Endocytosis of the dermatan sulfate proteoglycan decorin utilizes multiple pathways and is modulated by epidermal growth factor receptor signaling

David Denis Sofeu Feugaing; Raija Tammi; Frank G. Echtermeyer; Harald Stenmark; Hans Kresse; Martin Smollich; Elke Schönherr; Ludwig Kiesel; Martin Götte

doi:10.1016/j.biochi.2006.12.012

Endocytosis of the dermatan sulfate proteoglycan decorin utilizes multiple pathways and is modulated by epidermal growth factor receptor signaling

David Denis Sofeu Feugaing, Raija Tammi, Frank G. Echtermeyer, Harald Stenmark, Hans Kresse, Martin Smollich, Elke Schönherr, Ludwig Kiesel, Martin Götte^*

^*Korrespondierende/r Autor/-in für diese Arbeit

Institut für Ernährungsmedizin

25 Zitate (Scopus)

Abstract

Human skin fibroblasts efficiently internalize the matrikine decorin by receptor-mediated endocytosis, however, very little is known about its intracellular trafficking routes up to lysosomal degradation. In an in vitro system measuring uptake and degradation of [³⁵S]sulfate-labeled decorin, endocytosis was blocked by 46% when clathrin assembly/disassembly was inhibited using chlorpromazine. Pharmacological inhibition of EGF receptor signaling caused 34% reduction of decorin uptake, whereas inhibition of the IGF receptor had no effect. Using confocal immunofluorescence microscopy, we determined that only about 5-10% of internalized decorin colocalized with the EGFR. Thus, uptake depends on EGFR signaling rather than trafficking along the same pathway. Decorin passes through early endosomes towards trafficking to lysosomes, since more than 50% of decorin colocalized with EEA1. Moreover, inhibition of endosomal fusion by wortmannin caused a profound inhibition of decorin endocytosis. Overexpression of the clathrin-binding Hrs protein, which has previously been shown to inibit EGFR degradation blocked the degradation of decorin. Cholesterol depletion by filipin inhibited uptake of decorin by 34%, however, nearly no intracellular colocalization was found between decorin and caveolin-1. The combined use of filipin and chlorpromazine had an additive inhibitory effect on decorin endocytosis. Moreover, chlorpromazine diverted decorin from the chlorpromazine-sensitive pathway to an alternative uptake route. The CD44/hyaluronan pathway was excluded as an endocytic route for decorin. Our observations indicate that decorin is taken up by more than one endocytic pathway. Of note, lipid-raft-dependent EGFR signaling modulates decorin uptake, suggesting the presence of a potential feedback regulation mechanism for desensitization of signaling events mediated by decorin.

Originalsprache	Englisch
Zeitschrift	Biochimie
Jahrgang	89
Ausgabenummer	5
Seiten (von - bis)	637-657
Seitenumfang	21
ISSN	0300-9084
DOIs	https://doi.org/10.1016/j.biochi.2006.12.012
Publikationsstatus	Veröffentlicht - 05.2007

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The authors would like to thank Siegmund Budny, Petra Blumberg, Monika Offers, Birgit Pers and Arja Venäläinen for technical assistance, Heinz-Jürgen Hausser for discussions and for communicating unpublished results, Dagmar Zeuschner for performing experiments in the early stages of this project, Volker Gerke for discussions and the generous gift of antibodies and Dr. Markku Tammi for AlexaFluor HABC. Part of this work was performed by Hans Kresse at the Cleveland Clinic Foundation, Cleveland, OH, USA, in collaboration with Vincent Hascall and Carol De La Motte, who have helped with suggestions to improve the manuscript. This study was financially supported by Deutsche Forschungsgemeinschaft SFB492 TP A6/A9/B12 (HK,MG,ES,FE), a Protogenia Research grant (MG), the Norwegian Cancer Society (HS), IZKF Münster D18 (FE) and a travel award of the American Society for Cell Biology (DDSF).

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Forschungsschwerpunkt: Gehirn, Hormone, Verhalten - Center for Brain, Behavior and Metabolism (CBBM)

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10.1016/j.biochi.2006.12.012

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@article{5481c54360fa4cb8807274b257a47ee7,

title = "Endocytosis of the dermatan sulfate proteoglycan decorin utilizes multiple pathways and is modulated by epidermal growth factor receptor signaling",

abstract = "Human skin fibroblasts efficiently internalize the matrikine decorin by receptor-mediated endocytosis, however, very little is known about its intracellular trafficking routes up to lysosomal degradation. In an in vitro system measuring uptake and degradation of [35S]sulfate-labeled decorin, endocytosis was blocked by 46\% when clathrin assembly/disassembly was inhibited using chlorpromazine. Pharmacological inhibition of EGF receptor signaling caused 34\% reduction of decorin uptake, whereas inhibition of the IGF receptor had no effect. Using confocal immunofluorescence microscopy, we determined that only about 5-10\% of internalized decorin colocalized with the EGFR. Thus, uptake depends on EGFR signaling rather than trafficking along the same pathway. Decorin passes through early endosomes towards trafficking to lysosomes, since more than 50\% of decorin colocalized with EEA1. Moreover, inhibition of endosomal fusion by wortmannin caused a profound inhibition of decorin endocytosis. Overexpression of the clathrin-binding Hrs protein, which has previously been shown to inibit EGFR degradation blocked the degradation of decorin. Cholesterol depletion by filipin inhibited uptake of decorin by 34\%, however, nearly no intracellular colocalization was found between decorin and caveolin-1. The combined use of filipin and chlorpromazine had an additive inhibitory effect on decorin endocytosis. Moreover, chlorpromazine diverted decorin from the chlorpromazine-sensitive pathway to an alternative uptake route. The CD44/hyaluronan pathway was excluded as an endocytic route for decorin. Our observations indicate that decorin is taken up by more than one endocytic pathway. Of note, lipid-raft-dependent EGFR signaling modulates decorin uptake, suggesting the presence of a potential feedback regulation mechanism for desensitization of signaling events mediated by decorin.",

