Enhanced expression of cyclooxygenase-2 and nuclear beta-catenin are related to mutations in the APC gene in human colorectal cancer

Mutational inactivation of the human tumour suppressor gene adenomatous pol yposis coli (APC) results in constitutive activation of beta -catenin/T cel l factor-4 (Tcf-4) mediated transcription of target genes. Up-regulation of cyclooxygenase-2 (COX-2) protein is frequently found in human colorectal c ancer (CRC). We analysed 38 CRC for mutations in APC and beta -catenin and found an association between APC mutations and elevated COX-2 levels. Furth ermore, APC mutations were predominantly observed in tumour tissues from th e rectum compared to tumours of colonic origin. Western blot analysis revea led that nuclear beta -catenin levels were generally higher in tumours with APC mutations compared to tumours with wild type APC. However, there was a lso a higher level of nuclear beta -catenin in tumour compared to normal ti ssue, hut nuclear Tcf-4 protein was constitutively expressed in tumour and normal tissue and showed no differences. An identified putative Tcf-4 bindi ng element in the COX-2 promoter may partly explain the enhanced level of C OX-2 and support the idea that COX-2 may be a downstream target of the APC/ beta -catenin/Tcf-4 pathway.