Preferential Response of Basal-Like Head and Neck Squamous Cell Carcinoma Cell Lines to EGFR-Targeted Therapy Depending on -Driven Oncogenic Addiction

Overview

Journal Cancers (Basel)

Publisher MDPI

Specialty Oncology

Date 2019 Jun 12

PMID 31181806

Citations 12

Authors

Sylvie Job

Aurelien De Reynies

Betty Heller

Amelie Weiss

Eric Guerin

Christine Macabre

Sonia Ledrappier

Cyril Bour

Christine Wasylyk

Nelly Etienne-Selloum

Laurent Brino

Christian Gaiddon

Bohdan Wasylyk

Alain C Jung

Affiliations

Soon will be listed here.

Abstract

The management of locally advanced head and neck squamous cell carcinoma (HNSCC) with Cetuximab, a monoclonal antibody targeting the epidermal growth factor receptor (EGFR), achieves only moderate response rates, and clinical trials that evaluated EGFR-blockade with tyrosine kinase inhibitors (TKI) yielded disappointing results. Inter-tumor heterogeneity may hinder the therapeutic efficiency of anti-EGFR treatments. HNSCC heterogeneity was addressed in several studies, which all converged towards the definition of molecular subgroups. They include the basal subgroup, defined by the deregulated expression of factors involved in the EGFR signaling pathway, including the epiregulin EGFR ligand encoded by the gene. These observations indicate that basal tumors could be more sensitive to anti-EGFR treatments. To test this hypothesis, we performed a screen of a representative collection of basal versus non-basal HNSCC cell lines for their sensitivity to several anti-EGFR drugs (Cetuximab, Afatinib, and Gefitinib), tested as monotherapy or in combination with drugs that target closely-linked pathways [Mitogen-activated protein kinase kinase/ extracellular signal-regulated kinases (MEK), mammalian Target of Rapamycine (mTOR) or Human Epidermal growth factor Receptor 2 (HER2)]. Basal-like cell lines were found to be more sensitive to EGFR blockade alone or in combination with treatments that target MEK, mTOR, or HER2. Strikingly, the basal-like status was found to be a better predictor of cell response to EGFR blockade than clinically relevant mutations [e.g., cyclin-dependent kinase Inhibitor 2A ()]. Interestingly, we show that EGFR blockade inhibits expression, and that knock-down decreases basal cell clonogenic survival, suggesting that expression could be a predictive functional marker of sensitivity to EGFR blockade in basal-like HNSCC.

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