[Hereditary hypomelanocytoses: the role of PAX3, SOX10, MITF, SNAI2, KIT, EDN3 and EDNRB genes].

[oculocutaneous albinism]

Hypo- and hyperpigmentation disorders are the most severe dermatological diseases observed in patients from all over the world . These disorders can be divided into melanoses connected with disorders of melanocyte function and melanocytoses connected with melanocyte development . The article presents some hereditary hypomelanocytoses , which are caused by abnormal melanoblast development , migration and proliferation as well as by abnormal melanocyte viability and proliferation . These disorders are represented by Waardenburg syndrome , piebaldism and Tietz syndrome , and are caused by different mutations of various or the same genes . The types of mutations comprise missense and nonsense mutations , frameshifts (in -frame insertions or deletions ), truncating variations , splice alterations and non-stop mutations . It has been demonstrated that mutations of the same gene may cause different hypopigmentation syndromes that may have similar phenotypes . For example , mutations of the MITF gene cause Waardenburg syndrome type 2 A as well as Tietz syndrome . It has also been demonstrated that mutations of different genes may cause an identical syndrome . For example , mutations of MITF , SNAI 2 and SOX 10 genes are observed in Waardenburg syndrome type II and mutations of EDNRB , EDN 3 and SOX 10 genes are responsible for Waardenburg syndrome type IV . In turn , mutation of the KIT gene and /or heterozygous deletion of the SNAI 2 gene result in piebaldism disease . The knowledge of the exact mechanisms of pigmentary disorders may be useful in the development of new therapeutic approaches to their treatment .