A prospective, comprehensive registry that integrates the molecular analysis of pediatric and adolescent melanocytic lesions

Pappo, Alberto S.; McPherson, Valerie; Pan, Haitao; Wang, Fang; Wang, Lu; Wright, Teresa S.; Hussong, Margaret; Hawkins, Dana; Kaste, Sue C.; Davidoff, Andrew M.; Bahrami, Armita

doi:10.1002/cncr.33750

Cited by 20 publications

(22 citation statements)

References 25 publications

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“…6,7 Childhood and adolescent melanomas, characterized by a high mutation burden, likely represent distinct biologic/genetic entities with variable prognosis. 6,8 The heightened risk for SPM within the first year of initial primary CM diagnosis aligns with previous studies. 3 This is likely due to congenital melanocytic nevi or underlying genetic predisposition, 7,8 underscoring the importance of diligent skin surveillance during this critical period.…”

Section: Discussionsupporting

confidence: 85%

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Risk for second primary cancers among pediatric and young adult melanoma survivors

Luu,

Han,

Agarwal

et al. 2023

Pediatric Dermatology

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Background/ObjectivesSecond primary cancers (SPCs) are a leading cause of morbidity and mortality among cancer survivors. In this study, we aimed to characterize the incidence of SPCs among pediatric and young adult survivors of CM.MethodsUsing the Surveillance, Epidemiology, and End Results Program data spanning 2000–2018, we calculated standardized incidence ratios (SIR) to assess SPC risk in all pediatric (0–18 years) and young adult (19–29 years) patients with a first primary cancer diagnosis of CM.ResultsOf 7,169 total CM survivors, 632 (8.82%) developed a SPC, corresponding to a 5‐fold increased risk (standardized incidence ratio [SIR] 4.98; 95% confidence interval [CI] 4.60–5.38) compared to the general population. There was a highly elevated risk for second primary melanoma across all age groups (SIR 32.5; 95% CI 29.7–35.6), constituting the majority of SPC diagnoses (N = 485). Infants diagnosed with CM before 1 year of age had the highest risk for any SPC (SIR 164; 95% CI 19.8–592) and young adults diagnosed at 25–29 years had the lowest risk (SIR 4.64; 95% CI 4.19–5.13). SPC incidence was highest within the first year of CM diagnosis (SIR 27.5; 95% CI 23.7–31.6) and progressively decreased with time.ConclusionsVariation exists in the incidence and type of SPC according to age among pediatric and young adult survivors of CM.

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Section: Discussionsupporting

confidence: 85%

“…6,8 The heightened risk for SPM within the first year of initial primary CM diagnosis aligns with previous studies. 3 This is likely due to congenital melanocytic nevi or underlying genetic predisposition, 7,8 underscoring the importance of diligent skin surveillance during this critical period.…”

Section: Discussionsupporting

confidence: 85%

Risk for second primary cancers among pediatric and young adult melanoma survivors

Luu,

Han,

Agarwal

et al. 2023

Pediatric Dermatology

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“…Breslow thickness, dermal mitotic activity, and epidermal ulceration are to be assessed. A BRAF.pV600E mutation is frequently present (>80%) both in the melanoma and the nevus from which it arose [4,[6][7][8]. The need for an oncogenetic consultation must be evaluated according to the clinical setting.…”

Section: Superficial Spreading Melanoma (Ssm)mentioning

confidence: 99%

“…These include HRAS mutations, receptor tyrosine kinase fusions, and serine-threonine kinase mutations and fusions, described in Table 1. For benign cases, the most common fusions involve NTRK1/3, ALK1, and ROS1, whereas MAP3K8 and ALK1 predominate in atypical and malignant Spitz tumors [6]. Histologically, Spitz nevi are symmetrical compound lesions with either a pediculated or elevated silhouette.…”

Section: Malignant Spitz Tumor (Melanoma With a Spitzoid Morphology And Specific Genetic Features)mentioning

confidence: 99%

Cutaneous Melanomas Arising during Childhood: An Overview of the Main Entities

et al. 2021

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Cutaneous melanomas are exceptional in children and represent a variety of clinical situations, each with a different prognosis. In congenital nevi, the risk of transformation is correlated with the size of the nevus. The most frequent type is lateral transformation, extremely rare before puberty, reminiscent of a superficial spreading melanoma (SSM) ex-nevus. Deep nodular transformation is much rarer, can occur before puberty, and must be distinguished from benign proliferative nodules. Superficial spreading melanoma can also arise within small nevi, which were not visible at birth, usually after puberty, and can reveal a cancer predisposition syndrome (CDKN2A or CDK4 germline mutations). Prognosis is correlated with classical histoprognostic features (mainly Breslow thickness). Spitz tumors are frequent in adolescents and encompass benign (Spitz nevus), intermediate (atypical Spitz tumor), and malignant forms (malignant Spitz tumor). The whole spectrum is characterized by specific morphology with spindled and epithelioid cells, genetic features, and an overall favorable outcome even if a regional lymph node is involved. Nevoid melanomas are rare and difficult to diagnose clinically and histologically. They can arise in late adolescence. Their prognosis is currently not very well ascertained. A small group of melanomas remains unclassified after histological and molecular assessment.

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“…Neither study compared melanoma genetics to that of ASTs. A 2021 study of 70 pediatric melanomas highlights the advancements in our understanding of genomic alterations for distinct clinical presentations of melanomas; in this study, the ASTs and Spitz melanomas are considered together 13 . Our study focused on the challenges of distinguishing AST from melanoma, and presents a genomic comparison of MM and ASTs in the pediatric patients in the context of comprehensive clinical annotation.…”

Section: Introductionmentioning

confidence: 99%

Genomic comparison of malignant melanoma and atypical Spitz tumor in the pediatric population

Church

Moustafa

Pinches

et al. 2022

Pediatric Dermatology

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A prospective, comprehensive registry that integrates the molecular analysis of pediatric and adolescent melanocytic lesions

Cited by 20 publications

References 25 publications

Risk for second primary cancers among pediatric and young adult melanoma survivors

Risk for second primary cancers among pediatric and young adult melanoma survivors

Cutaneous Melanomas Arising during Childhood: An Overview of the Main Entities

Genomic comparison of malignant melanoma and atypical Spitz tumor in the pediatric population

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