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人类子宫内膜癌及其癌前阶段中编码内源性逆转录病毒(ERV)包膜基因的重新激活:新分子靶点的出现

Reactivation of codogenic endogenous retroviral (ERV) envelope genes in human endometrial carcinoma and prestages: Emergence of new molecular targets.

作者信息

Strissel Pamela L, Ruebner Matthias, Thiel Falk, Wachter David, Ekici Arif B, Wolf Friedericke, Thieme Franziska, Ruprecht Klemens, Beckmann Matthias W, Strick Reiner

机构信息

University-Clinic Erlangen, Department of Gynecology and Obstetrics, Laboratory for Molecular Medicine, Erlangen, Germany.

出版信息

Oncotarget. 2012 Oct;3(10):1204-19. doi: 10.18632/oncotarget.679.

Abstract

Endometrial carcinoma (EnCa) is the most common invasive gynaecologic carcinoma. Over 85% of EnCa are classified as endometrioid, expressing steroid hormone receptors and mostly involving pathological prestages. Human endogenous retroviruses (ERV) are chromosomally integrated genes, account for about 8% of the human genome and are implicated in the etiology of carcinomas. The majority of ERV envelope (env) coding genes are either not present or not consistently represented between common gene expression microarrays. The aim of this study was to analyse the absolute gene expression of all known 21 ERV env genes including 19 codogenic and two env genes with premature stop codons in EnCa, endometrium as well as in hyperplasia and polyps. For EnCa seven env genes had high expression with >200 mol/ng cDNA (e.g. envH1-3, Syncytin-1, envT), two middle >50 mol/ng cDNA (envFc2, erv-3) and 12 low less than 50 mol/ng cDNA (e.g. Syncytin-2, envV2). Regarding tumor parameters, Syncytin-1 and Syncytin-2 were significantly over-expressed in advanced stage pT2 compared to pT1b. In less differentiated EnCa Syncytin-1, erv-3, envT and envFc2 were significantly over-expressed. Syncytin-1, Syncytin-2 and erv-3 were specific to glandular epithelial cells of polyps, hyperplasia and EnCa using immunohistochemistry. An analysis of 10 patient-matched EnCa with endometrium revealed that the ERV-W 5' long terminal repeat regulating Syncytin-1 was hypomethylated, including the ERE and CRE overlapping MeCP2 sites. Functional analyses showed that 10 env genes were regulated by methylation in EnCa using the RL95-2 cell line. In conclusion, over-expressed env genes could serve as indicators for pathological pre-stages and EnCa.

摘要

子宫内膜癌(EnCa)是最常见的侵袭性妇科癌症。超过85%的EnCa被归类为子宫内膜样癌,表达类固醇激素受体,且大多涉及病理前期。人类内源性逆转录病毒(ERV)是染色体整合基因,约占人类基因组的8%,与癌症的病因有关。大多数ERV包膜(env)编码基因在常见的基因表达微阵列中要么不存在,要么表达不一致。本研究的目的是分析21种已知ERV env基因的绝对基因表达,包括EnCa、子宫内膜以及增生和息肉中的19个编码基因和两个带有提前终止密码子的env基因。对于EnCa,7个env基因高表达,>200 mol/ng cDNA(如envH1 - 3、Syncytin - 1、envT),2个中等表达>50 mol/ng cDNA(envFc2、erv - 3),12个低表达低于50 mol/ng cDNA(如Syncytin - 2、envV2)。关于肿瘤参数,与pT1b相比,Syncytin - 1和Syncytin - 2在晚期pT2中显著过表达。在分化程度较低的EnCa中,Syncytin - 1、erv - 3、envT和envFc2显著过表达。使用免疫组织化学方法,Syncytin - 1、Syncytin - 2和erv - 3对息肉、增生和EnCa的腺上皮细胞具有特异性。对10例患者匹配的EnCa与子宫内膜的分析表明,调控Syncytin - 1的ERV - W 5'长末端重复序列发生低甲基化,包括与甲基化CpG结合蛋白2(MeCP2)位点重叠的雌激素反应元件(ERE)和CRE。功能分析表明,使用RL95 - 2细胞系,10个env基因在EnCa中受甲基化调控。总之,过表达的env基因可作为病理前期和EnCa的指标。

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