Defining the Criteria for Reflex Testing for BRAF Mutations in Cutaneous Melanoma Patients

Author:

Zhou SarahORCID,Sikorski Daniel,Xu Honghao,Zubarev Andrei,Chergui May,Lagacé FrançoisORCID,Miller Wilson H.,Redpath Margaret,Ghazal Stephanie,Butler Marcus O.ORCID,Petrella Teresa M.,Claveau Joël,Nessim CarolynORCID,Salopek Thomas G.ORCID,Gniadecki Robert,Litvinov Ivan V.ORCID

Abstract

Targeted therapy has been developed through an in-depth understanding of molecular pathways involved in the pathogenesis of melanoma. Approximately ~50% of patients with melanoma have tumors that harbor a mutation of the BRAF oncogene. Certain clinical features have been identified in BRAF-mutated melanomas (primary lesions located on the trunk, diagnosed in patients <50, visibly pigmented tumors and, at times, with ulceration or specific dermatoscopic features). While BRAF mutation testing is recommended for stage III–IV melanoma, guidelines differ in recommending mutation testing in stage II melanoma patients. To fully benefit from these treatment options and avoid delays in therapy initiation, advanced melanoma patients harboring a BRAF mutation must be identified accurately and quickly. To achieve this, clear definition and implementation of BRAF reflex testing criteria/methods in melanoma should be established so that patients with advanced melanoma can arrive to their first medical oncology appointment with a known biomarker status. Reflex testing has proven effective for a variety of cancers in selecting therapies and driving other medical decisions. We overview the pathophysiology, clinical presentation of BRAF-mutated melanoma, current guidelines, and present recommendations on BRAF mutation testing. We propose that reflex BRAF testing should be performed for every melanoma patient with stages ≥IIB.

Funder

Cancer Research Society

Canadian Dermatology Foundation

Canadian Institutes for Health Research

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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