Chelsea Fidai scite author profile

Keratoacanthoma (KA) is a common skin tumour that remains controversial regarding classification, epidemiology, diagnosis, prognosis and management. Classically, a KA manifests as a rapidly growing, well-differentiated, squamoid lesion with a predilection for sun-exposed sites in elderly people and a tendency to spontaneously regress. Historically, KAs have been considered a variant of cutaneous squamous cell carcinoma (cSCC) and are often reported as KA-type cSCC. However, the penchant for regression has led many to categorize KAs as biologically benign tumours with distinct pathophysiological mechanisms from malignant cSCC. The clinical and histopathological similarities between KA and cSCC, particularly the well-differentiated variant of cSCC, have made definitive differentiation difficult or impossible in many cases. The ambiguity between entities has led to the general recommendation for surgical excision of KAs to ensure a potentially malignant cSCC is not left untreated. This current standard creates unnecessary surgical morbidity and financial strain for patients, especially the atrisk elderly population. There have been no reports of death from a definitive KA to date, while cSCC has an approximate mortality rate of 1Á5%. Reliably distinguishing cSCC from KA would shift management strategies for KAs towards lessinvasive treatment modalities, prevent unnecessary surgical morbidity, and likely reduce associated healthcare costs. Herein, we review the pathophysiology and clinical characteristics of KA, and conclude on the balance of current evidence that KA is a benign lesion and distinct from cSCC.Defective mismatch repair genes (MLH1, MSH2, MSH6) leading to microsatellite instability 59,60 HPV, human papillomavirus.

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A pediatric case of pigmented epithelioid melanocytoma with chromosomal copy number alterations in 15q and 17q and a novel NTRK3‐SCAPER gene fusion

Friedman

Hernández

Fidai

et al. 2019

J Cutan Pathol

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Pigmented epithelioid melanocytoma (PEM) represents a group of rare, heavily pigmented melanocytic tumors encompassing lesions previously designated as "animal-type melanomas" and "epithelioid blue nevi." Despite the association of multiple such tumors in the setting of Carney complex, most cases of PEM occur spontaneously as solitary neoplasms in otherwise healthy patients. PEM may arise in both children and adults, and has a known propensity to spread to the regional lymph nodes.Despite this latter finding, recurrence at the biopsy site or spread beyond the lymph node basin is exceptionally uncommon. Although the molecular basis for PEM continues to be characterized, findings to date suggest that this category of melanocytic neoplasia has genetic alterations distinct from those seen in common nevi, dysplastic nevi, Spitz nevi, and melanoma. Herein, we present an in-depth clinical, histopathologic, and molecular analysis of a case of PEM occurring on the scalp of a young African American girl found to have a novel NTRK3-SCAPER gene fusion. K E Y W O R D S melanocytic neoplasms, melanocytic lesions, dermatopathology, pigmented epithelioid melanocytoma, NTRK3 fusion

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Successful treatment of facial port-wine birthmark in a premature infant

Fidai

Geronemus

2021

JAAD Case Reports

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Inpatient Diseases of Significance

Chadha

Fidai

McHargue

2019

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Response to ‘A clinical and biological review of keratoacanthoma’: reply from authors

et al. 2021

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Chelsea Fidai

A clinical and biological review of keratoacanthoma*

A pediatric case of pigmented epithelioid melanocytoma with chromosomal copy number alterations in 15q and 17q and a novel NTRK3‐SCAPER gene fusion

Successful treatment of facial port-wine birthmark in a premature infant

Inpatient Diseases of Significance

Response to ‘A clinical and biological review of keratoacanthoma’: reply from authors

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