Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients

E. Miele; S. Rossi; A. Stracuzzi; S. Patrizi; S. Barresi; M. Cajozzo; L. Pedace; I. Giovannoni; F. Dell'Otto; A. Diociaiuti; F. Grussu; F. Vinciarelli; A. Crocoli; A. Castellano; M. C. Garganese; Angela Mastronuzzi; Franco Locatelli; R. Alaggio; M. E. Hachem; M. Zama; Pasquale M. D. De

doi:10.1007/s12672-025-03965-3

Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients

E. Miele^*
, S. Rossi
, A. Stracuzzi
, S. Patrizi
, S. Barresi
, M. Cajozzo
, L. Pedace
, I. Giovannoni
, F. Dell'Otto
, A. Diociaiuti
, F. Grussu
, F. Vinciarelli
, A. Crocoli
, A. Castellano
, M. C. Garganese
, Angela Mastronuzzi
, Franco Locatelli
, R. Alaggio
, M. E. Hachem
, M. Zama

Pasquale M. D. De

^*Autore corrispondente per questo lavoro

IRCCS Ospedale pediatrico Bambino Gesù - Roma
Sapienza University

Risultato della ricerca: Contributo in rivista › Articolo

Abstract

Background: Congenital giant melanocytic nevi (CGMN) are rare melanocytic proliferations present at birth, associated with an increased risk of pediatric malignant melanoma (MM). Melanomas arising within CGMN are uncommon but clinically aggressive, with diagnostic challenges due to overlapping histopathological features with benign proliferations. This case series explores the clinicopathologic, molecular, and therapeutic profiles of three pediatric patients with MM arising in CGMN. Methods: An integrated analysis—including histopathology, immunohistochemistry, mutational profiling (NRAS, BRAF, PRKAR1A), copy number variation (CNV) analysis, and DNA methylation profiling using the classifier developed at the German Cancer Research Center (DFKZ) in Heidelberg—was performed on tumor and matched nevus samples. Results: All tumors harbored MAPK pathway alterations, including NRAS Q61 mutations or BRAF fusions. DNA methylation profiling confirmed malignant transformation, while matched nevi clustered as melanocytoma with flat CNV profiles. Immunotherapy with checkpoint inhibitors (nivolumab ± ipilimumab) was used in all cases despite low PD-1/PD-L1 expression. However, therapeutic response was inconsistent, and two patients developed severe immune-related hepatitis requiring treatment discontinuation. Only one patient remains in remission. Epigenomic analyses revealed that benign and malignant components shared a close clustering pattern, suggesting a common cellular origin and patient-specific epigenetic imprinting. Conclusion: MM arising within CGMN poses diagnostic and therapeutic challenges. While molecular and epigenomic profiling supports accurate classification and understanding of disease biology, the role of immunotherapy remains uncertain—marked by reduced efficacy and significant immune-related toxicity. A multidisciplinary approach is essential to guide management and improve outcomes in this rare pediatric malignancy.

Lingua originale	Inglese
pagine (da-a)	1-12
Numero di pagine	12
Rivista	Hormones and Cancer
Volume	16
Numero di pubblicazione	1
DOI	https://doi.org/10.1007/s12672-025-03965-3
Stato di pubblicazione	Pubblicato - 2025

OSS delle Nazioni Unite

Questo processo contribuisce al raggiungimento dei seguenti obiettivi di sviluppo sostenibile

SDG 3 Salute e benessere

All Science Journal Classification (ASJC) codes

Endocrinologia, Diabete e Metabolismo
Oncologia
Endocrinologia
Sistema Endocrino e Autonomo
Ricerca sul Cancro

Keywords

BRAF fusion
CNV
Case report
Congenital giant melanocytic nevus
DNA methylation profiling
Immune checkpoint inhibitors
NRAS mutation
Pediatric melanoma

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10.1007/s12672-025-03965-3

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Miele, E., Rossi, S., Stracuzzi, A., Patrizi, S., Barresi, S., Cajozzo, M., Pedace, L., Giovannoni, I., Dell'Otto, F., Diociaiuti, A., Grussu, F., Vinciarelli, F., Crocoli, A., Castellano, A., Garganese, M. C., Mastronuzzi, A., Locatelli, F., Alaggio, R., Hachem, M. E., ... De, P. M. D. (2025). Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients. Hormones and Cancer, 16(1), 1-12. https://doi.org/10.1007/s12672-025-03965-3

