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Juvenile xanthogranuloma: A clinical, histopathologic and immunohistochemical study
Authors:Omar P Sangüeza  Julie K Salmon  Clifton R White Jr  Jay H Beckstead
Affiliation:Department of Pathology, Medical College of Georgia, Augusta, Georgia, USA;Department of Dermatology, Kaiser Medical Center, Portland, OR, USA;Department of Dermatology, Oregon Health Sciences University, Portland, Oregon, USA;Department of Pathology, Oregon Health Sciences University, Portland, Oregon, USA
Abstract:Juvenile xanthogranuloma (JXC) is a benign histiocylic proliferation of uncertain histogenesis which usually resolves spontaneously. Histopathologically, classic lesions are characterized by diffuse proliferations of foamy histiocytes, many of which may be multinucleated (Toulon cells), admixed with lymphocytes and eosinophils. Histologic variants of JXG, perhaps representing evolving lesions, may lack these typical histopathological features, showing diffuse infiltrates of non-foamy mononuclear histiocytes without Toulon cells, posing problems in differentiation from other histiocylic or melanocylic proliferations. Immunohistochemically, JXG is characterized by variable expressions of several histiocytic markers as well as the absence of staining for SI00 protein. To assess better the spectrum of histopathological and immunohistochemical features of JXG, we studied nine cases of classic or histologic variant of JXG. The cases were evaluated by light microscopy and with an extensive battery of antibodies. All 9 cases, regardless of their light microscopic appearance, showed markedly positive staining with histiocytic markers including CD68, HAM56, cathepsin B and vimentin, but did not stain for S100 protein. Antibodies to factor XIIIa stained positively in 8 cases while staining for other markers was variable. Our results suggest that the histiocytes in JXG lesions have macrophagic differentiation, probably representing a reactive process to an unknown stimulus.
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