Colorectal Cancer
Copyright ©2007 Baishideng Publishing Group Co., Limited. All rights reserved.
World J Gastroenterol. Sep 7, 2007; 13(33): 4437-4444
Published online Sep 7, 2007. doi: 10.3748/wjg.v13.i33.4437
Importance of MutL homologue MLH1 and MutS homologue MSH2 expression in Turkish patients with sporadic colorectal cancer
Sibel Erdamar, Esra Ucaryilmaz, Gokhan Demir, Tayfun Karahasanoglu, Gulen Dogusoy, Ahmet Dirican, Suha Goksel
Sibel Erdamar, Esra Ucaryilmaz, Gulen Dogusoy, Suha Goksel, Department of Pathology, Cerrahpasa Medical College, Istanbul University, Cerrahpasa 34303, Istanbul, Turkey
Gokhan Demir, Department of Oncology, Cerrahpasa Medical College, Istanbul University, Cerrahpasa 34303, Istanbul, Turkey
Tayfun Karahasanoglu, Department of General Surgery, Cerrahpasa Medical College, Istanbul University, Cerrahpasa 34303, Istanbul, Turkey
Ahmet Dirican, Department of Statistics, Cerrahpasa Medical College, Istanbul University, Cerrahpasa 34303, Istanbul, Turkey
Author contributions: All authors contributed equally to the work.
Supported by the Research Foundation of Istanbul University, No T-493/25062004
Correspondence to: Sibel Erdamar, MD, Department of Pathology, Cerrahpasa Medical College, Istanbul University, Cerrahpasa 34303, Istanbul, Turkey. serdamar@hotmail.com
Telephone: +90-532-7098456 Fax: +90-212-4143000-21850
Received: May 23, 2007
Revised: June 6, 2007
Accepted: June 9, 2007
Published online: September 7, 2007
Abstract

AIM: To assess the incidence of MLH1 (the human MutL homologue) and MSH2 (the human MutS homologue) protein expression in Turkish patients with sporadic colorectal cancers and to compare their survival and clinicopathological features.

METHODS: We validated the tissue microarray technology in 77 colorectal carcinomas by analyzing the immunohistochemical expression of proteins involved in two main pathways of colorectal carcinogenesis: p53 protein for loss of heterozygosity tumors; MLH1 and MSH2 proteins for microsatellite instability (MSI).

RESULTS: Our analysis showed that 29 (39.2%) had loss of MLH1 expression, 5 (6.8%) had loss of MSH2 expression and 2 cases had loss of expression of both proteins. We found that 60% of MSH2-negative tumors were located in the right side of the colon; all MSH2-negative cases were women. In addition, the loss of MSH2 expression was correlated with low p53 expression. Neither MLH1 nor MSH2 expressions were associated with prognosis, although there seemed a tendency of longer survival (71.7 ± 8.65 mo vs 47.08 ± 5.26 mo) for the patients with MLH1-negative versus MLH1-positive carcinomas. There were not significant differences in overall and recurrence-free survival among MLH1/MSH2-positive and -negative cases.

CONCLUSION: Our data supports that Turkish patients with MLH1- and MSH2-defective tumors have some distinct features from each other. Although prognostic importance remains controversial, immunohistochemical analysis of mismatch repair genes may be used as a routine histopathological examination of sporadic colorectal carcinomas.

Keywords: Colorectal carcinoma; MLH1; MSH2; Immunohistochemistry; Prognosis