EGF, but not TGFα, efficiently induces degradation of the EGF receptor (EGFR). We show that EGFR was initially polyubiquitinated to the same extent upon incubation with EGF and TGFα, whereas the ubiquitination was more sustained by incubation with EGF than with TGFα. Consistently, the ubiquitin ligase c-Cbl was recruited to the plasma membrane upon activation of the EGFR with EGF and TGFα, but localized to endosomes only upon activation with EGF. EGF remains bound to the EGFR upon endocytosis, whereas TGFα dissociates from the EGFR. Therefore, the sustained polyubiquitination is explained by EGF securing the kinase activity of endocytosed EGFR. Overexpression of the dominant negative N-Cbl inhibited ubiquitination of the EGFR and degradation of EGF and EGFR. This demonstrates that EGF-induced ubiquitination of the EGFR as such is important for lysosomal sorting. Both lysosomal and proteasomal inhibitors blocked degradation of EGF and EGFR, and proteasomal inhibitors inhibited translocation of activated EGFR from the outer limiting membrane to inner membranes of multivesicular bodies (MVBs). Therefore, lysosomal sorting of kinase active EGFR is regulated by proteasomal activity. Immuno-EM showed the localization of intact EGFR on internal membranes of MVBs. This demonstrates that the EGFR as such is not the proteasomal target.
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4 March 2002
Article|
February 25 2002
Ubiquitination and proteasomal activity is required for transport of the EGF receptor to inner membranes of multivesicular bodies
Karianne E. Longva,
Karianne E. Longva
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
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Frøydis D. Blystad,
Frøydis D. Blystad
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
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Espen Stang,
Espen Stang
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
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Astrid M. Larsen,
Astrid M. Larsen
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
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Lene E. Johannessen,
Lene E. Johannessen
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
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Inger H. Madshus
Inger H. Madshus
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
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Karianne E. Longva
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
Frøydis D. Blystad
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
Espen Stang
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
Astrid M. Larsen
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
Lene E. Johannessen
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
Inger H. Madshus
Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway
Address correspondence to Inger H. Madshus, Institute of Pathology, The University of Oslo, Rikshospitalet, N-0027 Oslo, Norway. Tel.: 47-23-073-536. Fax: 47-23-071-511. E-mail: [email protected]
K.E. Longva, F.D. Blystad, and E. Stang contributed equally to this work.
*
Abbreviations used in this paper: CHX, cycloheximide; EGFR, EGF receptor; GFP, green fluorescent protein; HA, hemagglutinin; MVBs, multivesicular bodies; PDGFR, PDGF receptor; Tf, transferrin.
Received:
June 11 2001
Revision Received:
June 18 2001
Accepted:
January 23 2002
Online ISSN: 1540-8140
Print ISSN: 0021-9525
The Rockefeller University Press
2002
J Cell Biol (2002) 156 (5): 843–854.
Article history
Received:
June 11 2001
Revision Received:
June 18 2001
Accepted:
January 23 2002
Citation
Karianne E. Longva, Frøydis D. Blystad, Espen Stang, Astrid M. Larsen, Lene E. Johannessen, Inger H. Madshus; Ubiquitination and proteasomal activity is required for transport of the EGF receptor to inner membranes of multivesicular bodies . J Cell Biol 4 March 2002; 156 (5): 843–854. doi: https://doi.org/10.1083/jcb.200106056
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