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Internalization of Met requires the co-receptor CD44v6 and its link to ERM proteins

Hasenauer, S.; Malinger, D.; Koschut, D.; Pace, G.; Matzke, A.; Au, A. von; Orian-Rousseau, V.

Abstract:

Receptor Tyrosine Kinases (RTKs) are involved in many cellular processes and play a major role in the control of cell fate. For these reasons, RTK activation is maintained under tight control. Met is an essential RTK that induces proliferation, differentiation, migration, survival and branching morphogenesis. Deregulation of Met by overexpression, amplification or lack of effective degradation leads to cancer and metastasis. We have shown that Met relies on CD44v6 for its activation and for signaling in several cancer cell lines and also in primary cells. In this paper, we show that internalization of Met is dependent on CD44v6 and the binding of Ezrin to the CD44v6 cytoplasmic domain. Both CD44v6 and Met are co-internalized upon Hepatocyte Growth Factor induction suggesting that Met-induced signaling from the endosomes relies on its collaboration with CD44v6 and the link to the cytoskeleton provided by ERM proteins.


Volltext §
DOI: 10.5445/IR/1000040279
Originalveröffentlichung
DOI: 10.1371/journal.pone.0062357
Scopus
Zitationen: 38
Web of Science
Zitationen: 36
Dimensions
Zitationen: 38
Cover der Publikation
Zugehörige Institution(en) am KIT Institut für Toxikologie und Genetik (ITG)
Publikationstyp Zeitschriftenaufsatz
Publikationsjahr 2013
Sprache Englisch
Identifikator ISSN: 1932-6203
urn:nbn:de:swb:90-402791
KITopen-ID: 1000040279
HGF-Programm 47.02.01 (POF II, LK 01) Synth. biomimetische Werkzeuge ITG
Erschienen in PLoS one
Verlag Public Library of Science (PLoS)
Band 8
Heft 4
Seiten e62357/1-15
Bemerkung zur Veröffentlichung Gefördert durch den KIT-Publikationsfonds
Nachgewiesen in Dimensions
Scopus
Web of Science
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