血小板线粒体 DNA 甲基化可预测超重和肥胖成年人的未来心血管结局。
Platelet mitochondrial DNA methylation predicts future cardiovascular outcome in adults with overweight and obesity.
机构信息
William Leech Building, Population Health Sciences Institute, Newcastle University, Newcastle upon Tyne, NE2 4HH, UK.
EPIGET Lab, Department of Clinical Sciences and Community Health, Università degli Studi di Milano, via San Barnaba 8, 20122, Milan, Italy.
出版信息
Clin Epigenetics. 2020 Feb 17;12(1):29. doi: 10.1186/s13148-020-00825-5.
BACKGROUND
The association between obesity and cardiovascular disease (CVD) is proven, but why some adults with obesity develop CVD while others remain disease-free is poorly understood. Here, we investigated whether mitochondrial DNA (mtDNA) methylation in platelets is altered prior to CVD development in a population of adults with overweight and obesity.
METHODS
We devised a nested case-control study of 200 adults with overweight or obesity who were CVD-free at baseline, of whom 84 developed CVD within 5 years, while 116 remained CVD-free. Platelet mtDNA was isolated from plasma samples at baseline, and mtDNA methylation was quantified in mitochondrially encoded cytochrome-C-oxidase I (MT-CO1; nt6797 and nt6807), II (MT-CO2; nt8113 and nt8117), and III (MT-CO3; nt9444 and nt9449); tRNA leucine 1 (MT-TL1; nt3247 and nt3254); D-loop (nt16383); tRNA phenylalanine (MT-TF; nt624); and light-strand-origin-of-replication (MT-OLR; nt5737, nt5740, and nt5743) by bisulfite-pyrosequencing. Logistic regression was used to estimate the contribution of mtDNA methylation to future CVD risk. ROC curve analysis was used to identify the optimal mtDNA methylation threshold for future CVD risk prediction. A model was generated incorporating methylation at three loci (score 0, 1, or 2 according to 0, 1, or 2-3 hypermethylated loci, respectively), adjusted for potential confounders, such as diastolic and systolic blood pressure, fasting blood glucose, and cholesterol ratio. mtDNA methylation at MT-CO1 nt6807 (OR = 1.08, 95% CI 1.02-1.16; P = 0.014), MT-CO3 nt9444 (OR = 1.22, 95% CI 1.02-1.46, P = 0.042), and MT-TL1 nt3254 (OR = 1.30, 95% CI 1.05-1.61, P = 0.008) was higher at baseline in those who developed CVD by follow-up, compared with those who remained CVD-free. Combined use of the three loci significantly enhanced risk prediction, with hazard ratios of 1.38 (95% CI 0.68-2.78) and 2.68 (95% CI 1.41-5.08) for individuals with score 1 or 2, respectively (P = 0.003). Methylation at these sites was independent of conventional CVD risk factors, including inflammation markers, fasting blood glucose concentration, and blood pressure.
CONCLUSIONS
Methylations of MT-CO1, MT-CO3, and MT-TL1 are, together, strong predictors of future CVD incidence. Since methylation of these mtDNA domains was independent of conventional CVD risk factors, these markers may represent a novel intrinsic predictor of CVD risk in adults with overweight and obesity.
背景
肥胖与心血管疾病(CVD)之间的关联已得到证实,但为什么一些肥胖的成年人会患上 CVD,而另一些成年人则不会,这一点还不太清楚。在这里,我们研究了在超重和肥胖人群中,是否存在血小板中线粒体 DNA(mtDNA)甲基化在 CVD 发生之前发生改变。
方法
我们设计了一项嵌套病例对照研究,纳入了 200 名基线时无 CVD 的超重或肥胖成年人,其中 84 人在 5 年内发生了 CVD,而 116 人仍无 CVD。在基线时从血浆样本中分离血小板 mtDNA,并通过亚硫酸氢盐-焦磷酸测序定量分析线粒体编码细胞色素 C-氧化酶 I(MT-CO1;nt6797 和 nt6807)、II(MT-CO2;nt8113 和 nt8117)、III(MT-CO3;nt9444 和 nt9449);tRNA 亮氨酸 1(MT-TL1;nt3247 和 nt3254);D 环(nt16383);tRNA 苯丙氨酸(MT-TF;nt624)和轻链复制起始区(MT-OLR;nt5737、nt5740 和 nt5743)的 mtDNA 甲基化。采用 logistic 回归估计 mtDNA 甲基化对未来 CVD 风险的贡献。采用 ROC 曲线分析确定 mtDNA 甲基化预测未来 CVD 风险的最佳阈值。生成一个模型,该模型包含三个位点的甲基化(根据 0、1 或 2 个超甲基化位点分别赋值 0、1 或 2-3),并根据潜在的混杂因素(如舒张压和收缩压、空腹血糖和胆固醇比值)进行调整。与无 CVD 患者相比,随访期间发生 CVD 的患者基线时 MT-CO1 nt6807(OR = 1.08,95%CI 1.02-1.16;P = 0.014)、MT-CO3 nt9444(OR = 1.22,95%CI 1.02-1.46,P = 0.042)和 MT-TL1 nt3254(OR = 1.30,95%CI 1.05-1.61,P = 0.008)的甲基化水平更高。三个位点的联合使用显著提高了风险预测,评分 1 或 2 的个体的危险比分别为 1.38(95%CI 0.68-2.78)和 2.68(95%CI 1.41-5.08)(P = 0.003)。这些位点的甲基化独立于传统的 CVD 危险因素,包括炎症标志物、空腹血糖浓度和血压。
结论
MT-CO1、MT-CO3 和 MT-TL1 的甲基化是未来 CVD 发病率的有力预测因子。由于这些 mtDNA 区域的甲基化独立于传统的 CVD 危险因素,因此这些标志物可能代表超重和肥胖成年人 CVD 风险的新型内在预测因子。
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