Research Papers:
Combined MEK and Pi3’-kinase inhibition reveals synergy in targeting thyroid cancer in vitro and in vivo
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Abstract
Oussama ElMokh1, Dorothée Ruffieux-Daidié1, Matthias A. Roelli1, Amandine Stooss1, Wayne A. Phillips3, Jürg Gertsch1, Matthias S. Dettmer2, Roch-Philippe Charles1
1Institut für Biochemie und Molekulare Medizin, Universität Bern, Bern, Switzerland
2Institut für Pathologie, Universität Bern, Bern, Switzerland
3Cancer Biology Laboratory, Peter MacCallum Cancer Centre, Melbourne, Australia
Correspondence to:
Roch-Philippe Charles, email: [email protected]
Keywords: genetically engineered mice, thyroid cancer, BRAF, Pi3K, combination treatment
Received: September 01, 2016 Accepted: February 06, 2017 Published: February 21, 2017
ABSTRACT
Anaplastic thyroid cancers and radioiodine resistant thyroid cancer are posing a major treat since surgery combined with Iodine131 therapy is ineffective on them. Small-molecule inhibitors are presenting a new hope for patients, but often lead to drug resistance in many cancers. Based on the major mutations found in thyroid cancer, we propose the combination of a MEK inhibitor and a Pi3’-kinase inhibitor in pre-clinical models. We used human thyroid cancer cell lines and genetically engineered double mutant BRAFV600E PIK3CAH1047R mice to evaluate the effect of both inhibitors separately or in combination in terms of proliferation and signaling in vitro; tumor burden, histology, cell death induction and tumor markers expression in vivo. The combination of MEK and Pi’3-kinase inhibition shows a synergistic effect in term of proliferation and apoptosis induction through Survivin down-regulation in vitro. We show for the first time the effects of the combination of a MEK inhibitor and Pi3’-kinase inhibitor in a genetically engineered mouse model of aggressively lethal thyroid cancer. In fine, the two drugs cooperate to promote tumor shrinkage by inducing a proliferation arrest and an elevation of apoptosis in vivo. Moreover, a phenotypic reversion is also observed with a partial restoration of normal thyroid marker transcription, and thyroid cancer marker expression reduction.
In conclusion, combination therapy of MEK and Pi3’-kinase inhibition synergizes to target double mutant thyroid cancer in vitro and in vivo. This multidrug approach could readily be translated into clinical practice and bring new perspectives for the treatment of incurable thyroid carcinoma.
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