AUTHOR=Forschner Andrea , Sinnberg Tobias , Mroz Gabi , Schroeder Christopher , Reinert Christian Philipp , Gatidis Sergios , Bitzer Michael , Eigentler Thomas , Garbe Claus , Niessner Heike , Röcken Martin , Roggia Cristiana , Armeanu-Ebinger Sorin , Riess Olaf , Mattern Sven , Nann Dominik , Bonzheim Irina 

TITLE=Case Report: Combined CDK4/6 and MEK Inhibition in Refractory CDKN2A and NRAS Mutant Melanoma

JOURNAL=Frontiers in Oncology

VOLUME=11

YEAR=2021

URL=https://www.frontiersin.org/journals/oncology/articles/10.3389/fonc.2021.643156

DOI=10.3389/fonc.2021.643156

ISSN=2234-943X

ABSTRACT=<p>There are only limited treatment options for metastatic <italic>NRAS</italic> mutant melanoma patients with resistance to immune checkpoint inhibitors. Besides activation of the mitogen-activated protein (MAP) kinase pathway, they often have additional disturbances in cell cycle regulation. However, unlike <italic>BRAF</italic> mutant melanoma, no targeted therapy has yet been approved for <italic>NRAS</italic> mutant melanoma so far. Here we present a <italic>NRAS</italic> mutant melanoma patient with response to combined binimetinib and ribociclib therapy following characterization of the molecular defects of the tumor by panel sequencing. Next generation sequencing (708 cancer genes) of a soft tissue metastasis revealed a homozygous deletion of <italic>CDKN2A</italic> in addition to the previously known <italic>NRAS</italic> mutation, as well as amplification of <italic>CCNE1</italic> and <italic>CDK6.</italic> Immunohistochemical staining of the altered cell cycle genes confirmed loss of p16, reduced expression of p21 and high expression of CDK6 and cyclin D1. As the patient had been progressive on combined immunotherapy, targeted therapy with combined MEK and CDK4/6 inhibition was initiated as recommended by the molecular tumor board. Response to treatment was monitored with PET/CT and liquid biopsy, serum LDH, and S100. In addition, a patient-derived xenograft (PDX) was used to prove the efficacy of the two drugs in combination. Furthermore, senescence-associated beta-galactosidase staining showed that more cells were senescent under the combination treatment of binimetinib and ribociclib. Our case demonstrates how an individualized, molecular-based therapeutic approach could be found based on next-generation sequencing results. Furthermore our report highlights the fruitful and efficient collaboration of dermatooncologists, human geneticists, molecular pathologists, biochemists, radiologists, and nuclear physicians. Further studies are urgently needed to expand the very limited therapeutic landscape of <italic>NRAS</italic> mutated melanoma.</p>