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Association of PLA2G4A with myocardial infarction is modulated by dietary PUFAs

机译:饮食PUFA调节PLA2G4A与心肌梗死的关系

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摘要

>Background: Leukotrienes are proinflammatory molecules derived from dietary PUFAs and have been associated with cardiovascular disease (CVD). We previously reported that an A→G variant (rs12746200) of the cytosolic phospholipase A2 group IVA gene (PLA2G4A), which encodes the enzyme that liberates PUFAs from cellular membranes for leukotriene synthesis, decreases the risk of CVD.>Objective: We sought to replicate these initial observations with a more clinically relevant phenotype, such as myocardial infarction (MI), and to determine whether dietary PUFAs mediate this association.>Design: In a Costa Rican case-control data set (n = 3971), rs12746200 was genotyped and was tested for an association with MI. Functional experiments were carried out to determine whether rs12746200 led to differences in mRNA expression.>Results: Risk of MI was significantly lower in AG/GG subjects than in AA homozygotes (OR: 0.86; 95% CI: 0.75, 0.99; P = 0.040). The reduced risk of MI was observed primarily in AG/GG subjects who were above the median for intake of dietary omega-6 (n−6) PUFAs (OR: 0.71; 95% CI: 0.59, 0.87; P-interaction = 0.005). A similar analysis with dietary omega-3 (n−3) PUFAs did not show a statistically significant nutrigenetic association (P-interaction = 0.23). Functional analysis in human aortic endothelial cells showed that the carriers of the G allele had significantly lower PLA2G4A gene expression (P = 0.014), consistent with the atheroprotective association of this variant.>Conclusion: These results replicate the association of rs12746200 with CVD phenotypes and provide evidence that the protective association of this functional PLA2G4A variant is mediated by dietary PUFAs.
机译:>背景:白三烯是饮食中的PUFA促炎分子,与心血管疾病(CVD)有关。我们先前曾报道,胞质磷脂酶A2组IVA基因(PLA2G4A)的A→G变体(rs12746200)编码从细胞膜中释放PUFA用于白三烯合成的酶,可降低CVD的风险。>目的:< / strong>我们试图将这些初步观察结果与临床上更相关的表型(例如心肌梗塞(MI))进行复制,并确定饮食中的PUFA是否介导这种关联。>设计:在哥斯达黎加病例中-对照数据集(n = 3971),对rs12746200进行了基因分型并测试了与MI的关联。进行功能性实验以确定rs12746200是否导致mRNA表达差异。>结果: AG / GG受试者的MI风险显着低于AA纯合子(OR:0.86; 95%CI:0.75) ,0.99; P = 0.040)。主要在AG / GG受试者中观察到MI降低,这些受试者的饮食摄入量高于饮食中的omega-6(n-6)PUFA(OR:0.71; 95%CI:0.59、0.87; P相互作用= 0.005) 。饮食中ω-3(n-3)PUFA的类似分析未显示出统计学上显着的营养遗传相关性(P相互作用= 0.23)。对人主动脉内皮细胞的功能分析表明,G等位基因携带者的PLA2G4A基因表达明显降低(P = 0.014),与该变体的动脉粥样硬化保护相关。>结论: rs12746200具有CVD表型的证据,并提供证据表明该功能性PLA2G4A变体的保护性结合是由饮食PUFA介导的。

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