PARP Inhibition Increases the Response to Chemotherapy in Uveal Melanoma

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

doi:10.3390/cancers11060751

Cancers (May 2019)

PARP Inhibition Increases the Response to Chemotherapy in Uveal Melanoma

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

Affiliations

Leanne de Koning: RPPA Platform, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Didier Decaudin: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Rania El Botty: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
André Nicolas: Department of Tumor Biology, Institut Curie, 75248 Paris, France
Guillaume Carita: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Mathieu Schuller: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Bérengère Ouine: RPPA Platform, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Aurélie Cartier: RPPA Platform, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Adnan Naguez: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Justine Fleury: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Vesselina Cooke: Novartis Institutes for BioMedical Research, Translational Clinical Oncology, Cambridge, MA 02139, USA
Andrew Wylie: Novartis Institutes for BioMedical Research, Translational Clinical Oncology, Cambridge, MA 02139, USA
Paul Smith: Oncology IMED, AstraZeneca, 1 Francis Crick Avenue, Cambridge Biomedical Campus, Cambridge CB2 0AA, UK
Elisabetta Marangoni: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
David Gentien: Genomics Platform, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Didier Meseure: Department of Tumor Biology, Institut Curie, 75248 Paris, France
Pascale Mariani: Department of Surgery, Institut Curie, 75248 Paris, France
Nathalie Cassoux: Department of Ophthalmologic Surgery, Institut Curie, University of Medicine René Descartes Paris V, 75248 Paris, France
Sophie Piperno-Neumann: Department of Medical Oncology, Institut Curie, 75248 Paris, France
Sergio Roman-Roman: Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France
Fariba Némati: Laboratory of Preclinical Investigation, Department of Translational Research, Institut Curie, PSL University, 75248 Paris, France

DOI: https://doi.org/10.3390/cancers11060751
Journal volume & issue: Vol. 11, no. 6
p. 751

Abstract

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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.

Published in Cancers

ISSN: 2072-6694 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://www.mdpi.com/journal/cancers/

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