Smooth muscle hyperplasia in protein kinase C‐fused blue naevi: Report of 12 cases

Author:

Goutas Dimitrios1,Hayenne Pauline2,Tirode Franck2,Pissaloux Daniel2ORCID,Yeh Iwei34,de la Fouchardiere Arnaud2

Affiliation:

1. First Department of Pathology School of Medicine, The National and Kapodistrian University of Athens Athens Greece

2. Centre Léon Bérard, Cancer Research Center of Lyon, Equipe Labellisée Ligue contre le Cancer Université de Lyon, Université Claude Bernard Lyon 1 Lyon France

3. Department of Dermatology University of California San Francisco CA USA

4. Department of Pathology University of California San Francisco CA USA

Abstract

Background and aimsPKC‐fused blue naevi are a recently described group of melanocytic tumours that have distinctive morphological features, including a pigmented epithelioid melanocytoma‐like junctional component or a dermal biphasic architecture associating with naevocytoid nests surrounded by dendritic and spindled pigmented melanocytes (so‐called ‘combined common and blue naevus’). There have been reports of smooth muscle hyperplasia in a hamartoma‐like pattern in cases of combined blue naevi without genetic exploration.Materials and methodsHerein, we describe 12 cases of protein kinase C (PKC)‐fused blue tumours associated with a co‐existing smooth muscle hyperplasia, identified from a total of 98 PKC‐fused melanocytic tumours. Archived slides of PKC‐fused blue naevi with haematoxylin, eosin and phloxin staining, immunohistochemistry and molecular confirmation of a PKC‐fusion by fluorescence in‐situ hybridisation (FISH) or RNAseq were re‐evaluated for identification of notable smooth muscle hyperplasia. Fifty‐one of these slides had already been studied in a previous publication from our group.ResultsThe hyperplasia ranged from hypertrophic arrector pili muscles to extensive horizontal bundles of disorganised fibres constantly associated and limited within a biphasic dermal melanocytic component. At least one arrector pili muscle was always visible within the tumour, with occasionally direct extension of the hyperplastic fibres from the main muscle body. These muscle fibres were devoid of a PKC‐fusion signal by FISH. PKC molecules are involved in the regulation of smooth muscle function, offering an explanatory framework.ConclusionsThese data suggest incorporating smooth muscle hyperplasia as a diagnostic morphological feature of PKC‐fused blue melanocytic tumours.

Publisher

Wiley

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