Literature DB >> 21732224

Gene expression of the mismatch repair gene MSH2 in primary colorectal cancer.

Lars Henrik Jensen1, Hidekazu Kuramochi, Dorthe Gylling Crüger, Jan Lindebjerg, Steen Kolvraa, Peter Danenberg, Kathleen Danenberg, Anders Jakobsen.   

Abstract

Microsatellite instability (MSI) is caused by defective mismatch repair (MMR) and is one of the very few molecular markers with proven clinical importance in colorectal cancer with respect to heredity, prognosis, and treatment effect. The gene expression of the MMR gene MSH2 may be a quantitative marker for the level of MMR and a potential molecular marker with clinical relevance. The aim was to investigate the gene expression of MSH2 in primary operable colorectal cancer in correlation with MSI, protein expression, and promoter hypermethylation. In a cohort of 210 patients, the primary tumor and lymphnode metastases were analyzed with immunohistochemistry, methylation and MSI analyses, and quantitative polymerase chain reaction (PCR). The median gene expression of MSH2 was 1.00 (range 0.16-11.2, quartiles 0.70-1.51) and there was good agreement between the gene expression in primary tumor and lymph node metastasis (Spearman's rho = 0.57, p < 0.001, n = 73). The validity of gene expression analysis was made probable by a significant correlation to protein expression (p = 0.005). MSI was most often caused by deficient MLH1 and was not correlated to MSH2 expression. Hypermethylation of the MSH2 gene promoter was only detected in 14 samples and only at a low level with no correlation to gene expression. MSH2 gene expression was not a prognostic factor for overall survival in univariate or multivariate analysis. The gene expression of MSH2 is a potential quantitative marker ready for further clinical validation.

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Year:  2011        PMID: 21732224     DOI: 10.1007/s13277-011-0199-9

Source DB:  PubMed          Journal:  Tumour Biol        ISSN: 1010-4283


  32 in total

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  5 in total

1.  Regulation of MLH1 mRNA and protein expression by promoter methylation in primary colorectal cancer: a descriptive and prognostic cancer marker study.

Authors:  Lars Henrik Jensen; Anders Aamann Rasmussen; Lene Byriel; Hidekazu Kuramochi; Dorthe Gylling Crüger; Jan Lindebjerg; Peter V Danenberg; Anders Jakobsen; Kathleen Danenberg
Journal:  Cell Oncol (Dordr)       Date:  2013-09-12       Impact factor: 6.730

2.  Quantitative assessment of the association between XRCC6 C1310G polymorphism and cancer risk.

Authors:  Hong Jiang; Yun Lin; Chang-qing Yang; Qi Li; Jinhong Luo; Ying Zhou; Junli Xue; Wei Wei; Yong Gao
Journal:  Tumour Biol       Date:  2012-12-28

3.  XRCC1 codon 280 polymorphism and susceptibility to lung cancer: a meta-analysis of the literatures.

Authors:  Qin-xiang Guo; Wei-hua Yang; Jin-fang Zhai; Fu-cai Han; Chun-yan Wang
Journal:  Tumour Biol       Date:  2013-06-04

4.  Retrospective analysis of KRAS status in metastatic colorectal cancer patients: a single-center feasibility study.

Authors:  Jonathan Montomoli; Stephen Jacques Hamilton-Dutoit; Trine Frøslev; Aliki Taylor; Rune Erichsen
Journal:  Clin Exp Gastroenterol       Date:  2012-09-18

5.  Prognostic values of DNA mismatch repair genes in ovarian cancer patients treated with platinum-based chemotherapy.

Authors:  Chuchu Zhao; Saisai Li; Menghuang Zhao; Haiyan Zhu; Xueqiong Zhu
Journal:  Arch Gynecol Obstet       Date:  2017-10-23       Impact factor: 2.344

  5 in total

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