Abstract EN:

Our work aims to study the action of an EGFR inhibitor (erlotinib) in patients with HNSCC; and to identify predictive markers of response in order to select patients that can benefit of the treatment. Immunochemistry analyses were performed on tumor tissues and show that basal p21waf expression (CDK-cyclins inhibitor) was positively associated with tumor response. EGFR mutations and Kras mutations were not detected in HNSCC patients of our study. . The EGFR gene copy number, that has been identified as a factor linked with tyrosine kinase inhibitors sensitivity in lung cancer, did not correlate with clinical response. We also studied erlotinib pharmacokinetics and try to establish pharmacokinetics/pharmacodynamics relationships (PK /PD relationships). Pharmacokinetic analysis show that the smoking status, the hepatic function and age were relevant covariates to predict erlotinib elimination. Moreover, there is a relationship between drug exposure and toxicity but not between exposure and response. The last part of this work consisted in analysing genomic expression of the tumors before and after treatment by using microarrays (Affymetrix HG U133A GeneChip(r)) to identify genes differentially expressed in responders versus non responders and to characterize erlotinib effect on genes expression.