The utility of DNA methylation profiling in the diagnosis of un‐, de‐ and trans‐differentiated melanoma: a series of 11 cases

Author:

Erdem Zeynep Betul1ORCID,Ameline Baptiste2ORCID,Bovée Judith V M G1ORCID,van Boven Hester3,Baumhoer Daniel24ORCID,Chrisinger John S A5ORCID,Fritchie Karen J6ORCID

Affiliation:

1. Department of Pathology Leiden University Medical Center Leiden the Netherlands

2. Bone Tumor Reference Center at the Institute of Pathology University Hospital Basel and University of Basel Basel Switzerland

3. Department of Pathology Netherlands Cancer Institute‐Antoni van Leeuwenhoek Hospital Amsterdam the Netherlands

4. Basel Research Centre for Child Health Basel Switzerland

5. Department of Pathology and Immunology, Division of Anatomic and Molecular Pathology Washington University School of Medicine St Louis MO USA

6. Department of Anatomic Pathology Cleveland Clinic Cleveland OH USA

Abstract

AimsMelanomas are recognised for their remarkable morphological plasticity. Some tumours may lose conventional features and/or acquire non‐melanocytic characteristics, referred to as undifferentiated, dedifferentiated and transdifferentiated melanoma. Despite this phenotypical variability, melanomas typically maintain their cancer driver aberrations, affecting genes such as BRAF, NRAS and NF1. Currently, little is known about whether the DNA methylation profile follows the loss or change of differentiation or is retained despite extensive morphological transformation.Methods and resultsIn this study we analysed 11 melanoma cases, comprising six males and five females, with a median age of 67 years, including five undifferentiated, four trans‐differentiated and two de‐differentiated melanomas. Undifferentiated and trans‐differentiated tumours either arose in a patient with known melanoma and/or presented in the groin/axilla with molecular alterations consistent with melanoma. Cases with heterologous differentiation resembled chondrosarcoma, osteosarcoma, angiosarcoma and rhabdomyosarcoma both morphologically and immunohistochemically, while undifferentiated tumours resembled undifferentiated pleomorphic sarcoma. Methylome profiling was performed, and unsupervised clustering analysis revealed nine cases (five undifferentiated, three trans‐differentiated and one de‐differentiated) to cluster closely together with conventional melanomas from a reference set. Two cases clustered separately with a distinct group of conventional melanomas exhibiting H3K27me3 loss.ConclusionsDespite loss of differentiation and phenotypical plasticity, methylation patterns seem to be retained in undifferentiated, de‐differentiated and trans‐differentiated melanomas and represent useful diagnostic tools to enhance diagnostic precision in these diagnostically challenging cases.

Publisher

Wiley

Reference29 articles.

1. Morphological and immunophenotypic variations in malignant melanoma

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3. The clinicopathologic spectrum and genomic landscape of de‐/trans‐differentiated melanoma;Ingrid F;Mod. Pathol.,2021

4. A case of dedifferentiated melanoma with lymph node metastasis where molecular biological tests were useful for diagnosis;Kamata M;Cureus,2022

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