Influence of MIF polymorphisms on CpG island hyper-methylation of CDKN2A in the patients with ulcerative colitis.

4区医学 Q4 Medicine

BMC Medical Genetics Pub Date : 2020-10-12 DOI:10.1186/s12881-020-01140-9

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

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引用次数: 3

Abstract

Background: CDKN2A hypermethylation is among the major events associated with carcinogenesis and is also observed in non-neoplastic colonic mucosa in patients with ulcerative colitis (UC). Macrophage migration inhibitory factor (MIF) plays a crucial role in promoting gastrointestinal inflammation characteristic of UC. The aim of this study is to explore associations between CDKN2A methylation status and MIF polymorphisms (rs755622 and rs5844572).

Methods: One hundred and fifty-nine patients diagnosed with UC were enrolled in this study. The methylation status of p14^ARF and p16^INK4a was determined by MSP; MIF genotypes were identified by PCR-SSCP.

Results: We found no differences with respect to mean age, gender, clinical type (chronic continuous or relapse/remitting), or extent of disease among the patients with methylated and unmethylated p14^ARF or p16^INK4a. Carrying the rs755622 C allele indicated a significantly higher risk for p14^ARF methylation (odds ratio (OR), 2.16; 95% confidence interval (CI), 1.08-4.32; p = 0.030); similarly, carrying the rs5844572 7-repeat allele indicated a significantly higher risk for p16^INK4a methylation (OR, 2.57; 95% CI, 1.26-5.24; p = 0.0094) after an adjusted regression analysis. The carriers of the rs755662 C allele or the rs5844572 7-repeat allele were both at a significantly higher risk for methylation of both p14^ARF and p16^INK4a when compared to the cohort in which neither of the genes were methylated (OR, 2.70; 95% CI, 1.22-6.01; p = 0.015 and OR, 2.87; 95% CI, 1.25-6.62; p = 0.013, respectively). Additionally, carrying rs755622 C allele was significantly associated with CIHM in chronic continuous of clinical type and total colitis (OR, 25.9; 95% CI, 2.55-262.6; p = 0.0059 and OR, 4.38; 95% CI, 1.12-17.2; p = 0.034, respectively), and carrying 7-repeat allele of rs5844572 was significantly associated in chronic continuous type (OR, 14.5; 95%CI, 1.46-144.3; p = 0.022).

Conclusions: Taken together, our findings suggest that MIF genotypes associated with inflammation may also be involved in promoting carcinogenesis via CDKN2A hypermethylation in patients diagnosed with UC.

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MIF多态性对溃疡性结肠炎患者CDKN2A CpG岛超甲基化的影响

背景:CDKN2A高甲基化是与癌变相关的主要事件之一，也在溃疡性结肠炎(UC)患者的非肿瘤性结肠粘膜中观察到。巨噬细胞迁移抑制因子(Macrophage migration inhibitory factor, MIF)在UC的胃肠道炎症中起着重要的促进作用。本研究的目的是探索CDKN2A甲基化状态与MIF多态性(rs755622和rss5844572)之间的关系。方法:159例诊断为UC的患者被纳入本研究。MSP检测p14ARF和p16INK4a的甲基化状态;采用PCR-SSCP技术鉴定MIF基因型。结果:我们发现p14ARF或p16INK4a甲基化和非甲基化患者在平均年龄、性别、临床类型(慢性持续或复发/缓解)或疾病程度方面没有差异。携带rs755622 C等位基因表明p14ARF甲基化的风险显著增加(优势比(OR)， 2.16;95%置信区间(CI)， 1.08-4.32;p = 0.030);同样，携带rs5844572 7-repeat等位基因表明p16INK4a甲基化的风险显著增加(OR, 2.57;95% ci, 1.26-5.24;P = 0.0094)。携带rs755662 C等位基因或携带rss5844572 7-repeat等位基因的人，其p14ARF和p16INK4a基因甲基化的风险明显高于不携带这两种基因甲基化的人(or, 2.70;95% ci, 1.22-6.01;p = 0.015, OR为2.87;95% ci, 1.25-6.62;P = 0.013)。此外，携带rs755622 C等位基因与慢性连续临床型和完全性结肠炎的CIHM显著相关(OR, 25.9;95% ci, 2.55-262.6;p = 0.0059, OR = 4.38;95% ci, 1.12-17.2;p = 0.034)，慢性连续型患者携带rs5844572 7重复等位基因显著相关(OR, 14.5;95%置信区间,1.46 - -144.3;p = 0.022)。结论:综上所述，我们的研究结果表明，与炎症相关的MIF基因型也可能通过CDKN2A高甲基化参与UC患者的致癌作用。

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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来源期刊

BMC Medical Genetics 医学-遗传学

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0.00%

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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.