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血浆中驱动蛋白家族成员1a的启动子甲基化差异与乳腺癌及DNA修复能力相关。

Differential promoter methylation of kinesin family member 1a in plasma is associated with breast cancer and DNA repair capacity.

作者信息

Guerrero-Preston Rafael, Hadar Tal, Ostrow Kimberly Laskie, Soudry Ethan, Echenique Miguel, Ili-Gangas Carmen, Pérez Gabriela, Perez Jimena, Brebi-Mieville Priscilla, Deschamps José, Morales Luisa, Bayona Manuel, Sidransky David, Matta Jaime

机构信息

Department of Otolaryngology - Head and Neck Cancer Research Division, Johns Hopkins School of Medicine, Baltimore, MD 21231, USA.

Cancer Center, Auxilio Mutuo Hospital, San Juan, Puerto Rico.

出版信息

Oncol Rep. 2014 Aug;32(2):505-12. doi: 10.3892/or.2014.3262. Epub 2014 Jun 13.

Abstract

Methylation alterations of CpG islands, CpG island shores and first exons are key events in the formation and progression of human cancer, and an increasing number of differentially methylated regions and genes have been identified in breast cancer. Recent studies of the breast cancer methylome using deep sequencing and microarray platforms are providing a novel insight on the different roles aberrant methylation plays in molecular subtypes of breast cancer. Accumulating evidence from a subset of studies suggests that promoter methylation of tumor-suppressor genes associated with breast cancer can be quantified in circulating DNA. However, there is a paucity of studies that examine the combined presence of genetic and epigenetic alterations associated with breast cancer using blood-based assays. Dysregulation of DNA repair capacity (DRC) is a genetic risk factor for breast cancer that has been measured in lymphocytes. We isolated plasma DNA from 340 participants in a breast cancer case control project to study promoter methylation levels of five genes previously shown to be associated with breast cancer in frozen tissue and in cell line DNA: MAL, KIF1A, FKBP4, VGF and OGDHL. Methylation of at least one gene was found in 49% of the cases compared to 20% of the controls. Three of the four genes had receiver characteristic operator curve values of ≥ 0.50: MAL (0.64), KIF1A (0.51) and OGDHL (0.53). KIF1A promoter methylation was associated with breast cancer and inversely associated with DRC. This is the first evidence of a significant association between genetic and epigenetic alterations in breast cancer using blood-based tests. The potential diagnostic utility of these biomarkers and their relevance for breast cancer risk prediction should be examined in larger cohorts.

摘要

CpG岛、CpG岛岸和首个外显子的甲基化改变是人类癌症形成和进展中的关键事件,并且在乳腺癌中已鉴定出越来越多的差异甲基化区域和基因。最近使用深度测序和微阵列平台对乳腺癌甲基化组进行的研究,为异常甲基化在乳腺癌分子亚型中所起的不同作用提供了新的见解。来自一部分研究的证据不断积累,表明与乳腺癌相关的肿瘤抑制基因的启动子甲基化可以在循环DNA中进行量化。然而,使用基于血液的检测方法来检查与乳腺癌相关的基因和表观遗传改变共同存在情况的研究却很少。DNA修复能力(DRC)失调是乳腺癌的一种遗传风险因素,已在淋巴细胞中进行过测量。我们从一个乳腺癌病例对照项目的340名参与者中分离了血浆DNA,以研究先前在冷冻组织和细胞系DNA中显示与乳腺癌相关的五个基因的启动子甲基化水平:MAL、KIF1A、FKBP4、VGF和OGDHL。在49%的病例中发现至少一个基因发生甲基化,而对照组为20%。四个基因中的三个基因的受试者操作特征曲线值≥0.50:MAL(0.64)、KIF1A(0.51)和OGDHL(0.53)。KIF1A启动子甲基化与乳腺癌相关,且与DRC呈负相关。这是使用基于血液的检测方法首次证明乳腺癌中基因和表观遗传改变之间存在显著关联。这些生物标志物的潜在诊断效用及其与乳腺癌风险预测的相关性应在更大的队列中进行研究。

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