Diagnostic discordance among histopathological reviewers of melanocytic lesions

Gregory A Hosler; Matthew S Goldberg; Sarah I Estrada; Brendan O'Neil; Sapna M Amin; Jose A Plaza

doi:10.1111/cup.14635

Diagnostic discordance among histopathological reviewers of melanocytic lesions

J Cutan Pathol. 2024 May 9. doi: 10.1111/cup.14635. Online ahead of print.

Authors

Gregory A Hosler¹, Matthew S Goldberg^{2

3}, Sarah I Estrada⁴, Brendan O'Neil⁵, Sapna M Amin⁶, Jose A Plaza⁷

Affiliations

¹ ProPath, Dallas, Texas, USA.
² Castle Biosciences, Inc, Friendswood, Texas, USA.
³ Icahn School of Medicine at Mount Sinai, New York, New York, USA.
⁴ Affiliated Dermatology, Scottsdale, Arizona, USA.
⁵ Northern Arizona Dermatology Center, Flagstaff, Arizona, USA.
⁶ Clin-Path Associates, Tempe, Arizona, USA.
⁷ Department of Pathology and Dermatology, The Ohio State University Wexner Medical Center, Columbus, Ohio, USA.

PMID: 38725224
DOI: 10.1111/cup.14635

Abstract

Background: Histopathological examination is adequate for the diagnosis of most cutaneous melanocytic neoplasms. However, there is a subset that is either difficult to definitively diagnose or would have diagnostic disagreement upon review by multiple dermatopathologists if a more exhaustive review was performed.

Methods: Melanocytic lesions underwent an independent, blinded diagnostic histopathological review of hematoxylin and eosin-stained sections. Each lesion was reviewed by three to six dermatopathologists and categorized as benign, malignant, or unknown malignant potential (UMP). Diagnoses were grouped as concordant (all the same designation); opposing (received benign and malignant designations); majority (single designation with the highest number of diagnoses, no benign/malignant opposing designations); and non-definitive (equal number of non-opposing designations [i.e., benign/UMP or malignant/UMP]). Lesions with equivocal designations (concordant or majority UMP, opposing, majority, and non-definitive) were utilized in a patient treatment model of projected surgical treatment discrepancies.

Results: In total, 3317 cases were reviewed, and 23.8% of lesions received equivocal diagnoses. Of these, 7.3% were majority benign, 4.8% were majority malignant, 2.7% were majority UMP, 0.5% were concordant UMP, 6.9% were opposing, and 1.6% were non-definitive. Patient treatment models of those with equivocal lesions (n = 788) revealed a potential of overall surgical treatment variations ranging from 18% to 72%, with the highest variation amongst lesions with opposing, non-definitive, or majority UMP (40%-72%) diagnoses.

Conclusion: Histopathologic review in this large cohort demonstrated substantial diagnostic variation, with 23.8% of cases receiving equivocal diagnoses. We identified diagnostic ambiguity even in lesions where a definitive diagnosis was previously rendered by a single real-world dermatopathologist. The combined clinical impact of diagnostic discordance or a final diagnosis of UMP is highlighted by high diagnosis-dependent treatment variation in the patient treatment model, which could be underreported in a real-world setting, where review by more than one to two dermatopathologists is relatively rare.

Keywords: dermatopathology; diagnostic discordance; equivocal; melanocytic; melanoma.

Grants and funding

Castle Biosciences