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Identification of molecular targets for the targeted treatment of gastric cancer using dasatinib

Authors :
Alessandro Ceroni
Vita Fedele
Batoul Farran
Felipe Pantoja Mesquita
Martin Frejno
Rommel Mario Rodriguez Burbano
Raquel Carvalho Montenegro
Stephanie Heinzlmeir
Stefan Knapp
Susanne Müller
Bernhard Kuster
Alison Howarth
Roberta Tesch
Heba Z. Sailem
Daniel Ebner
Benedict-Tilman Berger
Source :
Oncotarget, Scopus-Elsevier
Publication Year :
2020
Publisher :
Impact Journals LLC, 2020.

Abstract

Gastric cancer (GC) remains the third leading cause of cancer-related death despite several improvements in targeted therapy. There is therefore an urgent need to investigate new treatment strategies, including the identification of novel biomarkers for patient stratification. In this study, we evaluated the effect of FDA-approved kinase inhibitors on GC. Through a combination of cell growth, migration and invasion assays, we identified dasatinib as an efficient inhibitor of GC proliferation. Mass-spectrometry-based selectivity profiling and subsequent knockdown experiments identified members of the SRC family of kinases including SRC, FRK, LYN and YES, as well as other kinases such as DDR1, ABL2, SIK2, RIPK2, EPHA2, and EPHB2 as dasatinib targets. The expression levels of the identified kinases were investigated on RNA and protein level in 200 classified tumor samples from patients, who had undergone gastrectomy, but had received no treatment. Levels of FRK, DDR1 and SRC expression on both mRNA and protein level were significantly higher in metastatic patient samples regardless of the tumor stage, while expression levels of SIK2 correlated with tumor size. Collectively, our data suggest dasatinib for treatment of GC based on its unique property, inhibiting a small number of key kinases (SRC, FRK, DDR1 and SIK2), highly expressed in GC patients.

Details

Language :
English
ISSN :
19492553
Volume :
11
Issue :
5
Database :
OpenAIRE
Journal :
Oncotarget
Accession number :
edsair.doi.dedup.....2cf76ce7abc732a96718ad42c687aa0d