Dual epigenetic changes in diabetes mellitus-associated pancreatic ductal adenocarcinoma correlate with downregulation of E-cadherin and worsened prognosis

IF 3.4 2区医学 Q1 PATHOLOGY

Journal of Pathology Clinical Research Pub Date : 2023-05-28 DOI:10.1002/cjp2.326

Yutaro Hara, Hiroki Mizukami, Keisuke Yamazaki, Takahiro Yamada, Akiko Igawa, Yuki Takeuchi, Takanori Sasaki, Hanae Kushibiki, Kotaro Murakami, Kazuhiro Kudoh, Keinosuke Ishido, Kenichi Hakamada

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引用次数: 1

Abstract

Diabetes mellitus (DM) is a risk factor for pancreatic ductal adenocarcinoma (PDAC) that promotes the promoter methylation of CDH1. It is still unclear whether DM can exert other epigenetic effects, such as altering microRNA (miR) expression, in PDAC. The expression of miR-100-5p is known to be changed in DM patients and can suppress the expression of E-cadherin. In this study, the correlation between DM status and dual epigenetic changes was evaluated in PDAC specimens from patients who underwent radical surgical resection. A total of 132 consecutive patients with PDAC were clinicopathologically evaluated. E-cadherin and nuclear β-catenin expression was measured using immunohistochemistry. DNA and miRs were extracted from the main tumor site on formalin-fixed paraffin-embedded tissue sections. TaqMan miR assays were applied to assess miR-100-5p expression. Bisulfite modification was conducted on the extracted DNA, which was then subjected to methylation-specific polymerase chain reaction. Immunohistochemistry revealed that decreased E-cadherin expression and increased nuclear β-catenin expression were significantly associated with DM and poor tumor cell differentiation. The presence of long-duration DM (≥3 years) was a significant factor contributing to CDH1 promoter methylation (p < 0.01), while miR-100-5p expression was proportionally correlated with the preoperative HbA1c level (R = 0.34, p < 0.01), but not the duration of DM. The subjects with high miR-100-5p expression and CDH1 promoter methylation showed the highest level of vessel invasion and prevalence of tumor size ≥30 mm. PDAC subjects with dual epigenetic changes showed poorer overall survival (OS) than those with a single epigenetic change. miR-100-5p expression ≥4.13 and CDH1 promoter methylation independently predicted poor OS and disease-free survival (DFS) in the multivariate analysis. OS and DFS worsened in DM subjects with both HbA1c ≥ 6.5% and DM duration ≥3 years. Thus, DM is associated with two modes of epigenetic change by independent mechanisms and worsens prognosis.

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糖尿病相关胰腺导管腺癌的双表观遗传改变与e -钙粘蛋白下调和预后恶化相关

糖尿病(DM)是胰腺导管腺癌(PDAC)的危险因素，可促进CDH1启动子甲基化。目前尚不清楚DM是否可以在PDAC中发挥其他表观遗传作用，例如改变microRNA (miR)的表达。已知miR-100-5p在DM患者中表达改变，可抑制E-cadherin的表达。在本研究中，对接受根治性手术切除的患者的PDAC标本中DM状态与双表观遗传改变的相关性进行了评估。对132例PDAC患者进行临床病理评估。免疫组化法检测E-cadherin和细胞核β-catenin的表达。在福尔马林固定石蜡包埋组织切片上提取肿瘤主要部位的DNA和mir。应用TaqMan miR检测检测miR-100-5p的表达。对提取的DNA进行亚硫酸氢盐修饰，然后进行甲基化特异性聚合酶链反应。免疫组化显示，E-cadherin表达降低和细胞核β-catenin表达升高与DM和肿瘤细胞分化不良有显著相关性。长期DM(≥3年)的存在是CDH1启动子甲基化的重要因素(p <miR-100-5p表达与术前HbA1c水平成比例相关(R = 0.34, p < 0.01)，但与DM持续时间无关。miR-100-5p高表达和CDH1启动子甲基化的受试者血管侵犯水平最高，肿瘤大小≥30 mm的患病率最高。具有双重表观遗传改变的PDAC受试者的总生存率(OS)低于具有单一表观遗传改变的PDAC受试者。在多变量分析中，miR-100-5p表达≥4.13和CDH1启动子甲基化独立预测不良OS和无病生存期(DFS)。当糖化血红蛋白≥6.5%、糖尿病病程≥3年时，糖尿病患者的OS和DFS均恶化。因此，糖尿病通过独立的机制与两种模式的表观遗传改变相关，并使预后恶化。

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来源期刊

Journal of Pathology Clinical Research Medicine-Pathology and Forensic Medicine

CiteScore

7.40

自引率

2.40%

发文量

审稿时长

20 weeks

期刊介绍： The Journal of Pathology: Clinical Research and The Journal of Pathology serve as translational bridges between basic biomedical science and clinical medicine with particular emphasis on, but not restricted to, tissue based studies. The focus of The Journal of Pathology: Clinical Research is the publication of studies that illuminate the clinical relevance of research in the broad area of the study of disease. Appropriately powered and validated studies with novel diagnostic, prognostic and predictive significance, and biomarker discover and validation, will be welcomed. Studies with a predominantly mechanistic basis will be more appropriate for the companion Journal of Pathology.

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