Effect of DNMT3A polymorphisms on CpG island hypermethylation in gastric mucosa.

4区医学 Q4 Medicine BMC Medical Genetics Pub Date : 2020-10-16 DOI:10.1186/s12881-020-01142-7

Hikaru Takano, Tomoyuki Shibata, Masakatsu Nakamura, Naoko Sakurai, Tasuku Hayashi, Masafumi Ota, Tomoe Nomura-Horita, Ranji Hayashi, Takeo Shimasaki, Toshimi Otsuka, Tomomitsu Tahara, Tomiyasu Arisawa

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引用次数: 5

Abstract

Background: CpG methylation of tumor suppressor genes occurs in the early stage of carcinogenesis. Detecting risk factors for aberrant CpG methylation is clinically important for predicting cancer development. DNA methyltransferase (DNMT) 3a is considered to play critical roles in the DNA methylation process during pathogenesis. In this study, we evaluated the association between DNMT3A polymorphisms (rs6733868 and rs13428812) and CpG methylation status in non-cancerous gastric mucosa.

Methods: We determined the DNMT3A genotype and CpG methylation status of 4 genes (p14^ARF, p16^INK4a, DAPK, and CDH1) in 510 subjects without gastric cancer. Helicobacter pylori (HP) infection status was determined by the rapid urease test, urea breath test, speculum examination, or serum antibody test. We determined the DNMT3A genotype using polymerase chain reaction single-strand conformation polymorphism (PCR-SSCP). CpG methylation status was determined by methylation-specific polymerase chain reaction (MSP). When the methylated band was stronger than 10 ng/μL according to the DNA marker, we judged CpG island hypermethylation (CIHM) to be present. Associations between genotypes and susceptibilities were assessed by logistic regression analysis.

Results: The minor allele frequencies of both polymorphisms (rs6733868 and rs13428812) were lower in the CpG methylated groups of each of the 4 genes (p14^ARF, p16^INK4a, DAPK, and CDH1). Using a dominant genetic model, rs6733868 was significantly associated with the hypermethylation of each gene, whereas rs13428812 was associated with the methylation of 3 genes (all except p14^ARF). When low-CIHM was defined as 1 or 2 CpG islands methylated and high-CIHM was defined as 3 or more CpG islands methylated, carrying the minor allele of rs6733868 was associated with both decreased low- and high-CIHM, and that of rs13428812 also was associated with a decrease. Comparing low-CIHM with high-CIHM, carrying the minor alleles of rs6733868 or rs13428812 was related to decreased susceptibility to high-CIHM. In HP-infected subjects, carrying the minor alleles of rs6733868 or rs13428812 had a significantly greater association with decreased susceptibility to high-CIHM.

Conclusions: Our study indicates that polymorphisms of DNMT3A are associated with the accumulation of gene methylation in gastric mucosa. Carrying the minor alleles of rs6733868 or rs13428812 inhibits aberrant gene methylations, which are typically enhanced by HP infection.

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DNMT3A多态性对胃黏膜CpG岛高甲基化的影响。

背景:肿瘤抑制基因的CpG甲基化发生在癌变的早期。检测异常CpG甲基化的危险因素对预测癌症发展具有重要的临床意义。DNA甲基转移酶(DNMT) 3a被认为在发病过程中DNA甲基化过程中起关键作用。在这项研究中，我们评估了DNMT3A多态性(rs6733868和rs13428812)与非癌性胃粘膜CpG甲基化状态之间的关系。方法:测定510例非胃癌患者DNMT3A基因型和4个基因(p14ARF、p16INK4a、DAPK、CDH1)的CpG甲基化状态。通过快速脲酶试验、尿素呼气试验、窥镜检查或血清抗体试验确定幽门螺杆菌(HP)感染状态。我们使用聚合酶链反应单链构象多态性(PCR-SSCP)确定DNMT3A基因型。通过甲基化特异性聚合酶链反应(MSP)测定CpG甲基化状态。根据DNA标记，当甲基化条带大于10 ng/μL时，我们判断存在CpG岛超甲基化(CIHM)。通过logistic回归分析评估基因型与易感性之间的关系。结果:在4个基因(p14ARF、p16INK4a、DAPK和CDH1)的CpG甲基化组中，两种多态性(rs6733868和rs13428812)的次要等位基因频率都较低。使用显性遗传模型，rs6733868与每个基因的超甲基化显著相关，而rs13428812与3个基因的甲基化相关(除p14ARF外)。当低cihm被定义为1个或2个CpG岛甲基化，高cihm被定义为3个或更多CpG岛甲基化时，携带rs6733868的小等位基因与低和高cihm均降低相关，携带rs13428812的小等位基因也与降低相关。与高cihm相比，携带rs6733868或rs13428812等位基因与高cihm敏感性降低有关。在hp感染的受试者中，携带rs6733868或rs13428812的次要等位基因与高cihm易感性降低的相关性显著更大。结论:我们的研究表明，DNMT3A基因多态性与胃黏膜基因甲基化积累有关。携带rs6733868或rs13428812的小等位基因可以抑制异常基因的甲基化，而这种异常基因的甲基化通常在HP感染时增强。

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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BMC Medical Genetics 医学-遗传学

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审稿时长

12 months

期刊介绍： BMC Medical Genetics is an open access journal publishing original peer-reviewed research articles in the effects of genetic variation in individuals, families and among populations in relation to human health and disease. Note: BMC Medical Genetics is now closed. This journal has merged with BMC Medical Genomics, a broad-scope, open access community journal for all medical genetics and genomics research.