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无蒂锯齿状腺瘤和经典腺瘤:胃肠道癌前肿瘤病变的表观遗传学观点。

Sessile serrated adenomas and classical adenomas: an epigenetic perspective on premalignant neoplastic lesions of the gastrointestinal tract.

机构信息

Department of Surgery, Johns Hopkins University, Baltimore 21287, MD, USA.

出版信息

Int J Cancer. 2011 Oct 15;129(8):1889-98. doi: 10.1002/ijc.25847. Epub 2011 Mar 11.

Abstract

The diagnosis of sessile serrated adenomas (SSAs) is challenging, and there is a great deal of interobserver variability amongst pathologists in differentiating SSAs from hyperplastic polyps (HPPs). The aim of this study was (i) to assess the utility of epigenetic changes such as DNA methylation in differentiating SSAs from HPPs and (ii) to identify common methylation based molecular markers potentially useful for early detection of premalignant neoplastic lesions of gastrointestinal tract. A total of 97 primary patient adenoma samples were obtained from The Johns Hopkins Hospital pathology archive with IRB approval and HIPAA compliance. We analyzed the promoter associated CpG island methylation status of 17 genes using nested multiplex methylation specific PCR (MSP). Methylation of CDX2, hMLH1 and TLR2 was detected in SSAs and SSAs with dysplasia but not in HPPs. A subset of genes including EVL, GATAs (4 and 5), HIN-1, SFRPs (1, 2, 4 and 5), SOX17 and SYNE1 were methylated frequently in all premalignant gastrointestinal adenomas including tubular adenomas, villous adenomas, SSAs and SSAs with dysplasia but infrequently in non-premalignant polyps such as HPPs. Methylation of CDX2, hMLH1 and TLR2 may be of diagnostic utility in differentiating, histologically challenging cases of SSAs from HPPs. Genes such as EVL, GATAs, HIN-1, SFRPs, SOX17 and SYNE1, which are frequently methylated in all types of tested premalignant adenomas, may be useful as biomarkers in stool-based strategies for early detection of these adenomas and CRCs in future.

摘要

锯齿状腺瘤(SSA)的诊断具有挑战性,病理学家在区分 SSA 和增生性息肉(HPP)方面存在很大的观察者间变异性。本研究的目的是:(i)评估表观遗传变化(如 DNA 甲基化)在区分 SSA 和 HPP 中的作用;(ii)确定常见的基于甲基化的分子标志物,这些标志物可能有助于早期检测胃肠道的癌前肿瘤病变。本研究共从约翰霍普金斯医院病理档案中获得了 97 例原发性患者腺瘤样本,这些样本均获得了机构审查委员会的批准和 HIPAA 合规性。我们使用嵌套多重甲基化特异性 PCR(MSP)分析了 17 个基因的启动子相关 CpG 岛甲基化状态。在 SSA 和伴异型增生的 SSA 中检测到 CDX2、hMLH1 和 TLR2 的甲基化,但在 HPP 中未检测到。包括 EVL、GATAs(4 和 5)、HIN-1、SFRPs(1、2、4 和 5)、SOX17 和 SYNE1 在内的一组基因在所有癌前胃肠道腺瘤(包括管状腺瘤、绒毛状腺瘤、SSA 和伴异型增生的 SSA)中经常发生甲基化,但在非癌前息肉(如 HPP)中很少发生甲基化。CDX2、hMLH1 和 TLR2 的甲基化可能有助于区分组织学上具有挑战性的 SSA 和 HPP 病例。在所有类型的测试癌前腺瘤中经常发生甲基化的基因,如 EVL、GATAs、HIN-1、SFRPs、SOX17 和 SYNE1,可能作为粪便为基础的策略在未来用于早期检测这些腺瘤和 CRC 的生物标志物。

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