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Applicability of HIN-1, MGMT and RASSF1A promoter methylation as biomarkers for detecting field cancerization in breast cancer

机译:HIN-1,MGMT和RASSF1A启动子甲基化作为检测乳腺癌现场癌变的生物标记物的适用性

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IntroductionIt has been shown in some articles that genetic and epigenetic abnormalities cannot only be found in tumor tissues but also in adjacent regions that appear histologically normal. This phenomenon is metaphorically called field cancerization or field defect. Field cancerization is regarded as clinically significant because it is assumed to be an important factor in local recurrence of cancer. As the field showing these molecular abnormalities may not be removed completely by surgery, these changes might lead to neoplasms and subsequent transformation to a tumor. We aimed to investigate the applicability of the methylation status of six tumor suppressor genes as biomarkers for detecting field cancerization in breast cancer.MethodsThe promoter methylation status of CCND2, DAPK1, GSTP1, HIN-1, MGMT and RASSF1A was determined by methylation-sensitive high-resolution melting (MS-HRM) analysis. MS-HRM methods for CCND2, MGMT and RASSF1A were developed in-house, primer sequences for DAPK1, GSTP1 and HIN-1 have already been published. Biopsy samples were taken from tumor, tumor-adjacent and tumor-distant tissue from 17 breast cancer patients. Normal breast tissues of four healthy women served as controls.ResultsAll MS-HRM methods proved to be very sensitive. LODs were in the range from 0.1 to 1.5?%, LOQs ranged from 0.3 to 5.3?%. A total of 94?%, 82?% and 65?% of the tumors showed methylation of RASSF1A, HIN-1 and MGMT promoters, respectively. The methylation status of these promoters was significantly lower in tumor-distant tissues than in tumor tissues. Tumor-adjacent tissues showed higher methylation status of RASSF1A, HIN-1 and MGMT promoters than tumor-distant tissues, indicating field cancerization. The methylation status of the HIN-1 promoter in tumor-adjacent tissues was found to correlate strongly with that in the corresponding tumors (r?=?0.785, p?
机译:引言在一些文章中已经表明,遗传和表观遗传异常不仅可以在肿瘤组织中发现,而且可以在组织学上正常的邻近区域发现。将该现象比喻为田野癌化或田野缺陷。田间癌化被认为是临床上重要的,因为它被认为是局部癌症复发的重要因素。由于显示这些分子异常的区域可能无法通过手术完全清除,因此这些变化可能会导致肿瘤并随后转化为肿瘤。我们旨在研究六个抑癌基因的甲基化状态作为检测乳腺癌现场癌变的生物标志物的适用性。方法通过甲基化敏感性高检测CCND2,DAPK1,GSTP1,HIN-1,MGMT和RASSF1A的启动子甲基化状态分辨率熔解(MS-HRM)分析。内部开发了CCND2,MGMT和RASSF1A的MS-HRM方法,DAPK1,GSTP1和HIN-1的引物序列已经发布。活检样本取自17例乳腺癌患者的肿瘤,邻近肿瘤和远离肿瘤的组织。结果以四名健康女性的正常乳腺组织作为对照。结果所有MS-HRM方法均被证明非常敏感。 LOD的范围为0.1至1.5%,LOQ的范围为0.3至5.3%。分别有94%,82%和65%的肿瘤分别显示RASSF1A,HIN-1和MGMT启动子甲基化。这些启动子的甲基化状态在远处肿瘤组织中明显低于在肿瘤组织中。邻近肿瘤的组织显示RASSF1A,HIN-1和MGMT启动子的甲基化状态要比远离肿瘤的组织高,表明发生了癌变。发现邻近肿瘤组织中HIN-1启动子的甲基化状态与相应肿瘤中的甲基化状态高度相关(r?=?0.785,p?<?0.001),但与相应肿瘤远处组织中的甲基化状态却没有相关性。 (r = 0.312,p = 0.239)。结论在研究的基因启动子中,HIN-1启动子的甲基化状态可以被认为是检测田间癌变的最佳生物标记。需要进行进一步的研究,以测试其是否可用于定义手术切缘,以防止将来再次发生乳腺癌。

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