CYP loci. We also identified an additional rare variant (MAF = 0.002) near CARS2 in two-degree-of-freedom tests. Our analyses revealed shared and distinct genetic architecture underlying fatty acids and oxylipins, providing insights into genetic factors and motivating work to characterize these compounds and elucidate their roles in disease.

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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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