‘Pitfalls for differentiating basal cell carcinoma from non‐basal cell carcinoma on optical coherence tomography: A clinical series’

Author:

Wolswijk Tom12ORCID,Nelemans Patty J.3,Adan Fieke12,Abdul Hamid Myrurgia4,Mosterd Klara12

Affiliation:

1. Department of Dermatology Maastricht University Medical Center+ Maastricht The Netherlands

2. GROW Research Institute for Oncology and Reproduction Maastricht University Maastricht The Netherlands

3. Department of Epidemiology Maastricht University Maastricht The Netherlands

4. Department of Pathology Maastricht University Medical Center+ Maastricht The Netherlands

Abstract

AbstractOptical coherence tomography (OCT), a non‐invasive diagnostic modality, may replace biopsy for diagnosing basal cell carcinoma (BCC) if a high‐confidence BCC diagnosis can be established. In other cases, biopsy remains necessary to establish a histopathological diagnosis and treatment regimen. It is, therefore, essential that OCT assessors have a high specificity for differentiating BCC from non‐BCC lesions. To establish high‐confidence BCC diagnoses, specific morphological BCC characteristics on OCT are used. This study aimed to review several cases of non‐BCC lesions that were misclassified as BCC by experienced OCT assessors, thereby providing insight into the causes of these misclassifications and how they may be prevented. The study population consisted of patients who had a histopathologically‐verified non‐BCC lesion. Patients from Maastricht University Medical Center+ from February 2021 to April 2021 were included in the study. Two independent OCT assessors assessed OCT scans. One OCT assessor recorded the presence or absence of validated morphological BCC characteristics. A false‐positive OCT test result was defined as certainty of BCC presence in a non‐BCC lesion. The frequency of misclassifications and the presence or absence of morphological BCC features are discussed. A total of 124 patients with non‐BCC lesions were included. Six patients were misclassified by both OCT assessors and are discussed in more detail. Histopathological diagnoses were squamous cell carcinoma (n = 2/21), actinic keratosis (n = 2/29), squamous cell carcinoma in situ/Bowen's disease (n = 1/16), or interphase dermatitis (n = 1/4). In all misclassified cases, multiple, apparent morphological BCC characteristics on OCT were present. Most non‐BCC lesions are recognized as such by OCT assessors. However, there remains a small risk that a high‐confidence BCC diagnosis is established in non‐BCC lesions wherein features mimicking validated BCC characteristics are present. Misclassification may be prevented by careful delineation of epidermal layers and good differentiation between dermal ovoid structures typical of BCC versus squamous cell carcinoma.

Publisher

Wiley

Subject

Dermatology,General Medicine

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