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A common FADS2 promoter polymorphism increases promoter activity and facilitates binding of transcription factor ELK1

机译:常见的FADS2启动子多态性可提高启动子活性并促进转录因子ELK1的结合

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摘要

Fatty acid desaturases (FADS) play an important role in the formation of omega-6 and omega-3 highly unsaturated fatty acids (HUFAs). The composition of HUFAs in the human metabolome is important for membrane fluidity and for the modulation of essential physiological functions such as inflammation processes and brain development. Several recent studies reported significant associations of single nucleotide polymorphisms (SNPs) in the human FADS gene cluster with HUFA levels and composition. The presence of the minor allele correlated with a decrease of desaturase reaction products and an accumulation of substrates. We performed functional studies with two of the associated polymorphisms (rs3834458 and rs968567) and showed an influence of polymorphism rs968567 on FADS2 promoter activity by luciferase reporter gene assays. Electrophoretic mobility shift assays proved allele-dependent DNA-binding ability of at least two protein complexes to the region containing SNP rs968567. One of the proteins binding to this region in an allele-specific manner was shown to be the transcription factor ELK1 (a member of ETS domain transcription factor family). These results indicate that rs968567 influences FADS2 transcription and offer first insights into the modulation of complex regulation mechanisms of FADS2 gene transcription by SNPs.
机译:脂肪酸去饱和酶(FADS)在omega-6和omega-3高不饱和脂肪酸(HUFAs)的形成中起着重要作用。人类代谢组中HUFA的组成对于膜流动性和调节必要的生理功能(例如炎症过程和大脑发育)非常重要。最近的一些研究报道了人类FADS基因簇中单核苷酸多态性(SNP)与HUFA水平和组成的显着关联。次要等位基因的存在与去饱和酶反应产物的减少和底物的积累有关。我们对两个相关的多态性(rs3834458和rs968567)进行了功能研究,并通过萤光素酶报告基因检测显示了多态性rs968567对FADS2启动子活性的影响。电泳迁移率变动分析证明了至少两种蛋白质复合物对含有SNP rs968567的区域的等位基因依赖性DNA结合能力。以等位基因特异性方式与该区域结合的蛋白质之一显示为转录因子ELK1(ETS域转录因子家族的成员)。这些结果表明,rs968567影响FADS2转录,并为SNP调节FADS2基因转录的复杂调控机制提供了初步见解。

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