CBS 基因多态性及其启动子甲基化对高同型半胱氨酸血症患者叶酸治疗效果的介导作用。
CBS gene polymorphism and promoter methylation-mediating effects on the efficacy of folate therapy in patients with hyperhomocysteinemia.
机构信息
Department of Epidemiology, School of Public Health, Zhengzhou University, Zhengzhou, Henan, People's Republic of China.
Department of International Medicine, Beaumont Health System, Royal Oak, MI, USA.
出版信息
J Gene Med. 2020 Apr;22(4):e3156. doi: 10.1002/jgm.3156. Epub 2020 Jan 19.
BACKGROUND
A decrease in cystathionine beta-synthase (CBS) enzyme activity could lead to hyperhomocysteinemia (HHcy). Studies have revealed that DNA methylation has a mediating effect on the development of diseases. The present study aimed to explore CBS promoter methylation-mediating effects on the efficacy of folate treatment for HHcy.
METHODS
HHcy patients were treated with folate (5 mg/day) for 90 days and then divided into a failure group (Hcy ≥ 15 μmol/l) and a success group (Hcy < 15 μmol/l) according to post-treatment plasma Hcy levels. Genotyping of CBS gene (rs2851391 and rs706209) in patients (n = 638) was detected using a MassArray system (Sequenom, San Diego, CA, USA). The baseline DNA methylation levels of patients (n = 299) were detected using MethylTarget™ technology (Genesky Biotechnologies Inc., Shanghai, China).
RESULTS
The CBS rs2851391 TC + CC genotype was related to a 57% reduction of failure risk in HHcy treatment compared to the TT genotype (95% confidence interval [CI] = 0.19-0.97). The CBS rs706209 CT + TT genotype had a 2.97-fold increased risk of failure to treatment compared to the CC genotype (95% CI = 1.52-5.80). After adjustment for confounding factors, the odds ratio (95% CI) for the risk of failure in HHcy treatment in total and male patients was 0.55 (0.32-0.93) and 0.34 (0.16-0.69), respectively, for patients with higher methylation levels (≥ methylation median). Additionally, baseline CBS promoter methylation mediated 33.39% of the effect of rs2851391 on the efficacy of folate treatment for HHcy (ACME [average causal mediation effects]: -0.05, 95% CI = -0.11 to 0.00, p = 0.046).
CONCLUSIONS
The present study indicates that CBS gene polymorphism and promoter methylation could affect the efficacy of HHcy. There were potentially causal effects of genetic, epigenetic variations at the CBS rs2851391 locus on the efficacy of HHcy therapy with folate.
背景
胱硫醚-β-合酶(CBS)酶活性降低可导致高同型半胱氨酸血症(HHcy)。研究表明,DNA 甲基化对疾病的发展具有介导作用。本研究旨在探讨 CBS 启动子甲基化对叶酸治疗 HHcy 疗效的介导作用。
方法
HHcy 患者接受叶酸(5mg/天)治疗 90 天,然后根据治疗后血浆 Hcy 水平将患者分为治疗失败组(Hcy≥15μmol/L)和治疗成功组(Hcy<15μmol/L)。采用 MassArray 系统(美国圣地亚哥赛昆公司)检测 638 例患者 CBS 基因(rs2851391 和 rs706209)的基因型。采用 MethylTargetTM 技术(中国上海基科生物技术有限公司)检测 299 例患者的基线 DNA 甲基化水平。
结果
与 TT 基因型相比,CBS rs2851391TC+CC 基因型与 HHcy 治疗失败风险降低 57%相关(95%置信区间[CI]为 0.19-0.97)。与 CC 基因型相比,CBS rs706209CT+TT 基因型的 HHcy 治疗失败风险增加 2.97 倍(95%CI=1.52-5.80)。调整混杂因素后,HHcy 治疗总人群和男性患者的风险比(95%CI)分别为 0.55(0.32-0.93)和 0.34(0.16-0.69),高甲基化水平(≥甲基化中位数)患者的风险比为 0.55(0.32-0.93)和 0.34(0.16-0.69)。此外,CBS 启动子甲基化在 rs2851391 对叶酸治疗 HHcy 疗效的影响中介导了 33.39%(平均因果中介效应[ACME]:-0.05,95%CI=-0.11 至 0.00,p=0.046)。
结论
本研究表明 CBS 基因多态性和启动子甲基化可能影响 HHcy 的疗效。CBS rs2851391 位点的遗传和表观遗传变异对叶酸治疗 HHcy 的疗效具有潜在的因果作用。
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