Mutagen Sensitivity, Apoptosis, and Polymorphism in DNA Repair as Measures of Prostate Cancer Risk

Abstract

This proposal evaluates interindividual differences in the response to genotoxic stress as prostate cancer risk factors. To this end we use measurements of mutagen sensitivity, apoptosis, comet assay, and single nucleotide polymorphisms in DNA repair genes OGG1 and XRCC1. These biomarkers are evaluated in 100 prostate cancer cases and 100 controls matched on age and race in order to measure response to bleomycin exposure is short-term cultured lymphocytes to define prostate cancer risk. We designed a new protocol, study questionnaire, updated consent forms and recruitment brochures to establish a case-control study of prostate cancer. During the second year of funding, we recruited 51 prostate cancer cases and 40 matched controls at the Georgetown University Hospital. A research assistant created a sample repository consisting of serum, plasma, buffy coat, urine, toenail clipping and saliva for every participant. We also created a computerized database of the samples in Microsoft Access. The research assistant measured mutagen sensitivity in all the subjects and determined the mean breaks in lymphocytes exposed to bleomycin in cases (mean 0.88 SD 0.32) and controls (mean 0.74 SD 0.34). We continue to optimize the apoptosis and comet assay protocols to measure DNA repair kinetic and cell death in exposed cells. We expect to proceed rapidly with the case-control study in the third year.

Document Details

Document Type

Technical Report

Publication Date

Feb 01, 2005

Accession Number

ADA437779

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