Connexin-26 mutations in deafness and skin disease

Gap junctions allow the exchange of ions and small molecules between adjacent cells through intercellular channels formed by connexin proteins, which can also form functional hemichannels in nonjunctional membranes. Mutations in connexin genes cause a variety of human diseases. For example, mutation...

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Bibliographic Details
Published in:Expert reviews in molecular medicine 2009-11, Vol.11, p.e35-e35, Article e35
Main Authors: Lee, Jack R., White, Thomas W.
Format: Article
Language:English
Subjects:
Connexin 26
Connexins - genetics
Deafness - genetics
Gap Junctions
Humans
Ichthyosis - genetics
Ion Channel Gating - genetics
Ion Channel Gating - physiology
Keratoderma, Palmoplantar - genetics
Molecular Sequence Data
Mutation
Pedigree
Retrocochlear Diseases - genetics
Skin Diseases - genetics
Syndrome
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Summary:Gap junctions allow the exchange of ions and small molecules between adjacent cells through intercellular channels formed by connexin proteins, which can also form functional hemichannels in nonjunctional membranes. Mutations in connexin genes cause a variety of human diseases. For example, mutations in GJB2, the gene encoding connexin-26 (Cx26), are not only a major cause of nonsyndromic deafness, but also cause syndromic deafness associated with skin disorders such as palmoplantar keratoderma, keratitis–ichthyosis deafness syndrome, Vohwinkel syndrome, hystrix–ichthyosis deafness syndrome and Bart–Pumphrey syndrome. The most common mutation in the Cx26 gene linked to nonsyndromic deafness is 35ΔG, a frameshift mutation leading to an early stop codon. The large number of deaf individuals homozygous for 35ΔG do not develop skin disease. Similarly, there is abundant experimental evidence to suggest that other Cx26 loss-of-function mutations cause deafness, but not skin disease. By contrast, Cx26 mutations that cause both skin diseases and deafness are all single amino acid changes. Since nonsyndromic deafness is predominantly a loss-of-function disorder, it follows that the syndromic mutants must show an alteration, or gain, of function to cause skin disease. Here, we summarise the functional consequences and clinical phenotypes resulting from Cx26 mutations that cause deafness and skin disease.
ISSN:1462-3994
1462-3994
DOI:10.1017/S1462399409001276