Inheritance of the 194Trp and the 399Gln variant alleles of the DNA repair gene XRCC1 are associated with increased risk of early-onset colorectal carcinoma in Egypt

Sherif Z. Abdel-Rahman, Amr S. Soliman, Melissa L. Bondy, Sherif Omar, Samy A. El-Badawy, Hussein M. Khaled, Ibrahim A. Seifeldin, Bernard Levin

    Research output: Contribution to journalArticlepeer-review

    179 Scopus citations

    Abstract

    Patients under age 40 constitute 35.6% of all colorectal cancer cases in Egypt, an unusual disease pattern to which both environmental exposures and inefficient DNA repair may contribute. While a number of polymorphisms in DNA repair genes have been recently identified, their role as cancer risk modifiers is yet to be determined. In a pilot case-control study, we tested the hypothesis that polymorphisms in the gene for the DNA repair enzyme XRCC1 are associated with increased risk of colorectal cancer among Egyptians. Using a multiplex polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) methodology, allelic variants of the XRCC1 gene at codons 194 (Arg → Trp) (194Trp) and 399 (Arg → Gln) (399Gln), were analyzed in DNA from lymphocytes of 48 newly-diagnosed colorectal cancer cases and 48 age- and sex-matched controls. Overall, the inheritance of 194Trp allele (Arg/Trp genotype) and 399Gln allele (combined Arg/Gln and Gln/Gln genotypes) was associated with increased colorectal cancer risk (odds ratio (OR) = 2.56, 95% confidence limits (CL) 0.73-9.40, and P = 0.08 for 194Trp allele and OR = 3.98, 95% CL 1.50-10.6, and P < 0.001 for 399Gln allele). Interestingly, the frequencies of 194Trp and 399Gln genotypes were higher in colorectal cancer cases under age 40 than in corresponding controls, and an association between both polymorphisms and early age of disease onset was observed (OR = 3.33, 95% CL 0.48-35.90, and P = 0.16 for 194Trp and OR = 11.90, 95% CL 2.30-51.50, and P = 0.0003 for 399Gln). Analysis of the data after adjustment for place of residence indicated that the frequencies of the genotypes with the 194Trp and the 399Gln alleles were higher among urban residents (OR = 3.33, 95% CL 0.48-35.90, and P = 0.16 for 194Trp and OR = 9.97, 95% CL 1.98-43.76, and P < 0.001 for 399Gln) than among rural residents (OR = 2.00, 95% CL 0.36-26.00, and P = 0.30 for 194Trp and OR = 1.90, 95% CL 0.50-7.53, and P = 0.20 for 399Gln). These findings support our hypothesis and suggest that polymorphisms in the XRCC1 gene, in conjunction with place of residence, may modify disease risk. This first demonstration that polymorphisms in DNA repair genes may contribute to colorectal cancer susceptibility and may increase the risk of early onset of the disease opens the door for future studies in that direction. (C) 2000 Published by Elsevier Science Ireland Ltd.

    Original languageEnglish (US)
    Pages (from-to)79-86
    Number of pages8
    JournalCancer Letters
    Volume159
    Issue number1
    DOIs
    StatePublished - Oct 16 2000

    Keywords

    • Aging
    • Biomarkers
    • Colorectal cancer
    • DNA repair
    • Genetic polymorphism
    • Genetic susceptibility
    • Polymerase chain reaction
    • XRCC1

    ASJC Scopus subject areas

    • Oncology
    • Cancer Research

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