Skip to Content
Merck
  • DIPG harbour alterations targetable by MEK inhibitors, with acquired resistance mechanisms overcome by combinatorial inhibition.

DIPG harbour alterations targetable by MEK inhibitors, with acquired resistance mechanisms overcome by combinatorial inhibition.

Cancer discovery (2021-11-06)
Elisa Izquierdo, Diana M Carvalho, Alan Mackay, Sara Temelso, Jessica Kr Boult, Giulia Pericoli, Elisabet Fernandez, Molina Das, Valeria Molinari, Yura Grabovska, Rebecca F Rogers, Maria Antonietta Ajmone-Cat, Paula Z Proszek, Mark Stubbs, Sarita Depani, Patricia O'Hare, Lu Yu, Georgia Roumelioti, Jyoti S Choudhary, Matthew Clarke, Amy R Fairchild, Thomas S Jacques, Richard G Grundy, Lisa Howell, Susan Picton, Jenny Adamski, Shaun Wilson, Juliet C Gray, Bassel Zebian, Lynley V Marshall, Fernando Carceller, Jacques Grill, Maria Vinci, Simon P Robinson, Michael Hubank, Darren Hargrave, Chris Jones
ABSTRACT

The survival of children with DIPG remains dismal, with new treatments desperately needed. In a prospective biopsy-stratified clinical trial, we combined detailed molecular profiling and drug screening in newly-established patient-derived models in vitro and in vivo. We identified in vitro sensitivity to MEK inhibitors in DIPGs harbouring MAPK pathway alterations, however treatment of PDX models and a patient at relapse failed to elicit a significant response. We generated trametinib-resistant clones in a BRAF_G469V model through continuous drug exposure, and identified acquired mutations in MEK1/2 with sustained pathway up-regulation. These cells showed hallmarks of mesenchymal transition, and expression signatures overlapping with inherently trametinib-insensitive patient-derived cells, predicting sensitivity to dasatinib. Combined trametinib and dasatinib showed highly synergistic effects in vitro and on ex vivo brain slices. We highlight the MAPK pathway as a therapeutic target in DIPG, and show the importance of parallel resistance modelling and combinatorial treatments for meaningful clinical translation.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
Phosphatase Inhibitor Cocktail 2, aqueous solution (dark coloration may develop upon storage, which does not affect the activity)
Roche
cOmplete, Mini Protease Inhibitor Cocktail, Tablets provided in a glass vial
Sigma-Aldrich
Dimethyl sulfoxide, Hybri-Max, sterile-filtered, BioReagent, suitable for hybridoma, ≥99.7%
Sigma-Aldrich
Anti-Nuclei Antibody, clone 3E1.3, clone 3E1.3, Chemicon®, from mouse