Christoph Schubert scite author profile

Five patients with widespread plaque-type psoriasis were treated continuously with clobetasol under occlusion. Clinical healing was seen after 6-10 days of treatment. All plaques treated in this way clinically relapsed approximately 12 days later. During the period of remission, sequential biopsies were taken and prepared for light and electron microscopy. Histologically, the earliest indications of relapse were endothelial alterations (swelling, intercellular widening) followed by the appearance of mast cells around the postcapillary venules; these mast cells showed signs of degranulation. Hours later, activated macrophages showing pericellular edema were present, and these migrated into the epidermis soon after. Associated with the presence of macrophages, there was a complete loss of desmosome-tonofilament complexes. Later, lymphocytes and neutrophils were seen. Under these experimental conditions, the psoriatic-tissue alterations appear to have been initiated by degranulating mast cells as well as by macrophages which later invaded the epidermis.

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Inflammatory Properties of Neutrophil-Activating Protein-1/Interleukin 8 (NAP-1/IL-8) in Human Skin: A Light- and Electronmicroscopic Study

Swensson¹,

Schubert²,

Christophers³

et al. 1991

Journal of Investigative Dermatology

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Proliferation marker Ki-S5 as a diagnostic tool in melanocytic lesions

Rudolph

Schubert²,

Schubert

et al. 1997

Journal of the American Academy of Dermatology

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Dupuytren's contracture is associated with sprouting of substance P positive nerve fibres and infiltration by mast cells

Schubert¹,

Weidler²,

Borisch³

et al. 2006

Annals of the Rheumatic Diseases

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Differential Expression of CD34 and Ki-M1p in Pleomorphic Fibroma and Dermatofibroma With Monster Cells

Rudolph¹,

Schubert²,

Zelger³

et al. 1999

The American Journal of Dermatopathology

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Pleomorphic fibroma (PF) and dermatofibroma with monster cells (DFMC) are characterized by the presence of numerous cells with large atypical nuclei. Despite cytologic similarities, the two entities are likely to be unrelated, but their histogenesis is poorly understood. In this study, we examined six cases of PF and eleven cases of DFMC by immunohistochemistry using antibodies against vimentin, alpha-smooth muscle actin, S-100 protein, CD34, factor XIIIa, and the pan-monocytic marker Ki-M1p. Strong vimentin expression was seen in all tumors, whereas none of them expressed S-100 protein. PF consistently exhibited CD34 staining but appeared to be depleted of Ki-M1p positive cells compared with the surrounding normal skin. Conversely, all cases of DFMC contained numerous Ki-M1p positive cells including atypical multinucleate cells, but virtually no CD34 reactivity was observed. A weak staining for alpha-smooth muscle actin was occasionally seen in a subset of the cells of both entities. Our results indicate that PF and DFMC are histogenetically distinct entities that may arise from two different types of dermal dendritic cells defined by their reactivity for CD34 and Ki-M1p, respectively. Immunohistochemistry using these two antibodies permits an easy and reliable discrimination between PF and DFMC.

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