Abstract

The complexity of hepatocellular carcinoma (HCC) challenges the identification of disease-relevant signals. C3G, a guanine nucleotide exchange factor for Rap and other Ras proteins, plays a dual role in cancer acting as either a tumor suppressor or promoter depending on tumor type and stage. The potential relevance of C3G upregulation in HCC patients suggested by database analysis remains unknown. We have explored C3G function in HCC and the underlying mechanisms using public patient data and in vitro and in vivo human and mouse HCC models. We found that C3G is highly expressed in progenitor cells and neonatal hepatocytes, whilst being down-regulated in adult hepatocytes and re-expressed in human HCC patients, mouse HCC models and HCC cell lines. Moreover, high C3G mRNA levels correlate with tumor progression and a lower patient survival rate. C3G expression appears to be tightly modulated within the HCC program, influencing distinct cell biological properties. Hence, high C3G expression levels are necessary for cell tumorigenic properties, as illustrated by reduced colony formation in anchorage-dependent and -independent growth assays induced by permanent C3G silencing using shRNAs. Additionally, we demonstrate that C3G down-regulation interferes with primary HCC tumor formation in xenograft assays, increasing apoptosis and decreasing proliferation. In vitro assays also revealed that C3G down-regulation enhances the pro-migratory, invasive and metastatic properties of HCC cells through an epithelial-mesenchymal switch that favors the acquisition of a more mesenchymal phenotype. Consistently, a low C3G expression in HCC cells correlates with lung metastasis formation in mice. However, the subsequent restoration of C3G levels is associated with metastatic growth. Mechanistically, C3G down-regulation severely impairs HGF/MET signaling activation in HCC cells. Collectively, our results indicate that C3G is a key player in HCC. C3G promotes tumor growth and progression, and the modulation of its levels is essential to ensure distinct biological features of HCC cells throughout the oncogenic program. Furthermore, C3G requirement for HGF/MET signaling full activation provides mechanistic data on how it works, pointing out the relevance of assessing whether high C3G levels could identify HCC responders to MET inhibitors.

Highlights

  • Hepatocellular carcinoma (HCC) is the sixth most common cancer worldwide and the second deadliest cancer for men and sixth for women [1]

  • HCC results as a neoplastic transformation of hepatocytes and/or progenitor cells [2] that can go through an epithelial to mesenchymal transition (EMT) acquiring pro-migratory properties [3]

  • We found that C3G protein levels increase in human and mouse HCC cell lines and in two models of mouse HCC, induced by either DEN treatment or enhanced MET expression in hepatocytes

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Summary

Introduction

Hepatocellular carcinoma (HCC) is the sixth most common cancer worldwide and the second deadliest cancer for men and sixth for women [1]. HCC results as a neoplastic transformation of hepatocytes and/or progenitor cells [2] that can go through an epithelial to mesenchymal transition (EMT) acquiring pro-migratory properties [3]. HCC heterogeneity and its late diagnosis are relevant factors for the lack of effective therapies and recurrence. The receptor tyrosine kinase MET is frequently overexpressed in HCC [4], activated in about. 50% of HCC patients, and linked to an aggressive phenotype [5,6]. A recent report based on a meta-analysis of tumors from patients suffering a surgical resection showed a significant poor prognosis associated to MET overexpression, due to a higher recurrence [7]. The implication of c-MET in HCC has prompted a number of clinical trials using MET targeting agents (alone or in combination) for HCC treatment in recent years [8,9,10]

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