Clinical outcome of concomitant vs interrupted BRAF inhibitor therapy during radiotherapy in melanoma patients

6533b86ffe1ef96bd12cdfea

RESEARCH PRODUCT

Clinical outcome of concomitant vs interrupted BRAF inhibitor therapy during radiotherapy in melanoma patients

Carsten Weishaupt Michael Geier Andrea Forschner Friedegund Meier Ursula Dietrich Jessica C. Hassel Patrick Clemens Markus Hecht Stephan Grabbe Ralf Gutzmer Bülent Polat Ricarda Rauschenberg Carmen Loquai Rainer Fietkau Felix Kiecker Lisa Zimmer Carola Berking Dirk Schadendorf (Essen)Simone M. Goldinger Gerhard G. Grabenbauer Luitpold Distel Gerold Schuler Jochen Utikal Jochen Utikal Lucie Heinzerling Panagiotis Balermpas

subject

0301 basic medicine Oncology Male Cancer Research Radiation-Sensitizing Agents Skin Neoplasms medicine.medical_treatment Medizin Cohort Studies 0302 clinical medicine Antineoplastic Combined Chemotherapy Protocols Oximes Vemurafenib Prospective cohort study Melanoma Aged 80 and over Melanoma Imidazoles Middle Aged Treatment Outcome Oncology 030220 oncology & carcinogenesis Female medicine.drug Adult Proto-Oncogene Proteins B-raf medicine.medical_specialty Adolescent Drug Administration Schedule BRAF 03 medical and health sciences Young Adult Internal medicine medicine Humans ddc:610 dabrafenib Protein Kinase Inhibitors radiotherapy Aged Retrospective Studies business.industry Dabrafenib Retrospective cohort study medicine.disease Radiation therapy radiation 030104 developmental biology Vemurafenib Concomitant Clinical Study Skin cancer business

description

Background: Concomitant radiation with BRAF inhibitor (BRAFi) therapy may increase radiation-induced side effects but also potentially improve tumour control in melanoma patients. Methods: A total of 155 patients with BRAF-mutated melanoma from 17 European skin cancer centres were retrospectively analysed. Out of these, 87 patients received concomitant radiotherapy and BRAFi (59 vemurafenib, 28 dabrafenib), while in 68 patients BRAFi therapy was interrupted during radiation (51 vemurafenib, 17 dabrafenib). Overall survival was calculated from the first radiation (OSRT) and from start of BRAFi therapy (OSBRAFi). Results: The median duration of BRAFi treatment interruption prior to radiotherapy was 4 days and lasted for 17 days. Median OSRT and OSBRAFi in the entire cohort were 9.8 and 12.6 months in the interrupted group and 7.3 and 11.5 months in the concomitant group (P=0.075/P=0.217), respectively. Interrupted vemurafenib treatment with a median OSRT and OSBRAFi of 10.1 and 13.1 months, respectively, was superior to concomitant vemurafenib treatment with a median OSRT and OSBRAFi of 6.6 and 10.9 months (P=0.004/P=0.067). Interrupted dabrafenib treatment with a median OSRT and OSBRAFi of 7.7 and 9.8 months, respectively, did not differ from concomitant dabrafenib treatment with a median OSRT and OSBRAFi of 9.9 and 11.6 months (P=0.132/P=0.404). Median local control of the irradiated area did not differ in the interrupted and concomitant BRAFi treatment groups (P=0.619). Skin toxicity of grade ≥2 (CTCAE) was significantly increased in patients with concomitant vemurafenib compared to the group with treatment interruption (P=0.002). Conclusions: Interruption of vemurafenib treatment during radiation was associated with better survival and less toxicity compared to concomitant treatment. Due to lower number of patients, the relevance of treatment interruption in dabrafenib treated patients should be further investigated. The results of this analysis indicate that treatment with the BRAFi vemurafenib should be interrupted during radiotherapy. Prospective studies are desperately needed.

year	journal	country	edition	language
2018-02-13	British Journal of Cancer

10.1038/bjc.2017.489 http://europepmc.org/articles/PMC5886123