RON (MST1R) is a Novel Prognostic Marker and Therapeutic Target for Gastroesophageal Adenocarcinoma

Overview

Journal Cancer Biol Ther

Specialties Oncology
Pharmacology

Date 2011 May 6

PMID 21543897

Citations 51

Authors

Daniel V T Catenacci

Gustavo Cervantes

Soheil Yala

Erik A Nelson

Essam El-Hashani

Rajani Kanteti

Mohamed El Dinali

Rifat Hasina

Johannes Bragelmann

Tanguy Seiwert

Michele Sanicola

Les Henderson

Tatyana A Grushko

Olufunmilayo Olopade

Theodore Karrison

Yung-Jue Bang

Woo Ho Kim

Maria Tretiakova

Everett Vokes

David A Frank

Hedy L Kindler

Heather Huet

Ravi Salgia

Affiliations

Soon will be listed here.

Abstract

RON (MST1R) is one of two members of the MET receptor tyrosine kinase family, along with parent receptor MET. RON has a putative role in several cancers, but its expression and function is poorly characterized in gastroesophageal adenocarcinoma. A recognized functional role of MET tyrosine kinase in gastroesophageal cancer has led to early phase clinical trials using MET inhibitors, with unimpressive results. Therefore, the role of RON in gastroesophageal cancer, as well as its role in cooperative signaling with MET and as a mechanism of resistance to MET inhibition, was studied in gastroesophageal tissues and cell lines. By IHC, RON was highly over-expressed in 74% of gastroesophageal samples (n=94), and over-expression was prognostic of poor survival (p=0.008); RON and MET co-expression occurred in 43% of samples and was prognostic of worst survival (p=0.03). High MST1R gene copy number by quantitative polymerase chain reaction, and confirmed by fluorescence in situ hybridization and/or array comparative genomic hybridization, was seen in 35.5% (16/45) of cases. High MST1R gene copy number correlated with poor survival (p=0.01), and was associated with high MET and ERBB2 gene copy number. A novel somatic MST1R juxtamembrane mutation R1018G was found in 11% of samples. RON signaling was functional in cell lines, activating downstream effector STAT3, and resulted in increased viability over controls. RON and MET co-stimulation assays led to enhanced malignant phenotypes over stimulation of either receptor alone. Growth inhibition as evidenced by viability and apoptosis assays was optimal using novel blocking monoclonal antibodies to both RON and MET, versus either alone. SU11274, a classic MET small molecule tyrosine kinase inhibitor, blocked signaling of both receptors, and proved synergistic when combined with STAT3 inhibition (combination index < 1). These preclinical studies define RON as an important novel prognostic marker and therapeutic target for gastroesophageal cancer warranting further investigation.

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