BRAF Mutations and Dysregulation of the MAP Kinase Pathway Associated to Sinonasal Mucosal Melanomas.

Maria Colombino,Maria Sini,Amelia Lissia,Antonella Manca,Paolo Ascierto,Panagiotis Paliogiannis,Gianmaria Miolo,Maria Fedeli,Antonio Cossu,Giuseppe Palmieri,Davide Santeufemia,Valentina Doneddu,Marina Pisano,Grazia Palomba,Milena Casula,Valli De Re,Filippo Fraggetta,Gerardo Botti,Giosuè Scognamiglio

doi:10.3390/jcm8101577

Abstract

Sinonasal mucosal melanoma (SNM) is a rare and aggressive type of melanoma, and because of this, we currently have a limited understanding of its genetic and molecular constitution. The incidence among SNMs of somatic mutations in the genes involved in the main molecular pathways, which have been largely associated with cutaneous melanoma, is not yet fully understood. Through a next-generation sequencing (NGS) approach using a panel of 25 genes involved in melanoma pathogenesis customized by our group, we performed a mutation analysis in a cohort of 25 SNM patients. Results showed that pathogenic mutations were found in more than 60% of SNM cases at a somatic level, with strikingly 32% of them carrying deleterious mutations in the BRAF gene. The identified mutations mostly lack the typical UV signature associated with cutaneous melanomas and showed no significant association with any histopathological parameter. Oncogenic activation of the BRAF-depending pathway, which may induce immune tolerance into the tumour microenvironment (i.e., by increasing the VEGF production) was poorly associated with mutations in genes that have been related to diminished clinical benefit of the treatment with BRAF inhibitors. Screening for mutations in BRAF and other MAPK genes should be included in the routine diagnostic test for a better classification of SNM patients.

Highlights

Melanomas are malignant tumours that develop from melanocytes
To increase the understanding of the prevalence and spectrum of mutations in an infrequent subtype of mucosal melanoma, we analyse next-generation sequencing (NGS) data from 25 primary sinonasal tract mucosal melanomas, and we report several somatic mutations which may be useful to make routinely applicable for the diagnostic use in Sinonasal mucosal melanoma (SNM)
A total of 29 patients with ascertained diagnosis of sinonasal mucosal melanoma were identified through a multicentre retrospective study

Summary

Introduction

Melanomas are malignant tumours that develop from melanocytes. Cutaneous melanomas are the most common type, but such a malignancy can arise in any organ containing melanocytes (e.g., eye, nose, mouth) [1,2,3]. The most common symptoms are nasal obstruction and epistaxis, symptomatology can develop late or be non-specific, delaying correct diagnosis and resulting in poorer prognosis [4]. It is one of the most common mucosal melanomas (41% of them) and comprises 1% of all melanomas [5,6]. The risk of local recurrence and metastasis are between 31%–85% and 25%–50%, respectively [9,10]

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Conclusion