PO-066 Knockdown of cadherin 17 inactivates WNT signalling pathway and induces apoptosis in colorectal cancer cells

Large scale sequencing studies have identified that 93% of the colorectal cancer (CRC) patients carry at least one mutation in genes implicated in Wnt signalling pathway. Notably, majority of the CRC patients (88%) carry either APC or β-catenin mutations that can activate the Wnt signalling pathway....

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Published in:ESMO open 2018-06, Vol.3, p.A47-A47
Main Authors: Atukorala, I., Mathivanan, S.
Format: Article
Language:English
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Summary:Large scale sequencing studies have identified that 93% of the colorectal cancer (CRC) patients carry at least one mutation in genes implicated in Wnt signalling pathway. Notably, majority of the CRC patients (88%) carry either APC or β-catenin mutations that can activate the Wnt signalling pathway. Recent evidences suggest that Wnt/β-catenin signalling activity is regulated by CDH17 in hepatocellular carcinoma. As CDH17 is exclusively expressed in the intestine and overexpressed in CRC, we hypothesised that CDH17 could be utilised as a therapeutic target to treat CRC patients. RNA interference-based stable knockdowns were established in a panel of CRC cells with varying mutations in APC and β-catenin. Wnt signalling activity of the cells were measured by TOPflash assay. Apoptosis studies were performed using fluorescence activated cell sorting. Cells were further subjected to immunoprecipitations with anti-CDH17 and anti-β-catenin antibodies followed by label-free quantitative proteomics analysis. A monoclonal antibody was developed to block CDH17 and sensitise CRC cells to chemotherapeutic drugs. Knockdown of CDH17 in CRC cells downregulated β-catenin and attenuated Wnt signalling activity irrespective of APC and/or β-catenin mutations. Furthermore, CDH17 silencing induced apoptosis and sensitised CRC cells to the chemotherapeutic drugs 5-Fluorouracil. Immunoprecipitations using anti-CDH17 and anti-β-catenin antibodies followed by label-free quantitative proteomics analysis highlighted no direct interaction between CDH17 and β-catenin hence implying an indirect regulation of β-catenin expression and Wnt signalling pathway by CDH17. The analysis revealed E-cadherin and FAT1 as common interactors of CDH17 and β-catenin. Quantitative proteomic analysis of cell lysates revealed the upregulation of FAT1, a negative regulator of Wnt signalling pathway, upon knockdown of CDH17. Monoclonal antibodies developed against CDH17 were able to increase apoptosis and sensitivity of CRC cells to 5-Fluorouracil. Overall, these findings suggest that CDH17 can attenuate Wnt signalling pathway and induce apoptosis irrespective of the APC and β-catenin mutational status. As Wnt signalling pathway is aberrated in 93% of CRC patients, the membrane protein CDH17 can be exploited as therapeutic target to treat CRC.
ISSN:2059-7029
2059-7029
DOI:10.1136/esmoopen-2018-EACR25.110