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Regulation of hemidesmosome disassembly by growth factor receptors.

Coert Margadant ,
Evelyne Frijns ,
Kevin Wilhelmsen ,
Arnoud Sonnenberg

Abstract

Hemidesmosomes (HDs) promote the stable adhesion of basal epithelial cells to the underlying basement membrane (BM). Critical for the mechanical stability of the HD is the interaction between integrin alpha6beta4 and plectin, which is destabilized when HD disassembly is required, for instance, to allow keratinocyte migration during wound healing. Growth factors such as epidermal growth factor (EGF) can trigger HD disassembly and induce phosphorylation of the beta4 intracellular domain. Whereas tyrosine phosphorylation appears to mediate cooperation with growth factor signaling pathways and invasion in carcinoma cells, serine phosphorylation seems the predominant mechanism for regulating HD destabilization. Here, we discuss recent advances that shed light on the residues involved, the identity of the kinases that phosphorylate them, and the interactions that become disrupted by these phosphorylations.

More about this publication

Current opinion in cell biology

Volume 20
Issue nr. 5
Pages 589-96
Publication date 01-10-2008

Full text links

Publisher website (DOI) 10.1016/j.ceb.2008.05.001
Europe PubMed Central 18583123
Pubmed 18583123

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