J B Welsh scite author profile

Identification of a mutant epidermal growth factor (EGF) receptor that does not undergo downregulation has provided a genetic probe to investigate the role of internalization in ligand-induced mitogenesis. Contact-inhibited cells expressing this internalization-defective receptor exhibited a normal mitogenic response at significantly lower ligand concentrations than did cells expressing wild-type receptors. A transformed phenotype and anchorage-independent growth were observed at ligand concentrations that failed to elicit these responses in cells expressing wild-type receptors. These findings imply that activation of the protein tyrosine kinase activity at the cell membrane is sufficient for the growth-enhancing effects of EGF. Thus, downregulation can serve as an attenuation mechanism, without which transformation ensues.

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Phosphorylation of the epidermal growth factor receptor at threonine 654 inhibits ligand-induced internalization and down-regulation

Lund

Lazar

Chen

et al. 1990

Journal of Biological Chemistry

120

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Specific factors are required for kinase-dependent endocytosis of insulin receptors.

Welsh

Worthylake

Wiley

et al. 1994

MBoC

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J B Welsh

Ligand-Induced Transformation by a Noninternalizing Epidermal Growth Factor Receptor

Phosphorylation of the epidermal growth factor receptor at threonine 654 inhibits ligand-induced internalization and down-regulation

Specific factors are required for kinase-dependent endocytosis of insulin receptors.

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