STAT3 paradoxically stimulates β‐catenin expression but inhibits β‐catenin function

Summary Wnt signalling and the signal transducer and activator of transcription 3 (STAT3) are oncogenic signalling pathways which are deregulated in colorectal cancer (CRC). Here we investigated the interaction of these two pathways. Firstly, we investigated biochemical interaction by inhibiting STAT3 and β‐catenin (through gene knock‐down and dominant‐negative TCF4 expression) in nine CRC cell lines. β‐catenin inhibition did not affect STAT3 levels, whereas STAT3 knock‐down resulted in reduced β‐catenin mRNA and protein levels. The reduction in β‐catenin protein was not prevented by proteasome inhibition, and IL6‐induced STAT3 activation resulted in increased β‐catenin mRNA. This suggests that STAT3 positively regulates β‐catenin (at a transcriptional level) and evaluation of 44 CRCs by immunostaining supported this by showing an association between nuclear STAT3 expression and nuclear β‐catenin (P = 0.022). We tested the functional interaction between STAT3 and Wnt signalling by knocking down STAT3 and β‐catenin individually and in combination. Knock‐down of β‐catenin and STAT3 individually inhibited cell proliferation (P < 0. 001 for each) through G1 arrest. However, simultaneous knock‐down of STAT3 and β‐catenin had a significantly weaker effect than knock‐down of β‐catenin alone (P < 0.01). Knock‐down of STAT3 and β‐catenin, individually and together, inhibited cell motility (P < 0.001) without evidence...
Source: International Journal of Experimental Pathology - Category: Pathology Authors: Tags: Original Article Source Type: research