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Evolutionary processes of melanomas from giant congenital melanocytic nevi.

Young-Kyoung LimHyun-Tae ShinYoung Hwan ChoiDong-Youn Lee
Published in: Pigment cell & melanoma research (2019)
Melanoma can develop in a congenital melanocytic nevus (CMN). In fact, a large CMN is associated with a high risk of developing melanoma. Although melanomas arising from CMNs are thought to have a pathogenesis distinct from conventional melanomas, no studies have been conducted on the evolution or tumor heterogeneity of CMN melanomas. We applied multi-region whole-exome sequencing to investigate the clonal nature of driver events and evolutionary processes in CMNs and melanomas arising from CMNs. In two patients, we observed an independent subclonal evolution in cancerized fields of CMNs and chromosome 8q amplification in both melanomas arising from CMNs. The amplification of MYC, located in chromosome 8q, was correlated with the percentage of tumor cells expressing high levels of MYC protein detected in melanoma cells by immunohistochemistry. Our analysis suggests that each CMN cell may evolve sporadically and that amplification of MYC might be a key event for melanoma development in CMNs.
Keyphrases
  • nucleic acid
  • single cell
  • transcription factor
  • ejection fraction
  • newly diagnosed
  • genome wide
  • copy number
  • stem cells
  • gene expression
  • dna methylation
  • label free
  • mesenchymal stem cells
  • small molecule
  • protein protein