Mitotic Rate As a Predictor of Sentinel Lymph Node Positivity in Patients with Thin Melanomas

Overview

Journal Ann Surg Oncol

Publisher Springer

Specialty Oncology

Date 2005 May 3

PMID 15864482

Citations 44

Authors

Susan B Kesmodel

Giorgos C Karakousis

Jeffrey D Botbyl

Robert J Canter

Robert T Lewis

Peter M Wahl

Kyla P Terhune

Abass Alavi

David E Elder

Michael E Ming

DuPont Guerry

Phyllis A Gimotty

Douglas L Fraker

Brian J Czerniecki

Francis R Spitz

Affiliations

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Abstract

Background: Lymphatic mapping and sentinel lymphadenectomy (LM/SL) provide important prognostic information for patients with early-stage melanoma. Although the use of this technique in patients with thin melanomas (< or =1.00 mm) is not routine, risk factors that may predict sentinel lymph node (SLN) positivity in this patient population are under investigation. We sought to determine whether mitotic rate (MR) is associated with SLN positivity in thin-melanoma patients and, therefore, whether it may be used to risk-stratify and select patients for LM/SL.

Methods: Clinical and histopathologic variables were reviewed for 181 patients with thin melanomas who underwent LM/SL from January 1996 through January 2004. Univariate and multivariate logistic regression analyses were performed to identify factors associated with SLN positivity. Risk groups were defined on the basis of the development of a classification tree.

Results: The overall SLN positivity rate was 5%. All patients with positive SLNs had an MR of >0. By univariate analysis, MR and thickness were significant predictors of SLN positivity. The association between MR and SLN positivity remained significant controlling for each of the other variables evaluated. On the basis of a classification tree, patients with an MR >0 and tumor thickness > or =.76 mm were identified as a higher-risk group, with an SLN positivity rate of 12.3%.

Conclusions: In patients with thin melanomas, MR >0 seems to be a significant predictor of SLN positivity that may be used to risk-stratify and select patients for LM/SL. To confirm these results, the predictive value of MR for SLN positivity needs to be validated in other populations of thin-melanoma patients.

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