EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling

EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling

Autocatalytic activation of epidermal growth factor receptor (EGFR) coupled to dephosphorylating activity of protein tyrosine phosphatases (PTPs) ensures robust yet diverse responses to extracellular stimuli. The inevitable tradeoff of this plasticity is spontaneous receptor activation and spurious...

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Main Authors: Martin Baumdick, Yannick Brüggemann, Malte Schmick, Georgia Xouri, Ola Sabet, Lloyd Davis, Jason W Chin, Philippe IH Bastiaens
Format: Article
Language:English
Published: eLife Sciences Publications Ltd 2015-11-01
Series:eLife
Subjects:
vesicular EGFR trafficking
spontaneous phosphorylation
autocatalysis
recycling endosome
partitioned phosphatase activities
ubiquitination
Online Access:https://elifesciences.org/articles/12223
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spelling doaj-4f7877276b08453cbe0051d2b6968af32021-05-05T00:07:52ZengeLife Sciences Publications LtdeLife2050-084X2015-11-01410.7554/eLife.12223EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signalingMartin Baumdick0Yannick Brüggemann1Malte Schmick2Georgia Xouri3Ola Sabet4Lloyd Davis5Jason W Chin6Philippe IH Bastiaens7Department of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Dortmund, GermanyDepartment of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Dortmund, Germany; Faculty of Chemistry and Chemical Biology, Technical University of Dortmund, Dortmund, GermanyDepartment of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Dortmund, GermanyDepartment of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Dortmund, GermanyDepartment of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Dortmund, GermanyMedical Research Council Laboratory of Molecular Biology, Cambridge, United KingdomMedical Research Council Laboratory of Molecular Biology, Cambridge, United KingdomDepartment of Systemic Cell Biology, Max Planck Institute of Molecular Physiology, Dortmund, Germany; Faculty of Chemistry and Chemical Biology, Technical University of Dortmund, Dortmund, GermanyAutocatalytic activation of epidermal growth factor receptor (EGFR) coupled to dephosphorylating activity of protein tyrosine phosphatases (PTPs) ensures robust yet diverse responses to extracellular stimuli. The inevitable tradeoff of this plasticity is spontaneous receptor activation and spurious signaling. We show that a ligand-mediated switch in EGFR trafficking enables suppression of spontaneous activation while maintaining EGFR’s capacity to transduce extracellular signals. Autocatalytic phosphorylation of tyrosine 845 on unliganded EGFR monomers is suppressed by vesicular recycling through perinuclear areas with high PTP1B activity. Ligand-binding results in phosphorylation of the c-Cbl docking tyrosine and ubiquitination of the receptor. This secondary signal relies on EGF-induced EGFR self-association and switches suppressive recycling to directional trafficking. The re-routing regulates EGFR signaling response by the transit-time to late endosomes where it is switched-off by high PTP1B activity. This ubiquitin-mediated switch in EGFR trafficking is a uniquely suited solution to suppress spontaneous activation while maintaining responsiveness to EGF.https://elifesciences.org/articles/12223vesicular EGFR traffickingspontaneous phosphorylationautocatalysisrecycling endosomepartitioned phosphatase activitiesubiquitination
collection DOAJ
language English
format Article
sources DOAJ
author Martin Baumdick
Yannick Brüggemann
Malte Schmick
Georgia Xouri
Ola Sabet
Lloyd Davis
Jason W Chin
Philippe IH Bastiaens
spellingShingle Martin Baumdick
Yannick Brüggemann
Malte Schmick
Georgia Xouri
Ola Sabet
Lloyd Davis
Jason W Chin
Philippe IH Bastiaens
EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling
eLife
vesicular EGFR trafficking
spontaneous phosphorylation
autocatalysis
recycling endosome
partitioned phosphatase activities
ubiquitination
author_facet Martin Baumdick
Yannick Brüggemann
Malte Schmick
Georgia Xouri
Ola Sabet
Lloyd Davis
Jason W Chin
Philippe IH Bastiaens
author_sort Martin Baumdick
title EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling
title_short EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling
title_full EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling
title_fullStr EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling
title_full_unstemmed EGF-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to EGFR signaling
title_sort egf-dependent re-routing of vesicular recycling switches spontaneous phosphorylation suppression to egfr signaling
publisher eLife Sciences Publications Ltd
series eLife
issn 2050-084X
publishDate 2015-11-01
description Autocatalytic activation of epidermal growth factor receptor (EGFR) coupled to dephosphorylating activity of protein tyrosine phosphatases (PTPs) ensures robust yet diverse responses to extracellular stimuli. The inevitable tradeoff of this plasticity is spontaneous receptor activation and spurious signaling. We show that a ligand-mediated switch in EGFR trafficking enables suppression of spontaneous activation while maintaining EGFR’s capacity to transduce extracellular signals. Autocatalytic phosphorylation of tyrosine 845 on unliganded EGFR monomers is suppressed by vesicular recycling through perinuclear areas with high PTP1B activity. Ligand-binding results in phosphorylation of the c-Cbl docking tyrosine and ubiquitination of the receptor. This secondary signal relies on EGF-induced EGFR self-association and switches suppressive recycling to directional trafficking. The re-routing regulates EGFR signaling response by the transit-time to late endosomes where it is switched-off by high PTP1B activity. This ubiquitin-mediated switch in EGFR trafficking is a uniquely suited solution to suppress spontaneous activation while maintaining responsiveness to EGF.
topic vesicular EGFR trafficking
spontaneous phosphorylation
autocatalysis
recycling endosome
partitioned phosphatase activities
ubiquitination
url https://elifesciences.org/articles/12223
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AT yannickbruggemann egfdependentreroutingofvesicularrecyclingswitchesspontaneousphosphorylationsuppressiontoegfrsignaling
AT malteschmick egfdependentreroutingofvesicularrecyclingswitchesspontaneousphosphorylationsuppressiontoegfrsignaling
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AT philippeihbastiaens egfdependentreroutingofvesicularrecyclingswitchesspontaneousphosphorylationsuppressiontoegfrsignaling
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