Hepatocellular Carcinoma Clinical Trial
Official title:
Analysis of the Role of Hepatocyte SLAMF3 Receptor and Drug Resistance Proteins (MDR) in Resistance to Treatment With Sorafenib in CHC Patients
Primary liver cancer or hepatocellular carcinoma (HCC) is the 7th most common cancer in
humans; 9th in women (figures from the Association for Research against Cancer ARC). This
cancer is a major public health problem on a global scale. Patients, whose diagnosis is
often late, are at advanced stages of the pathology, even those who benefit from
locoregional treatments have a poor prognosis and suffer from a lack of curative therapeutic
strategies. CHC is highly refractory to cytotoxic chemotherapy and so far the response rates
to conventional systemic chemotherapy has provided a clinical benefit where survival was
prolonged by more than 25% in patients with advanced CHC. Further efforts are needed to
effectively manage HCC. Knowledge of the mechanisms regulating proliferation and inhibiting
the sensitivity of transformed cells to apoptosis is the key to the development of more
effective therapeutic strategies.
Several new therapies, called targeted therapies, are tested in clinical trials. Currently,
the most effective molecular agent for targeting the Raf pathway is sorafenib capable of
also inhibiting tyrosine kinases of VEGFR and PDGFR. Sorafenib, a multikinase inhibitor,
decreases the proliferation of tumor cells in vitro that inhibit the activity of targets
present in tumor cells (CRAF, BRAF, V600E BRAF, c-KIT, and FLT-3) and tumor vascularization
VEGFR-2, VEGFR-3, and PDGFR-beta). Despite the real benefit of this treatment, its efficacy
(three months of overall survival) and its indication remain limited to Child-Pugh A, WHO
0-2 patients in whom curative treatment is contraindicated. In addition, several patients
have resistance to Sorafenib and thus find themselves in therapeutic failure, thus limiting
the therapeutic choice for these patients.
Resistance to treatment with Sorafenib limits the therapeutic choice. The mechanisms
responsible for this resistance remain to be elucidated. Drug resistance proteins, MDR
Multi-Drug Resistance, is a family of molecules whose expression increases in the cancer
cell and ensures the repression of chemotherapy molecules outside the target cancer cell.
This family includes the proteins ABCG2, MDR and MRP1. Our in vitro studies show that
treatment of CHC Huh-7 cells with Sorafenib (10 mM) induces the specific expression of the
transcripts of the MRP-1 protein without any effect on the expression of the ABCG2 and MDR
protein. In addition, sorafenib has an effect on the expression of hepatocyte SLAMF3
receptor transcripts, a receptor recently identified in hepatocyte tissue. Indeed, it has
been shown that the expression of SLAMF3 is lowered in the cancerous tissue compared to the
healthy tissue and that the reintroduction of a strong expression in the cancer cell
inhibits its proliferation by inhibiting the MAPK Erk pathway, Cancer cells to apoptosis and
inhibits the uptake of tumor masses in the Nude mouse (I. Marcq, et al., 2013).
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