High-resolution analysis of paraffin-embedded and formalin-fixed prostate tumors using comparative genomic hybridization to genomic microarrays |
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Authors: | Paris Pamela L Albertson Donna G Alers Janneke C Andaya Armann Carroll Peter Fridlyand Jane Jain Ajay N Kamkar Sherwin Kowbel David Krijtenburg Pieter-Jaap Pinkel Daniel Schröder Fritz H Vissers Kees J Watson Vivienne J E Wildhagen Mark F Collins Colin Van Dekken Herman |
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Affiliation: | Comprehensive Cancer Center, University of California at San Francisco, San Francisco, California 94115, USA. |
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Abstract: | We have used prostate cancer, the most commonly diagnosed noncutaneous neoplasm among men, to investigate the feasibility of performing genomic array analyses of archival tissue. Prostate-specific antigen and a biopsy Gleason grade have not proven to be accurate in predicting clinical outcome, yet they remain the only accepted biomarkers for prostate cancer. It is likely that distinct spectra of genomic alterations underlie these phenotypic differences, and that once identified, may be used to differentiate between indolent and aggressive tumors. Array comparative genomic hybridization allows quantitative detection and mapping of copy number aberrations in tumors and subsequent associations to be made with clinical outcome. Archived tissues are needed to have patients with sufficient clinical follow-up. In this report, 20 formalin-fixed and paraffin-embedded prostate cancer samples originating from 1986 to 1996 were studied. We present a straightforward protocol and demonstrate the utility of archived tissue for array comparative genomic hybridization with a 2400 element BAC array that provides high-resolution detection of both deletions and amplifications. |
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