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BTK inhibitors synergise with 5-FU to treat drug-resistant TP53-null colon cancers.

Marialuisa Lavitrano ,
Leonarda Ianzano ,
Sara Bonomo ,
Annamaria Cialdella ,
Maria Grazia Cerrito ,
Fabio Pisano ,
Carola Missaglia ,
Roberto Giovannoni ,
Gabriele Romano ,
Chelsea M McLean ,
Emile E Voest ,
Filomena D'Amato ,
Barbara Noli ,
Gian Luca Ferri ,
Marco Agostini ,
Salvatore Pucciarelli ,
Kristian Helin ,
Biagio E Leone ,
Vincenzo Canzonieri ,
Emanuela Grassilli

Abstract

Colorectal cancer (CRC) is the fourth cause of death from cancer worldwide mainly due to the high incidence of drug-resistance. During a screen for new actionable targets in drug-resistant tumours we recently identified p65BTK - a novel oncogenic isoform of Bruton's tyrosine kinase. Studying three different cohorts of patients here we show that p65BTK expression correlates with histotype and cancer progression. Using drug-resistant TP53-null colon cancer cells as a model we demonstrated that p65BTK silencing or chemical inhibition overcame the 5-fluorouracil resistance of CRC cell lines and patient-derived organoids and significantly reduced the growth of xenografted tumours. Mechanistically, we show that blocking p65BTK in drug-resistant cells abolished a 5-FU-elicited TGFB1 protective response and triggered E2F-dependent apoptosis. Taken together, our data demonstrated that targeting p65BTK restores the apoptotic response to chemotherapy of drug-resistant CRCs and gives a proof-of-concept for suggesting the use of BTK inhibitors in combination with 5-FU as a novel therapeutic approach in CRC patients. © 2019 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

More about this publication

The Journal of pathology

Volume 250
Issue nr. 2
Pages 134-147
Publication date 01-02-2020

Full text links

Publisher website (DOI) 10.1002/path.5347
Europe PubMed Central 31518438
Pubmed 31518438

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