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Mismatch repair hMSH2 hMLH1 hMSH6 and hPMS2 mRNA expression profiles in precancerous and cancerous urothelium

机译：癌前和癌前尿路上皮中的错配修复hMSH2hMLH1hMSH6和hPMS2 mRNA表达谱

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摘要

Changes in the expression of the mismatch repair (MMR) genes hMSH2, hMLH1, hMSH6 and hPMS2 reflect dysfunction of the DNA repair system that may allow the malignant transformation of tissue cells. The aim of the present study was to address the mRNA expression profiles of the mismatch DNA repair system in cancerous and precancerous urothelium. This is the first study to quantify MMR mRNA expression by applying quantitative real-time PCR (qPCR) and translate the results to mRNA phenotypic profiles (r, reduced; R, regular or elevated) in bladder tumors [24 urothelial cell carcinomas (UCCs) and 1 papillary urothelial neoplasm of low malignant potential (PUNLMP)] paired with their adjacent normal tissues (ANTs). Genetic instability analysis was applied at polymorphic sites distal or close to the hMSH2 and hMLH1 locus. Presenting our data, reduced hMSH2, hMSH6 and hPMS2 mRNA expression profiles were observed in cancerous and precancerous urothelia. Significantly, the ANTs of UCCs revealed the highest percentages of reduced hMSH2 (r2), hMSH6 (r6) and hPMS2 (p2) mRNA phenotypes relative to their tumors (P<0.03). In particular, combined r2r6 (P<0.02) presented a greater difference between ANTs of low-grade UCCs vs. their tumors compared with ANTs of high-grade UCCs (P= 0.000). Reduced hMLH1 (r1) phenotype was not expressed in precancerous or cancerous urothelia. The hMSH6 mRNA was the most changed in UCCs (47.8%), while hMSH2, hMLH1 and hPMS2 showed overexpression (47.8, 35 and 30%, respectively) that was associated with gender and histological tumor grading or staging. Genetic instability was rare in polymorphic regions distal to hMLH1. Our data reveal a previously unrecognized hMSH2 and hMSH6 mRNA combined phenotype (r2r6) correlated with a precancerous urothelium and show that hMLH1 is transcriptionally activated in precancerous or cancerous urothelium. In the present study, it is demonstrated that reduction of hMSH6 mRNA is a frequent event in bladder tumorigenesis and reflects a common mechanism of suppression with hMSH2, while alterations of hMSH2 or hMLH1 mRNA expression in UCCs does not correlate with the allelic imbalance of polymorphic regions harboring the genes.

机译：错配修复（MMR）基因hMSH2，hMLH1，hMSH6和hPMS2的表达变化反映了DNA修复系统功能异常，可能导致组织细胞发生恶性转化。本研究的目的是解决癌症和癌前尿路上皮中错配DNA修复系统的mRNA表达谱。这是第一项通过应用定量实时PCR（qPCR）量化MMR mRNA表达并将结果转化为膀胱肿瘤[24尿路上皮细胞癌（UCC）]中的mRNA表型特征（r，减少； R，正常或升高）的研究。和1例低恶性潜力的乳头状尿路上皮肿瘤[PUNLMP]与相邻的正常组织（ANTs）配对。遗传不稳定性分析应用于hMSH2和hMLH1基因座远端或附近的多态性位点。提供我们的数据，在癌性和癌前性尿路上皮中观察到hMSH2，hMSH6和hPMS2 mRNA表达降低。值得注意的是，相对于其肿瘤，UCC的ANTs显示出降低的hMSH2（r2），hMSH6（r6）和hPMS2（p2）mRNA表型的百分比最高（P <0.03）。特别地，与高级UCC的ANTs相比，组合r2r6（P <0.02）在低级UCC的ANTs与其肿瘤之间呈现出更大的差异（P = 0.000）。减少的hMLH1（r1）表型未在癌前或癌性尿路上皮中表达。 hMSH6 mRNA在UCC中变化最大（47.8％），而hMSH2，hMLH1和 hPMS2 显示过表达（分别为47.8、35和30％），这与性别和组织学肿瘤分级或分期有关。在 hMLH1 远端的多态性区域，遗传不稳定很少见。我们的数据显示与癌前尿道上皮相关的先前无法识别的 hMSH2 和 hMSH6 mRNA组合表型（r2r6），并显示 hMLH1 在癌前期中被转录激活或癌性尿路上皮。在本研究中，证明了 hMSH6 mRNA的降低是膀胱肿瘤发生中的常见事件，反映了 hMSH2 抑制的常见机制，而的改变UCCs中的hMSH2 或 hMLH1 mRNA表达与具有该基因的多态性区域的等位基因失衡无关。 展开▼

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期刊名称 Oncology Letters

作者
DIMITRA P. VAGELI; STAVROS GIANNOPOULOS; SOTIRIOS G. DOUKAS; CHRISTOS KALAITZIS; STILIANOS GIANNAKOPOULOS; ALEXANDRA GIATROMANOLAKI; GEORGE K. KOUKOULIS; STAVROS TOULOUPIDIS;
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作者单位

