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Expression of a Truncated Keratin 5 May Contribute to Severe Palmar–Plantar Hyperkeratosis in Epidermolysis Bullosa Simplex Patients

Authors :
Lynne T. Smith
Beverly A. Dale
Robert J. Livingston
Virginia P. Sybert
Richard B. Presland
Karen Stephens
Source :
Journal of Investigative Dermatology. 116(6):970-974
Publication Year :
2001
Publisher :
Elsevier BV, 2001.

Abstract

Epidermolysis bullosa simplex are dominant disorders of skin fragility characterized by intraepidermal blistering upon mild mechanical trauma. Skin fragility is caused by expression of either an abnormal keratin 5 or an abnormal keratin 14 protein, which compromises the structure and function of the keratin cytoskeleton of basal cells. We report an epidermolysis bullosa simplex patient with a novel single base substitution (A--T1414) that changes the lysine residue at amino acid 472 to a non-sense codon (K472X). This change predicts the synthesis of a truncated keratin 5, missing 119 amino acids, including the entire tail domain and the highly conserved KLLEGE motif at the carboxy terminus of the 2B domain of the central rod. Expression of an altered keratin 5, of predicted mass and pI for the product of the K472X allele, was documented by one- and two-dimensional western blots of protein extracts from patient skin. Ultrastructural analysis of the patient's nonhyperkeratotic skin was remarkable for basal keratinocytes with dense and irregular keratin filaments proximal to the basement membrane. Keratinocytes, transfected with a cDNA carrying the A--T1414 non-sense mutation, overexpressed a truncated keratin 5, and showed a disorganized and collapsed keratin filament cytoskeleton. This is the second epidermolysis bullosa simplex patient reported with a premature termination mutation in the KLLEGE motif. The remarkable occurrence of severe palmar--plantar hyperkeratosis in both patients suggests that the keratin 5 tail domain may have unrecognized, but important, normal functions in palmar-plantar tissues.

Details

ISSN :
0022202X
Volume :
116
Issue :
6
Database :
OpenAIRE
Journal :
Journal of Investigative Dermatology
Accession number :
edsair.doi.dedup.....55adc77e9079c3ce096f62f46317d4b9
Full Text :
https://doi.org/10.1046/j.1523-1747.2001.01324.x