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Multicenter Study
Prediction of Non-sentinel Node Status in Patients with Melanoma and Positive Sentinel Node Biopsy: An Italian Melanoma Intergroup (IMI) Study.
- Carlo Riccardo Rossi, Simone Mocellin, Luca Giovanni Campana, Lorenzo Borgognoni, Serena Sestini, Giuseppe Giudice, Corrado Caracò, Adriana Cordova, Nicola Solari, Dario Piazzalunga, Paolo Carcoforo, Pietro Quaglino, Virginia Caliendo, Simone Ribero, and Italian Melanoma Intergroup (IMI).
- Surgical Oncology Unit, IOV-IRCCS of Padova, Padua, Italy.
- Ann. Surg. Oncol. 2018 Jan 1; 25 (1): 271-279.
Background And PurposeApproximately 20% of melanoma patients harbor metastases in non-sentinel nodes (NSNs) after a positive sentinel node biopsy (SNB), and recent evidence questions the therapeutic benefit of completion lymph node dissection (CLND). We built a nomogram for prediction of NSN status in melanoma patients with positive SNB.MethodsData on anthropometric and clinicopathological features of patients with cutaneous melanoma who underwent CLND after a positive SNB were collected from nine Italian centers. Multivariate logistic regression was utilized to identify predictors of NSN status in a training set, while model efficiency was validated in a validation set.ResultsData were available for 1220 patients treated from 2000 through 2016. In the training set (n = 810), the risk of NSN involvement was higher when (1) the primary melanoma is thicker or (2) sited in the trunk/head and neck; (3) fewer nodes are excised and (4) more nodes are involved; and (5) the lymph node metastasis is larger or (6) is deeply located. The model showed high discrimination (area under the receiver operating characteristic curve 0.74, 95% confidence interval [CI] 0.70-0.79) and calibration (Brier score 0.16, 95% CI 0.15-0.17) performance in the validation set (n = 410). The nomogram including these six clinicopathological variables performed significantly better than five other previously published models in terms of both discrimination and calibration.ConclusionsOur nomogram could be useful for follow-up personalization in clinical practice, and for patient risk stratification while conducting clinical trials or analyzing their results.
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