APOE ε4 Allele and Methylation Patterns Linked to Cardiovascular Outcomes in Women With Breast Cancer.

IF 2.1
Emily K Mewborn, Myeong-Ga Cho, Kirk I Erickson, Catherine M Bender, Yvette Conley
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Abstract

DNA methylation affects gene expression. While the Apolipoprotein E (APOE) genotype impacts cardiovascular risk, APOE methylation impact remains unknown, particularly in women with breast cancer (BC). This study explored associations of APOE methylation with hypertension history and cardiovascular fitness (CVF) and whether APOE genotype and methylation moderate exercise effects over 6 months. This study leveraged data from a 6-month exercise randomized clinical trial in postmenopausal women with BC. Using peripheral blood, methylation M-values (Illumina Infinium Methylation EPIC Beadchip) and 13 CpG sites within and 2kb 5' and 3' to APOE were abstracted post data quality checks. Outcome variables: self-reported hypertension and CVF (peak oxygen consumed per kilogram per minute [VO2max/kg/min] and peak metabolic equivalents [METs] through graded exercise testing). Participants completed 150 min/week of aerobic exercise or usual care for 6 months. Logistic and linear regression examined associations between CpG M-values and hypertension, VO2max/kg/min and METs. Baseline M-value and APOE genotype were interaction terms for longitudinal analyses. This study included 102 women (Mean = 62 yrs). APOEε4 carriers had increased methylation of cg06750524 (p = 0.04) and cg19514613 (p = 0.03), but lower methylation of cg21879725 (p = 0.04). Increased cg06750524 methylation was associated with higher hypertension odds (p = 0.022, OR = 2.813) and lower VO2max/kg/min and METs (p = 0.005). Increased cg05501958 methylation (M = 4.539, SD = 0.17) was associated with lower hypertension odds (p = 0.02, OR = 0.035) and higher VO2max/kg/min and METs (p = 0.022). Neither APOE ε4 nor baseline methylation moderated exercise effects. APOE methylation, differentially by ε4 carriage, may impact cardiovascular outcomes and serve as a biomarker of risk in women with BC.

APOE ε4等位基因和甲基化模式与乳腺癌女性心血管结局相关
DNA甲基化影响基因表达。虽然载脂蛋白E (APOE)基因型影响心血管风险,但APOE甲基化的影响尚不清楚,特别是在乳腺癌女性中。本研究探讨了APOE甲基化与高血压史和心血管健康(CVF)的关系,以及APOE基因型和甲基化是否在6个月内调节运动影响。这项研究利用了一项针对绝经后乳腺癌妇女的为期6个月的随机临床试验数据。使用外周血,在数据质量检查后提取5‘和3’到APOE的2kb内的13个CpG位点的甲基化m值(Illumina Infinium methylation EPIC Beadchip)。结果变量:自我报告的高血压和CVF(通过分级运动测试的每公斤每分钟耗氧量峰值[VO2max/kg/min]和代谢当量峰值[METs])。参与者完成了每周150分钟的有氧运动或6个月的常规护理。Logistic和线性回归检验了CpG - m值与高血压、VO2max/kg/min和METs之间的关系。基线m值和APOE基因型是纵向分析的相互作用项。本研究纳入102名女性(平均62岁)。携带APOEε4基因的cg06750524 (p = 0.04)和cg19514613 (p = 0.03)的甲基化增加,而携带APOEε4基因的cg21879725的甲基化降低(p = 0.04)。升高的cg06750524甲基化与较高的高血压几率(p = 0.022, OR = 2.813)和较低的VO2max/kg/min和METs (p = 0.005)相关。升高的cg05501958甲基化(M = 4.539, SD = 0.17)与较低的高血压几率(p = 0.02, OR = 0.035)和较高的VO2max/kg/min和METs (p = 0.022)相关。APOE ε4和基线甲基化都没有调节运动效果。APOE甲基化(ε4携带差异)可能影响心血管结局,并可作为BC女性风险的生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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