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Wiley InterScience

Journal of the European Academy of Dermatology and Venereology

Journal of the European Academy of Dermatology and Venereology

Volume 19 Issue 2, Pages 147 - 152

Published Online: 19 Nov 2004

Journal compilation © 2010 European Academy of Dermatology and Venereology



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REVIEW
Pityriasis versicolor alba
W Thoma*†, H-J Krämer, P Mayser
  Center of Dermatology and Andrology, Gaffkystr. 14, D-35385 Giessen, Germany.
  *Corresponding author, fax +49 641 99 43209; E-mail: wiebke.thoma@derma.med.uni-giessen.de
Copyright © 2004 European Academy of Dermatology and Venereology

ABSTRACT

AbstractIntroductionClinic of pityriasis versicolor albaHistology and electron microscopy of pityriasis versicolor albaTherapyReferences

Pityriasis versicolor alba is a hypopigmented or depigmented variant of pityriasis versicolor characterized by maculous, partly pityriasiform, scaly depigmented lesions occurring particularly in seborrhoeic areas. Long-persisting hypopigmentation after healing of the pityriasis versicolor was first described by Gudden in 1853. Hypopigmentation and depigmentation were later differentiated as an independent variant of the disease. In 1848, Eichstedt recognized the pathogen-related character of pityriasis versicolor in its hyperpigmented form. Today it is generally accepted that the disease is caused by yeasts of the genus Malassezia, of which nine species are differentiated. It is controversial whether a single species is responsible for the disease. The pathogenesis of depigmentation has not been established. A screening effect by the scale layer as well as toxic effects on pigment synthesis by fungal metabolites have been discussed. With regard to the second mechanism, the newly discovered tryptophan-derived metabolites of M. furfur might be significant. Evidence-based data concerning the therapy of pityriasis versicolor alba do not exist. According to current recommendations, pityriasis versicolor should be rapidly treated with antimycotics, followed by ultraviolet therapy to induce maturation of existent melanosomes and accelerate repigmentation. However, depigmented lesions are difficult to improve by ultraviolet therapy.


Received: 24 December 2003; accepted 4 March 2004

DIGITAL OBJECT IDENTIFIER (DOI)
10.1111/j.1468-3083.2004.01085.x About DOI

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