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title = "Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients",

abstract = "Background: Congenital giant melanocytic nevi (CGMN) are rare melanocytic proliferations present at birth, associated with an increased risk of pediatric malignant melanoma (MM). Melanomas arising within CGMN are uncommon but clinically aggressive, with diagnostic challenges due to overlapping histopathological features with benign proliferations. This case series explores the clinicopathologic, molecular, and therapeutic profiles of three pediatric patients with MM arising in CGMN. Methods: An integrated analysis—including histopathology, immunohistochemistry, mutational profiling (NRAS, BRAF, PRKAR1A), copy number variation (CNV) analysis, and DNA methylation profiling using the classifier developed at the German Cancer Research Center (DFKZ) in Heidelberg—was performed on tumor and matched nevus samples. Results: All tumors harbored MAPK pathway alterations, including NRAS Q61 mutations or BRAF fusions. DNA methylation profiling confirmed malignant transformation, while matched nevi clustered as melanocytoma with flat CNV profiles. Immunotherapy with checkpoint inhibitors (nivolumab ± ipilimumab) was used in all cases despite low PD-1/PD-L1 expression. However, therapeutic response was inconsistent, and two patients developed severe immune-related hepatitis requiring treatment discontinuation. Only one patient remains in remission. Epigenomic analyses revealed that benign and malignant components shared a close clustering pattern, suggesting a common cellular origin and patient-specific epigenetic imprinting. Conclusion: MM arising within CGMN poses diagnostic and therapeutic challenges. While molecular and epigenomic profiling supports accurate classification and understanding of disease biology, the role of immunotherapy remains uncertain—marked by reduced efficacy and significant immune-related toxicity. A multidisciplinary approach is essential to guide management and improve outcomes in this rare pediatric malignancy.",

keywords = "BRAF fusion, CNV, Case report, Congenital giant melanocytic nevus, DNA methylation profiling, Immune checkpoint inhibitors, NRAS mutation, Pediatric melanoma, BRAF fusion, CNV, Case report, Congenital giant melanocytic nevus, DNA methylation profiling, Immune checkpoint inhibitors, NRAS mutation, Pediatric melanoma",

author = "E. Miele and S. Rossi and A. Stracuzzi and S. Patrizi and S. Barresi and M. Cajozzo and L. Pedace and I. Giovannoni and F. Dell'Otto and A. Diociaiuti and F. Grussu and F. Vinciarelli and A. Crocoli and A. Castellano and Garganese, \{M. C.\} and Angela Mastronuzzi and Franco Locatelli and R. Alaggio and Hachem, \{M. E.\} and M. Zama and De, \{Pasquale M. D.\}",

year = "2025",

doi = "10.1007/s12672-025-03965-3",

language = "English",

volume = "16",

pages = "1--12",

journal = "Hormones and Cancer",

issn = "1868-8497",

number = "1",

}

Miele, E, Rossi, S, Stracuzzi, A, Patrizi, S, Barresi, S, Cajozzo, M, Pedace, L, Giovannoni, I, Dell'Otto, F, Diociaiuti, A, Grussu, F, Vinciarelli, F, Crocoli, A, Castellano, A, Garganese, MC, Mastronuzzi, A , Locatelli, F, Alaggio, R, Hachem, ME, Zama, M & De, PMD 2025, 'Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients', Hormones and Cancer, vol. 16, n. 1, pagg. 1-12. https://doi.org/10.1007/s12672-025-03965-3

TY - JOUR

T1 - Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients

AU - Miele, E.

AU - Rossi, S.

AU - Stracuzzi, A.

AU - Patrizi, S.

AU - Barresi, S.

AU - Cajozzo, M.

AU - Pedace, L.

AU - Giovannoni, I.

AU - Dell'Otto, F.

AU - Diociaiuti, A.

AU - Grussu, F.

AU - Vinciarelli, F.

AU - Crocoli, A.

AU - Castellano, A.

AU - Garganese, M. C.

AU - Mastronuzzi, Angela

AU - Locatelli, Franco

AU - Alaggio, R.

AU - Hachem, M. E.

AU - Zama, M.

AU - De, Pasquale M. D.

