Histopathologic correlation of high-risk MelaFind TM lesions: a 3-year experience from a high-risk pigmented lesion clinic

A significant number of pigmented lesions are biopsied to rule out melanoma, but most will be benign. MelaFind is a highly sensitive, noninvasive computer-assisted system to aid in clinical diagnosis of melanoma. A total of 140 high-risk patients were followed by one expert dermatologist. Biopsies w...

Full description

Saved in:
Bibliographic Details
Published in:International journal of dermatology 2019-05, Vol.58 (5), p.569-576
Main Authors: Shrivastava, Vikas, Bailin, Phillip, Elliott, Jennifer, Bacnik, Elizabeth, Gastman, Brian, Bergfeld, Wilma, Billings, Steven D, Piliang, Melissa, Fernandez, Anthony, Kovalyshyn, Ivanka, Ko, Jennifer S
Format: Article
Language:English
Subjects:
Dysplastic Nevus Syndrome - diagnosis
Dysplastic Nevus Syndrome - diagnostic imaging
Dysplastic Nevus Syndrome - pathology
Humans
Image Interpretation, Computer-Assisted
Image Processing, Computer-Assisted
Melanoma - diagnosis
Melanoma - diagnostic imaging
Melanoma - pathology
Melanoma, Cutaneous Malignant
Nevus, Pigmented - diagnosis
Nevus, Pigmented - diagnostic imaging
Nevus, Pigmented - pathology
Skin Neoplasms - diagnosis
Skin Neoplasms - diagnostic imaging
Skin Neoplasms - pathology
Citations: Items that this one cites
Items that cite this one
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:A significant number of pigmented lesions are biopsied to rule out melanoma, but most will be benign. MelaFind is a highly sensitive, noninvasive computer-assisted system to aid in clinical diagnosis of melanoma. A total of 140 high-risk patients were followed by one expert dermatologist. Biopsies were blindly and independently evaluated by two dermatopathologists and given histologic severity scores (HSS, 0-12) based on the histologic features of melanoma/dysplastic nevi and compared to pathologic diagnoses and MelaFind scores. MelaFind reduced the biopsy number of clinically ambiguous lesions (923 scanned to 253 biopsied, 73% reduction). Biopsied cases were usually benign (135/253, 53.4%, HSS = 2.8-3.2). Dysplastic nevi with varying degrees of atypia were observed next most commonly (80/253, 31.6%, HSS = 4.7-5.2 for mild dysplasia and 7-7.6 for moderate to severe dysplasia). Melanomas comprised 11/253 (4.3%) of biopsies (HSS = 9.3-10.7). Twenty-four cases were given miscellaneous diagnoses not within the dysplastic nevus-melanoma spectrum (9.5%, HSS = 1.3). Dermal fibrosis was the most commonly identified worrisome histologic feature (177/253, 70%), closely followed by other known atypical features. Nonthreatening histologic features in benign lesions with high MelaFind disorganization scores were common. The HSS differed significantly depending on pathologic diagnosis severity, while the MelaFind score did not (benign = 2.2; mildly atypical = 4.8; moderately to severely atypical = 2.3; in-situ or invasive melanoma = 3.1). MelaFind unequivocally reduced the number of biopsies, but banal lesions had histologic attributes resulting in high-risk MelaFind scores, and MelaFind does not correlate with degree of cytologic atypia. Knowledge of these limitations should increase bidirectional confidence when making clinicopathologic correlations in high-risk patients.
ISSN:0011-9059
1365-4632
DOI:10.1111/ijd.14336