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首页> 外文期刊>The Journal of Nutrition: Official Organ of the American Institute of Nutrition >Arachidonate 5-Lipoxygenase Gene Variants Affect Response to Fish Oil Supplementation by Healthy African Americans
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Arachidonate 5-Lipoxygenase Gene Variants Affect Response to Fish Oil Supplementation by Healthy African Americans

机译:花生四烯酸5-脂氧合酶基因变异影响健康非洲裔美国人对鱼油补充的反应

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摘要

Arachidonate 5-lipoxygenase (ALOX5) gene variants that are common in people of African ancestry are associated with a differential cardiovascular disease (CVD) risk that may be ameliorated by intake of (n-3) PUFA, such as EPA or DHA. We conducted a double-masked, placebo (PL)-controlled trial of fish oil (FO) supplements to determine if changes in erythrocyte (n-3) PUFA composition, heart rate, blood pressure, and plasma lipid and lipoprotein concentrations are modified by genotype. Participants received 5 g/d FO (2 g EPA, 1 g DHA) or 5 g/d corn/soy oil (PL). A total of 116 healthy adults of African ancestry with selected genotypes (genotypes = “dd,” “d5,” and “55” with “d” representing the deletion of 1 or 2 Sp1 binding sites in the ALOX5 promoter and “5” indicating the common allele with 5 sites) were enrolled and 98 completed the study. FO caused significant increases (relative to PL) in erythrocyte EPA, DHA, and total (n-3) PUFA and a decrease in the (n-6) PUFA:(n-3) PUFA ratio in the low-CVD risk “d5” and “55” genotypes but not in the high-risk “dd” genotype. Similarly, HDL particle concentration decreased with FO relative to PL in the “d5” and “55” but not “dd” genotypes. The plasma TG concentration decreased significantly with FO relative to PL in the “d5” but not “dd” and “55” genotypes. No changes were seen in LDL particle or cholesterol concentrations, heart rate, or blood pressure. These findings indicate that the efficacy of FO supplements vary by ALOX5 genotype.
机译:在非洲血统的人中常见的花生四烯酸5-脂氧合酶(ALOX5)基因变异与心血管疾病(CVD)风险有关,可通过摄入(n-3)PUFA(例如EPA或DHA)来缓解这种疾病。我们进行了鱼油(FO)补充剂的双掩盖安慰剂(PL)对照试验,以确定是否可以通过以下方法改变红细胞(n-3)PUFA组成,心率,血压以及血浆脂质和脂蛋白浓度的变化基因型。参与者接受5 g / d FO(2 g EPA,1 g DHA)或5 g / d玉米/豆油(PL)。共有116名非洲血统的健康成人,具有选定的基因型(基因型=“ dd”,“ d5”和“ 55”,“ d”表示ALOX5启动子中1个或2个Sp1结合位点的缺失,“ 5”表示共有5个位点的共同等位基因被纳入,并完成了98个研究。在低CVD风险中,FO引起红细胞EPA,DHA和总(n-3)PUFA的显着增加(相对于PL),并且(n-6)PUFA:(n-3)PUFA比率降低。 ”和“ 55”基因型,但不是高风险“ dd”基因型。类似地,在“ d5”和“ 55”基因型中,HDL颗粒浓度随FO相对于PL降低,但不降低。相对于PL,“ d5”和“ 55”基因型中血浆TG浓度随FO显着降低。 LDL颗粒或胆固醇浓度,心率或血压未见变化。这些发现表明,FO补充剂的功效因ALOX5基因型而异。

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