AUTHOR=Ferrara Gerardo , Argenziano Giuseppe 

TITLE=The WHO 2018 Classification of Cutaneous Melanocytic Neoplasms: Suggestions From Routine Practice

JOURNAL=Frontiers in Oncology

VOLUME=11

YEAR=2021

URL=https://www.frontiersin.org/journals/oncology/articles/10.3389/fonc.2021.675296

DOI=10.3389/fonc.2021.675296

ISSN=2234-943X

ABSTRACT=<p>The “multidimensional” World Health Organization (WHO) classification 2018 of melanocytic tumors encompasses nine melanoma pathways (seven of which for cutaneous melanoma) according to a progression model in which morphologically intermediate melanocytic tumors are cosidered as simulators and/or precursors to melanoma. These “intermediates” can be subclassified into: i) a “classical” subgroup (superficial/thin compound: dysplastic nevus), which is placed within the morphologic and molecular progression spectrum of classical (Clark’s and McGovern’s) melanoma subtypes (superficial spreading and, possibly, nodular); and ii) a “non-classical” subgroup (thick compound/dermal: “melanocytomas”) whose genetic pathways diverge from classical melanoma subtypes. Such a progression model is aimed at giving a conceptual framework for a histopathological classification; however, routine clinicopathological practice strongly suggests that most melanomas arise <italic>de novo</italic> and that the vast majority of nevi are clinically stable or even involuting over time. Clinicopathological correlation can help identify some severely atypical but benign tumors (<italic>e.g.</italic>: sclerosing nevus with pseudomelanomatous features) as well as some deceptively bland melanomas (<italic>e.g.</italic>: lentiginous melanoma; nested melanoma), thereby addressing some ambiguous cases to a correct clinical management. The recently available adjuvant therapy regimens for melanoma raise the problem of a careful distinction between severely atypical (high grade) melanocytoma and “classical” melanoma: conventional morphology can guide an algorithmic approach based on an antibody panel (anti-mutated BRAF, BAP1, PRAME, ALK, TRKA, MET, HRAS-WT, ROS; beta catenin; R1alpha; p16; HMB45; Ki67), a first-line molecular study (identification of hot spot mutations of <italic>BRAF</italic> and <italic>NRAS</italic>) and an advanced molecular study (sequencing of <italic>NF1, KIT, BRAF, MAP2K1, GNAQ, GNA11, PLCB4, CYSLTR2, HRAS</italic>; fusions studies of <italic>BRAF, RET, MAP3K8, PRKCA</italic>); as a final step, next-generation sequencing can identify melanocytic tumors with rare genetic signatures and melanocytic tumors with a high tumor mutation burden which should be definitely ascribed to the category of classical melanoma with the respective therapeutic options.</p>