Background: Melanoma of the sole is an aggressive rare form, often diagnosed late. Plantar atypical nevi (pAN) are frequently misdiagnosed as plantar early melanomas (pEM) and therefore excised. Our aim was to develop a clinical-dermoscopic risk-scoring model to help discriminate these plantar atypical melanocytic lesions (pAMLs). Materials and Methods: We collected 490 pAMLs (98 pEM, 392 pAN) paired with histopathological diagnosis, dermoscopic and clinical image, maximum lesion diameter, plantar location and age and sex of the patient from 17 European centres. This plantar dataset was grouped into training (261), validation (174) and testing (55 pAMLs) subsets. European participants (104 dermatologists, 56 residents) performed a blinded tele-dermoscopic test, including intuitive diagnosis, pattern analysis, rating of case difficulty, diagnostic confidence assessment and management decision. Results: A total of 2887 dermoscopic evaluations were obtained. The iDScore_plantar model gave an average area under the receiver operating characteristic curve of 0.95 (against 0.77 for pattern analysis). It was composed of the sum of five scores (S) for the following items: maximum diameter 8–12 (S = 1)/>12 mm (S = 5); age 40–50 (S = 2)/>50 years (S = 5); location on heel (S4) or on toes/plantar eminence (S = 2); asymmetry of colours (S = 2) and/or asymmetry of structures (S = 1). ‘Long/short follow-up, biopsy, excision’ decisions were matched with four risk ranges: no risk (S = 0–3), low-medium risk (S = 4–8), medium-high risk (S = 9–12) and very high risk (S = 13–17). By applying the model, participants would have reduced the number of misdiagnosed pAN and the number of pAN excised by −25.5% and −27.7%, respectively, and would have increased the number of correctly diagnosed pEM by +18.5%, the number of pEM recommended for surgical excision by +8.5% and the number of pEM recommended directly for surgical excision instead of biopsy by +16.15%. Conclusion: The iDScore_plantar model proved to be a simple scoring tool to help clinicians in assigning a progressive risk of malignancy to pAMLs.
A clinical‐dermoscopic risk scoring model for early melanoma of the soles: The iDScore_plantar / L. Tognetti, S. Lo Conte, S. Leonardelli, A. Lallas, E. Moscarella, R. Giuffrida, J. Paoli, E. Dika, I. Stanganelli, S. Magi, M.C. Fargnoli, C. Longo, G. Nazzaro, P. Broganelli, F. Lacarrubba, M. Suppa, J. Perrot, P. Tschandl, H. Kittler, E. Cinotti, G. Cataldo, G. Cevenini, P. Rubegni, A. Cartocci. - In: JOURNAL OF THE EUROPEAN ACADEMY OF DERMATOLOGY AND VENEREOLOGY. - ISSN 0926-9959. - (2025 May 20). [Epub ahead of print] [10.1111/jdv.20740]
A clinical‐dermoscopic risk scoring model for early melanoma of the soles: The iDScore_plantar
G. Nazzaro;
2025
Abstract
Background: Melanoma of the sole is an aggressive rare form, often diagnosed late. Plantar atypical nevi (pAN) are frequently misdiagnosed as plantar early melanomas (pEM) and therefore excised. Our aim was to develop a clinical-dermoscopic risk-scoring model to help discriminate these plantar atypical melanocytic lesions (pAMLs). Materials and Methods: We collected 490 pAMLs (98 pEM, 392 pAN) paired with histopathological diagnosis, dermoscopic and clinical image, maximum lesion diameter, plantar location and age and sex of the patient from 17 European centres. This plantar dataset was grouped into training (261), validation (174) and testing (55 pAMLs) subsets. European participants (104 dermatologists, 56 residents) performed a blinded tele-dermoscopic test, including intuitive diagnosis, pattern analysis, rating of case difficulty, diagnostic confidence assessment and management decision. Results: A total of 2887 dermoscopic evaluations were obtained. The iDScore_plantar model gave an average area under the receiver operating characteristic curve of 0.95 (against 0.77 for pattern analysis). It was composed of the sum of five scores (S) for the following items: maximum diameter 8–12 (S = 1)/>12 mm (S = 5); age 40–50 (S = 2)/>50 years (S = 5); location on heel (S4) or on toes/plantar eminence (S = 2); asymmetry of colours (S = 2) and/or asymmetry of structures (S = 1). ‘Long/short follow-up, biopsy, excision’ decisions were matched with four risk ranges: no risk (S = 0–3), low-medium risk (S = 4–8), medium-high risk (S = 9–12) and very high risk (S = 13–17). By applying the model, participants would have reduced the number of misdiagnosed pAN and the number of pAN excised by −25.5% and −27.7%, respectively, and would have increased the number of correctly diagnosed pEM by +18.5%, the number of pEM recommended for surgical excision by +8.5% and the number of pEM recommended directly for surgical excision instead of biopsy by +16.15%. Conclusion: The iDScore_plantar model proved to be a simple scoring tool to help clinicians in assigning a progressive risk of malignancy to pAMLs.
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