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Genome-Wide Interaction Study of Omega-3 PUFAs and Other Fatty Acids on Inflammatory Biomarkers of Cardiovascular Health in the Framingham Heart Study

机译:弗雷明汉心脏研究中Omega-3 PUFA和其他脂肪酸对心血管健康炎症生物标志物的全基因组相互作用研究

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Numerous genetic loci have been identified as being associated with circulating fatty acid (FA) levels and/or inflammatory biomarkers of cardiovascular health (e.g., C-reactive protein). Recently, using red blood cell (RBC) FA data from the Framingham Offspring Study, we conducted a genome-wide association study of over 2.5 million single nucleotide polymorphisms (SNPs) and 22 RBC FAs (and associated ratios), including the four Omega-3 FAs (ALA, DHA, DPA, and EPA). Our analyses identified numerous causal loci. In this manuscript, we investigate the extent to which polyunsaturated fatty acid (PUFA) levels moderate the relationship of genetics to cardiovascular health biomarkers using a genome-wide interaction study approach. In particular, we test for possible gene–FA interactions on 9 inflammatory biomarkers, with 2.5 million SNPs and 12 FAs, including all Omega-3 PUFAs. We identified eighteen novel loci, including loci which demonstrate strong evidence of modifying the impact of heritable genetics on biomarker levels, and subsequently cardiovascular health. The identified genes provide increased clarity on the biological functioning and role of Omega-3 PUFAs, as well as other common fatty acids, in cardiovascular health, and suggest numerous candidate loci for future replication and biological characterization.
机译:已经确定许多遗传基因座与循环脂肪酸(FA)水平和/或心血管健康的炎性生物标记物(例如,C反应蛋白)有关。最近,我们使用Framingham后代研究的红细胞(RBC)FA数据,对250万个以上的单核苷酸多态性(SNP)和22个RBC FA(及相关比率)进行了全基因组关联研究,其中包括四个Omega- 3个FA(ALA,DHA,DPA和EPA)。我们的分析确定了许多因果位点。在本手稿中,我们使用全基因组相互作用研究方法,调查多不饱和脂肪酸(PUFA)水平在多大程度上缓解了遗传学与心血管健康生物标志物之间的关系。特别是,我们测试了9种炎症生物标志物(包括250万个SNP和12个FA,包括所有Omega-3 PUFA)可能的基因-FA相互作用。我们鉴定了18个新基因座,其中包括有力证据证明可遗传基因对生物标志物水平以及随后的心血管健康的影响发生了改变。鉴定出的基因提高了Omega-3 PUFA以及其他常见脂肪酸在心血管健康中的生物学功能和作用的清晰度,并为未来的复制和生物学表征提供了许多候选基因座。

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