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年(卷),期 -1(5),1

年度 -1

页码 283–294

总页数 12

原文格式 PDF

正文语种

中图分类肿瘤学;

关键词
bladder tumors urothelial cell carcinoma papillary urothelial neoplasm of low malignant potential normal urothelium hMSH2 hMLH1 hPMS2 hMSH6 quantitative real-time PCR;

机译：膀胱肿瘤;尿路上皮细胞癌;低恶性乳头状尿路上皮肿瘤;正常尿路上皮;hMSH2;hMLH1;hPMS2;hMSH6;实时荧光定量PCR;

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专利

1. Mismatch repair hMSH2, hMLH1, hMSH6 and hPMS2 mRNA expression profiles in precancerous and cancerous urothelium [J] . Vageli Dimitra P., Giannopoulos Stavros, Doukas Sotirios G., Oncology letters . 2013,第1期

机译：癌前和癌前尿路上皮中的错配修复hMSH2，hMLH1，hMSH6和hPMS2 mRNA表达谱

2. Mismatch repair genes (hMLH1, hPMS1, hPMS2, GTBP/hMSH6, hMSH2) in the pathogenesis of hepatocellular carcinoma [J] . Abdel-Rahman N. Zekri, Gelane M. Sabry, Abeer A. Bahnassy, World Journal of Gastroenterology . 2005,第20期

机译：肝细胞癌发病机理中的错配修复基因（hMLH1，hPMS1，hPMS2，GTBP / hMSH6，hMSH2）

3. Phenotypic mismatch repair hMSH2 and hMLH1 gene expression profiles in primary non-small cell lung carcinomas. [J] . Vageli D, Daniil Z, Dahabreh J, Lung cancer: Journal of the International Association for the Study of Lung Cancer . 2009,第3期

机译：表型错配修复原发性非小细胞肺癌中的hMSH2和hMLH1基因表达谱。

4. A-scan spectral intensity profile in OCT as a potential imaging biomarker of oral precancerous and cancerous tissues [C] . Prashanth Panta, Pawan Kumar, Sachin Sarode, Conference on Lasers in Dentistry;Society of Photo-Optical Instrumentation Engineers . 2020

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5. Insights Into the Mechanism of DNA Mismatch Repair Through a Biochemical Study of Cancer-Associated hMSH2-hMSH6 Mutations. [D] . Cyr, Jennifer Lynn. 2012

机译：通过与癌症相关的hMSH2-hMSH6突变的生化研究深入了解DNA错配修复的机制。

6. Mismatch repair genes (hMLH1 hPMS1 hPMS2 GTBP/hMSH6 hMSH2) in the pathogenesis of hepatocellular carcinoma [O] . Abdel-Rahman N. Zekri, Gelane M. Sabry, Abeer A. Bahnassy, 2005

机译：肝细胞癌发病机理中的错配修复基因（hMLH1hPMS1hPMS2GTBP / hMSH6hMSH2）

7. Mismatch repair hMSH2, hMLH1, hMSH6 and hPMS2 mRNA expression profiles in precancerous and cancerous urothelium [O] . Vageli, D. P., Giannopoulos, S., Doukas, S. G., 2013

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7. 印迹基因在人类种植前胚胎及卵巢上皮癌中的研究 [A] . 沈文洁 . 2006

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2. 抗HER2抗体药物偶联物在治疗尿路上皮癌中的用途 [P] . 中国专利： CN111655295A . 2020-09-11

3. Chemical compound, pharmaceutical composition, methods for synthesizing a chemical compound, for treating ischemia-reperfusion damage, liver disease, arrhythmia and cancerous and precancerous cell (s), to increase expression of connexin 43 is a disease with a chemical composition comprising a carotenoid derivative and for reducing a c-reactive protein. [P] . 外国专利： BR0313155A . 2005-07-12

机译：化合物，药物组合物，用于治疗缺血-再灌注损伤，肝病，心律不齐以及癌细胞和癌前细胞的合成化合物的方法，以增加连接蛋白的表达43是一种具有包含类胡萝卜素衍生物的化学组成的疾病并用于减少c反应蛋白。

4. Blood diagnostic procedure comprises removing blood sample form a dialysis patient before and/or after dialysis, extracting mRNAs from blood sample and carrying out a procedure for preparation of gene expression profile for the mRNAs [P] . 外国专利： DE102007034497A1 . 2008-01-31

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5. Methods for generating an mRNA expression profile from an ecellular mRNA containing blood sample and using the same to identify functional state markers [P] . 外国专利： US2003036077A1 . 2003-02-20

机译：从含有血细胞的mRNA中产生血液mRNA表达谱并用其鉴定功能状态标志物的方法

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Mismatch repair hMSH2 hMLH1 hMSH6 and hPMS2 mRNA expression profiles in precancerous and cancerous urothelium

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