Ectodermal dysplasia-skin fragility syndrome.

[epidermolysis bullosa simplex]

Pathogenic mutations have now been described in ten different desmosomal proteins : plakophilin 1 (PKP 1 ) and 2 (PKP 2 ); desmoplakin ; plakoglobin ; desmoglein 1 , 2 , and 4 ; desmocollin 2 , and 3 corneodesmosin . Nevertheless , the first report of an inherited desmosomal gene disorder , published in 1997 , involved loss -of-function mutations on both alleles of PKP 1 , the PKP 1 gene . Loss of PKP 1 expression in human skin leads to skin erosions and crusting , notably with perioral fissuring as well as palmoplantar hyperkeratosis with painful cracking of the skin . Other more variable features include abnormalities of ectodermal development with growth delay , hypotrichosis or alopecia , hypohidrosis , and nail dystrophy . In contrast to some other inherited disorders of desmosomes , there is no cardiac pathology in individuals with PKP 1 mutations since it is not expressed in the heart . The collection of clinical features in individuals with PKP 1 mutations has been termed ectodermal dysplasia -skin fragility (ED -SF ) syndrome . This genodermatosis is classified as a suprabasal form of epidermolysis bullosa simplex and thus far there have been 10 published cases . Skin biopsy shows acanthosis , acantholysis , and a reduced number of small , poorly formed desmosomes . Loss of PKP 1 expression results in an integral weakness within the desmosomal plaque , leading to desmosomal detachment and cell-cell separation . Thus , the clinicopathologic features attest to the significant role of PKP 1 in stabilization of desmosome structure and function , predominantly in the spinous layers of the epidermis . This article reviews the clinical , structural , and molecular pathology of this genetic disorder of desmosomes .