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Methylation at CPT1A locus is associated with lipoprotein subfraction profiles

机译:CPT1A位点的甲基化与脂蛋白亚组分谱相关

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摘要

Lipoprotein subfractions help discriminate cardiometabolic disease risk. Genetic loci validated as associating with lipoprotein measures do not account for a large proportion of the individual variation in lipoprotein measures. We hypothesized that DNA methylation levels across the genome contribute to interindividual variation in lipoprotein measures. Using data from participants of the Genetics of Lipid Lowering Drugs and Diet Network (n = 663 for discovery and n = 331 for replication stages, respectively), we conducted the first systematic screen of the genome to determine associations between methylation status at ∼470,000 cytosine-guanine dinucleotide (CpG) sites in CD4+ T cells and 14 lipoprotein subfraction measures. We modeled associations between methylation at each CpG site and each lipoprotein measure separately using linear mixed models, adjusted for age, sex, study site, cell purity, and family structure. We identified two CpGs, both in the carnitine palmitoyltransferase-1A (CPT1A) gene, which reached significant levels of association with VLDL and LDL subfraction parameters in both discovery and replication phases (P < 1.1 × 10−7 in the discovery phase, P < .004 in the replication phase, and P < 1.1 × 10−12 in the full sample). CPT1A is regulated by PPARα, a ligand for drugs used to reduce CVD. Our associations between methylation in CPT1A and lipoprotein measures highlight the epigenetic role of this gene in metabolic dysfunction.
机译:脂蛋白亚组分有助于区分心脏代谢疾病的风险。经验证与脂蛋白测量相关的遗传基因座不能解释脂蛋白测量中个体变异的很大一部分。我们假设整个基因组中的DNA甲基化水平有助于脂蛋白测量的个体差异。利用降脂药物遗传学和饮食网络参与者的数据(发现阶段分别为n = 663和复制阶段为n = 331),我们对基因组进行了首次系统筛选,以确定约470,000胞嘧啶的甲基化状态之间的关联CD4 + T细胞中的-鸟嘌呤二核苷酸(CpG)位点和14种脂蛋白亚组分测定。我们使用线性混合模型分别对每个CpG位点的甲基化与每个脂蛋白测量之间的关联进行了建模,并针对年龄,性别,研究位点,细胞纯度和家族结构进行了调整。我们在肉碱棕榈酰转移酶-1A(CPT1A)基因中鉴定了两个CpG,它们在发现和复制阶段均达到与VLDL和LDL亚组分参数的显着关联水平(P <1.1×10 −7 在发现阶段,P <.004在复制阶段,在完整样本中为P <1.1×10 -12 )。 CPT1A由PPARα调节,PPARα是用于减少CVD的药物的配体。我们在CPT1A中的甲基化与脂蛋白测量之间的关联突出了该基因在代谢功能障碍中的表观遗传学作用。

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