Therapeutic potential of combined BRAF/MEK blockade in BRAF-wild type preclinical tumor models

Anais Del Curatolo; Fabiana Conciatori; Ursula Cesta Incani; Chiara Bazzichetto; Italia Falcone; Vincenzo Corbo; Sabrina D’Agosto; Adriana Eramo; Giovanni Sette; Isabella Sperduti; Teresa De Luca; Mirko Marabese; Senji Shirasawa; Ruggero De Maria; Aldo Scarpa; Massimo Broggini; Donatella Del Bufalo; Francesco Cognetti; Michele Milella; Ludovica Ciuffreda

doi:10.1186/s13046-018-0820-5

Journal of Experimental & Clinical Cancer Research (Jul 2018)

Therapeutic potential of combined BRAF/MEK blockade in BRAF-wild type preclinical tumor models

Anais Del Curatolo,
Fabiana Conciatori,
Ursula Cesta Incani,
Chiara Bazzichetto,
Italia Falcone,
Vincenzo Corbo,
Sabrina D’Agosto,
Adriana Eramo,
Giovanni Sette,
Isabella Sperduti,
Teresa De Luca,
Mirko Marabese,
Senji Shirasawa,
Ruggero De Maria,
Aldo Scarpa,
Massimo Broggini,
Donatella Del Bufalo,
Francesco Cognetti,
Michele Milella,
Ludovica Ciuffreda

Affiliations

Anais Del Curatolo: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Fabiana Conciatori: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Ursula Cesta Incani: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Chiara Bazzichetto: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Italia Falcone: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Vincenzo Corbo: ARC-Net Research Centre and Department of Pathology, University of Verona
Sabrina D’Agosto: ARC-Net Research Centre and Department of Pathology, University of Verona
Adriana Eramo: Department of Hematology, Oncology and Molecular Medicine, Istituto Superiore di Sanità
Giovanni Sette: Department of Hematology, Oncology and Molecular Medicine, Istituto Superiore di Sanità
Isabella Sperduti: Biostatistics, IRCCS Regina Elena National Cancer Institute
Teresa De Luca: Preclinical Models and New Therapeutic Agents Unit, IRCCS Regina Elena National Cancer Institute
Mirko Marabese: Laboratory of Molecular Pharmacology, Department of Oncology, IRCCS - Istituto di Ricerche Farmacologiche “Mario Negri”
Senji Shirasawa: Central Research Institute for Advanced Molecular Medicine, Fukuoka University
Ruggero De Maria: Institute of General Pathology, Catholic University of the Sacred Heart
Aldo Scarpa: ARC-Net Research Centre and Department of Pathology, University of Verona
Massimo Broggini: Laboratory of Molecular Pharmacology, Department of Oncology, IRCCS - Istituto di Ricerche Farmacologiche “Mario Negri”
Donatella Del Bufalo: Preclinical Models and New Therapeutic Agents Unit, IRCCS Regina Elena National Cancer Institute
Francesco Cognetti: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Michele Milella: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute
Ludovica Ciuffreda: Medical Oncology 1, IRCCS Regina Elena National Cancer Institute

DOI: https://doi.org/10.1186/s13046-018-0820-5
Journal volume & issue: Vol. 37, no. 1
pp. 1 – 14

Abstract

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Abstract Background Mounting evidence suggests that RAF-mediated MEK activation plays a crucial role in paradox MAPK (re)activation, leading to resistance and therapeutic failure with agents hitting a single step along the MAPK cascade. Methods We examined the molecular and functional effects of single and combined BRAF (dabrafenib), pan-RAF (RAF265), MEK (trametinib) and EGFR/HER2 (lapatinib) inhibition, using Western Blot and conservative isobologram analysis to assess functional synergism, and explored genetic determinants of synergistic interactions. Immunoprecipitation based assays were used to detect the interaction between BRAF and CRAF. The Mann-Whitney U test was used for comparing quantitative variables. Results Here we demonstrated that a combination of MEK and BRAF inhibitors overcomes paradoxical MAPK activation (induced by BRAF inhibitors) in BRAF-wt/RAS-mut NSCLC and PDAC in vitro. This results in growth inhibitory synergism, both in vitro and in vivo, in the majority (65%) of the cellular models analyzed, encompassing cell lines and patient-derived cancer stem cells and organoids. However, RAS mutational status is not the sole determinant of functional synergism between RAF and MEK inhibitors, as demonstrated in KRAS isogenic tumor cell line models. Moreover, in EGFR-driven contexts, paradoxical MAPK (re)activation in response to selective BRAF inhibition was dependent on EGFR family signaling and could be offset by simultaneous EGFR/HER-2 blockade. Conclusions Overall, our data indicate that RAF inhibition-induced paradoxical MAPK activation could be exploited for therapeutic purposes by simultaneously targeting both RAF and MEK (and potentially EGFR family members) in appropriate molecular contexts. KRAS mutation per se does not effectively predict therapeutic synergism and other biomarkers need to be developed to identify patients potentially deriving benefit from combined BRAF/MEK targeting.

Published in Journal of Experimental & Clinical Cancer Research

ISSN: 1756-9966 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://jeccr.biomedcentral.com/

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