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Prostate cancer is one of the leading causes of cancer illness and death among men in the United States and world wide. There is an urgent need to discover good biomarkers for early clinical diagnosis and treatment. Previously, we developed an exon-junction microarray-based assay and profiled 1532 mRNA splice isoforms from 364 potential prostate cancer related genes in 38 prostate tissues. Here, we investigate the advantage of using splice isoforms, which couple transcriptional and splicingdoi:10.1186/1471-2105-7-202 pmid:16608523 pmcid:PMC1458362 fatcat:cgve6kwsxfbxnpooaxpeiwjbae