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Cell Growth and Development

Specific Changes of Ras GTPase-Activating Protein (GAP) and a GAP-Associated p62 Protein during Calcium-Induced Keratinocyte Differentiation

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Pages 5319-5328 | Received 23 Mar 1992, Accepted 01 Sep 1992, Published online: 01 Apr 2023
 

Abstract

Induction of tyrosine phosphorylation occurs as an early and specific event in keratinocyte differentiation. A set of tyrosine-phosphorylated substrates which transduce mitogenic signals by tyrosine kinases has previously been identified. We show here that of these substrates, the Ras GTPase-activating protein, GAP, is specifically affected during calcium-induced keratinocyte differentiation. As early as 10 min after calcium addition to cultured primary mouse keratinocytes, GAP associates with tyrosine-phosphoiylated proteins and translocates to the membrane. In addition, a GAP-associated protein of ~62 kDa (p62) becomes rapidly and heavily tyrosine phosphorylated in both membrane and cytosolic fractions. This protein corresponds to the major tyrosine-phosphoiylated protein that is induced in differentiating keratinocytes as early as 5 min after calcium addition. p62 phosphorylation was not observed after exposure of these cells to epidermal growth factor, phorbol ester, or transforming growth factor p. In contrast, PLCγ and PI3K were tyrosine phosphorylated after epidermal growth factor, but not calcium, stimulation. Thus, changes of Ras GAP and an associated p62 protein occur as early and specific events in keratinocyte differentiation and appear to involve a calcium- induced tyrosine kinase.

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