Down-regulation of MET, the receptor for hepatocyte growth factor

Down-regulation of MET, the receptor for hepatocyte growth factor

The ligand-dependent degradation of activated tyrosine kinase receptors provides a means by which mitogenic signalling can be attenuated. In many cell types the ligand-dependent degradation of the tyrosine kinase receptor Met is completely dependent on the activity of the 26S proteasome (Jeffers et...

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Veröffentlicht in:Oncogene 2001-05, Vol.20 (22), p.2761-2770
Hauptverfasser: HAMMOND, Dean E, URBE, Sylvie, VANDE WOUDE, George F, CLAGUE, Michael J
Format: Artikel
Sprache:eng
Schlagworte:
Acetylcysteine - analogs & derivatives
Acetylcysteine - pharmacology
Adenosine triphosphatase
Biological and medical sciences
c-Met protein
Cell physiology
Cell transformation and carcinogenesis. Action of oncogenes and antioncogenes
Cysteine Proteinase Inhibitors - pharmacology
Degradation
Down-Regulation
Dynamin
Endocytosis
Endosomes - metabolism
Epidermal growth factor
Fundamental and applied biological sciences. Psychology
HeLa Cells - drug effects
HeLa Cells - metabolism
Hepatocyte growth factor
Hepatocyte Growth Factor - metabolism
Hepatocyte Growth Factor - pharmacology
hepatocyte growth factor receptors
Humans
Internalization
Kinases
Lactacystin
Ligands
MET protein
Molecular and cellular biology
Proteasome 26S
Proteasome inhibitors
Protein-tyrosine kinase receptors
Proteins
Proto-Oncogene Proteins c-met - metabolism
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Zusammenfassung:The ligand-dependent degradation of activated tyrosine kinase receptors provides a means by which mitogenic signalling can be attenuated. In many cell types the ligand-dependent degradation of the tyrosine kinase receptor Met is completely dependent on the activity of the 26S proteasome (Jeffers et al., 1997b). We now show that degradation also requires trafficking to late endosomal compartments and the activity of acid dependent proteases as determined by the effects of a dominant negative form of dynamin (K44A) and a vacuolar-ATPase inhibitor, concanamycin. We show that in the presence of the proteasome inhibitor lactacystin, Met fails to redistribute from the plasma membrane to intracellular compartments. This observation is most consistent with the interpretation that proteasome activity is required for Met internalization and only indirectly for its degradation.
ISSN:0950-9232
1476-5594
DOI:10.1038/sj.onc.1204475