PARP Inhibition Increases the Response to Chemotherapy in Uveal Melanoma

Author:

de Koning Leanne,Decaudin Didier,El Botty Rania,Nicolas André,Carita Guillaume,Schuller Mathieu,Ouine Bérengère,Cartier Aurélie,Naguez Adnan,Fleury Justine,Cooke Vesselina,Wylie Andrew,Smith Paul,Marangoni Elisabetta,Gentien DavidORCID,Meseure Didier,Mariani Pascale,Cassoux Nathalie,Piperno-Neumann Sophie,Roman-Roman Sergio,Némati Fariba

Abstract

Uveal melanoma (UM) remains without effective therapy at the metastatic stage, which is associated with BAP-1 (BRCA1 associated protein) mutations. However, no data on DNA repair capacities in UM are available. Here, we use UM patient-derived xenografts (PDXs) to study the therapeutic activity of the PARP inhibitor olaparib, alone or in combination. First, we show that the expression and the activity of PARP proteins is similar between the PDXs and the corresponding patient’s tumors. In vivo experiments in the PDX models showed that olaparib was not efficient alone, but significantly increased the efficacy of dacarbazine. Finally, using reverse phase protein arrays and immunohistochemistry, we identified proteins involved in DNA repair and apoptosis as potential biomarkers predicting response to the combination of olaparib and dacarbazine. We also observed a high increase of phosphorylated YAP and TAZ proteins after dacarbazine + olaparib treatment. Our results suggest that PARP inhibition in combination with the alkylating agent dacarbazine could be of clinical interest for UM treatment. We also observe an interesting effect of dacarbazine on the Hippo pathway, confirming the importance of this pathway in UM.

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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