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Comethylation of p16 and MGMT genes in colorectal carcinoma: Correlation with clinicopathological features and prognostic value

摘要AIM: To investigate the significance of p16 and O6-methylguanine-DNA methyltransferase (MGMT) genes promoter hypermethylation and K-ras mutations on colorectal tumorigenesis and progression.METHODS: p16 and MGMT methylation status was examined on 47 tumor samples, and K-ras mutational status was examined on 85 tumor samples. For methylation analysis, a methylation specific PCR (MS-PCR)method was used.RESULTS: p16 and MGMT promoter methylation was found in 51% (24/47) and 43% (20/47) of CRCs,respectively, and the K-ras mutation was found in 44%(37/85) of CRCs. Comethylation ofp16 and MGMT genes was significantly associated with lower aggressiveness of the disease within a two-year period of observation.Only 27% of patients with simultaneous p16 and MGMT methylation showed the detectible occurrence of metastasis and/or death, compared to 67% of patients without double methylation or with no methylation (3/11vs 22/33, P < 0.05, x2-test). In addition, p16 and MGMT comethylation showed a trend toward an association with longer survival in patients with CRCs (35.5 ± 6.0 movs 23.1 ± 3.2 mo, P = 0.072, Log-rank test). Progression of the disease within a two-year period was observed in 66% of patients carrying the K-ras mutation, compared to only 19% of patients with wild type K-ras (29/44 vs7/37, P < 0.001, x2-test). The presence of the K-ras mutation significantly correlated to shortened overall survival (20.0 ± 1.9 mo vs 37.0 ± 1.8 mo, P < 0.001, Logrank test). The comethylation of p16 and MGMT genes was significantly associated with lower aggressiveness of the disease even when K-ras mutations were included in the analysis as an independent variable.CONCLUSION: Our data suggest that comethylation of promoters of p16 and MGMT genes could have a prognostic value in patients with CRC. Specifically,concurrent methylation of both genes correlates with better prognosis.

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作者单位 Laboratory for Radiobiology and Molecular Genetics, Institute of Nuclear Sciences "Vinca", P. O. BOX 522, Belgrade, Serbia [1] Institute of Oncology,Sremska Kamenica, Serbia [2] Institute for Medical Statistics of Medical University, Belgrade, Serbia [3]
分类号 R73(肿瘤学)
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发布时间 2007-05-10(万方平台首次上网日期,不代表论文的发表时间)
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