PY - 2025

Y1 - 2025

N2 - Background: Congenital giant melanocytic nevi (CGMN) are rare melanocytic proliferations present at birth, associated with an increased risk of pediatric malignant melanoma (MM). Melanomas arising within CGMN are uncommon but clinically aggressive, with diagnostic challenges due to overlapping histopathological features with benign proliferations. This case series explores the clinicopathologic, molecular, and therapeutic profiles of three pediatric patients with MM arising in CGMN. Methods: An integrated analysis—including histopathology, immunohistochemistry, mutational profiling (NRAS, BRAF, PRKAR1A), copy number variation (CNV) analysis, and DNA methylation profiling using the classifier developed at the German Cancer Research Center (DFKZ) in Heidelberg—was performed on tumor and matched nevus samples. Results: All tumors harbored MAPK pathway alterations, including NRAS Q61 mutations or BRAF fusions. DNA methylation profiling confirmed malignant transformation, while matched nevi clustered as melanocytoma with flat CNV profiles. Immunotherapy with checkpoint inhibitors (nivolumab ± ipilimumab) was used in all cases despite low PD-1/PD-L1 expression. However, therapeutic response was inconsistent, and two patients developed severe immune-related hepatitis requiring treatment discontinuation. Only one patient remains in remission. Epigenomic analyses revealed that benign and malignant components shared a close clustering pattern, suggesting a common cellular origin and patient-specific epigenetic imprinting. Conclusion: MM arising within CGMN poses diagnostic and therapeutic challenges. While molecular and epigenomic profiling supports accurate classification and understanding of disease biology, the role of immunotherapy remains uncertain—marked by reduced efficacy and significant immune-related toxicity. A multidisciplinary approach is essential to guide management and improve outcomes in this rare pediatric malignancy.

AB - Background: Congenital giant melanocytic nevi (CGMN) are rare melanocytic proliferations present at birth, associated with an increased risk of pediatric malignant melanoma (MM). Melanomas arising within CGMN are uncommon but clinically aggressive, with diagnostic challenges due to overlapping histopathological features with benign proliferations. This case series explores the clinicopathologic, molecular, and therapeutic profiles of three pediatric patients with MM arising in CGMN. Methods: An integrated analysis—including histopathology, immunohistochemistry, mutational profiling (NRAS, BRAF, PRKAR1A), copy number variation (CNV) analysis, and DNA methylation profiling using the classifier developed at the German Cancer Research Center (DFKZ) in Heidelberg—was performed on tumor and matched nevus samples. Results: All tumors harbored MAPK pathway alterations, including NRAS Q61 mutations or BRAF fusions. DNA methylation profiling confirmed malignant transformation, while matched nevi clustered as melanocytoma with flat CNV profiles. Immunotherapy with checkpoint inhibitors (nivolumab ± ipilimumab) was used in all cases despite low PD-1/PD-L1 expression. However, therapeutic response was inconsistent, and two patients developed severe immune-related hepatitis requiring treatment discontinuation. Only one patient remains in remission. Epigenomic analyses revealed that benign and malignant components shared a close clustering pattern, suggesting a common cellular origin and patient-specific epigenetic imprinting. Conclusion: MM arising within CGMN poses diagnostic and therapeutic challenges. While molecular and epigenomic profiling supports accurate classification and understanding of disease biology, the role of immunotherapy remains uncertain—marked by reduced efficacy and significant immune-related toxicity. A multidisciplinary approach is essential to guide management and improve outcomes in this rare pediatric malignancy.

KW - BRAF fusion

KW - CNV

KW - Case report

KW - Congenital giant melanocytic nevus

KW - DNA methylation profiling

KW - Immune checkpoint inhibitors

KW - NRAS mutation

KW - Pediatric melanoma

KW - BRAF fusion

KW - CNV

KW - Case report

KW - Congenital giant melanocytic nevus

KW - DNA methylation profiling

KW - Immune checkpoint inhibitors

KW - NRAS mutation

KW - Pediatric melanoma

UR - https://publicatt.unicatt.it/handle/10807/330101

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UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=105022872371&origin=inward

U2 - 10.1007/s12672-025-03965-3

DO - 10.1007/s12672-025-03965-3

M3 - Article

SN - 1868-8497

VL - 16

SP - 1

EP - 12

JO - Hormones and Cancer

JF - Hormones and Cancer

IS - 1

ER -

Epigenomic characterization and therapeutic challenges of melanoma arising in giant nevi in pediatric patients

Abstract

OSS delle Nazioni Unite

All Science Journal Classification (ASJC) codes

Keywords

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