author = "Feugaing, \{David Denis Sofeu\} and Raija Tammi and Echtermeyer, \{Frank G.\} and Harald Stenmark and Hans Kresse and Martin Smollich and Elke Sch{\"o}nherr and Ludwig Kiesel and Martin G{\"o}tte",

note = "Funding Information: The authors would like to thank Siegmund Budny, Petra Blumberg, Monika Offers, Birgit Pers and Arja Ven{\"a}l{\"a}inen for technical assistance, Heinz-J{\"u}rgen Hausser for discussions and for communicating unpublished results, Dagmar Zeuschner for performing experiments in the early stages of this project, Volker Gerke for discussions and the generous gift of antibodies and Dr. Markku Tammi for AlexaFluor HABC. Part of this work was performed by Hans Kresse at the Cleveland Clinic Foundation, Cleveland, OH, USA, in collaboration with Vincent Hascall and Carol De La Motte, who have helped with suggestions to improve the manuscript. This study was financially supported by Deutsche Forschungsgemeinschaft SFB492 TP A6/A9/B12 (HK,MG,ES,FE), a Protogenia Research grant (MG), the Norwegian Cancer Society (HS), IZKF M{\"u}nster D18 (FE) and a travel award of the American Society for Cell Biology (DDSF). Copyright: Copyright 2008 Elsevier B.V., All rights reserved.",

year = "2007",

month = may,

doi = "10.1016/j.biochi.2006.12.012",

language = "English",

volume = "89",

pages = "637--657",

journal = "Biochimie",

issn = "0300-9084",

publisher = "Elsevier B.V.",

number = "5",

}

Endocytosis of the dermatan sulfate proteoglycan decorin utilizes multiple pathways and is modulated by epidermal growth factor receptor signaling. / Feugaing, David Denis Sofeu; Tammi, Raija; Echtermeyer, Frank G. et al.
in: Biochimie, Jahrgang 89, Nr. 5, 05.2007, S. 637-657.

Publikation: Beiträge in Fachzeitschriften › Zeitschriftenaufsätze › Forschung › Begutachtung

TY - JOUR

T1 - Endocytosis of the dermatan sulfate proteoglycan decorin utilizes multiple pathways and is modulated by epidermal growth factor receptor signaling

AU - Feugaing, David Denis Sofeu

AU - Tammi, Raija

AU - Echtermeyer, Frank G.

AU - Stenmark, Harald

AU - Kresse, Hans

AU - Smollich, Martin

AU - Schönherr, Elke

AU - Kiesel, Ludwig

AU - Götte, Martin

N1 - Funding Information: The authors would like to thank Siegmund Budny, Petra Blumberg, Monika Offers, Birgit Pers and Arja Venäläinen for technical assistance, Heinz-Jürgen Hausser for discussions and for communicating unpublished results, Dagmar Zeuschner for performing experiments in the early stages of this project, Volker Gerke for discussions and the generous gift of antibodies and Dr. Markku Tammi for AlexaFluor HABC. Part of this work was performed by Hans Kresse at the Cleveland Clinic Foundation, Cleveland, OH, USA, in collaboration with Vincent Hascall and Carol De La Motte, who have helped with suggestions to improve the manuscript. This study was financially supported by Deutsche Forschungsgemeinschaft SFB492 TP A6/A9/B12 (HK,MG,ES,FE), a Protogenia Research grant (MG), the Norwegian Cancer Society (HS), IZKF Münster D18 (FE) and a travel award of the American Society for Cell Biology (DDSF). Copyright: Copyright 2008 Elsevier B.V., All rights reserved.

PY - 2007/5

Y1 - 2007/5

N2 - Human skin fibroblasts efficiently internalize the matrikine decorin by receptor-mediated endocytosis, however, very little is known about its intracellular trafficking routes up to lysosomal degradation. In an in vitro system measuring uptake and degradation of [35S]sulfate-labeled decorin, endocytosis was blocked by 46% when clathrin assembly/disassembly was inhibited using chlorpromazine. Pharmacological inhibition of EGF receptor signaling caused 34% reduction of decorin uptake, whereas inhibition of the IGF receptor had no effect. Using confocal immunofluorescence microscopy, we determined that only about 5-10% of internalized decorin colocalized with the EGFR. Thus, uptake depends on EGFR signaling rather than trafficking along the same pathway. Decorin passes through early endosomes towards trafficking to lysosomes, since more than 50% of decorin colocalized with EEA1. Moreover, inhibition of endosomal fusion by wortmannin caused a profound inhibition of decorin endocytosis. Overexpression of the clathrin-binding Hrs protein, which has previously been shown to inibit EGFR degradation blocked the degradation of decorin. Cholesterol depletion by filipin inhibited uptake of decorin by 34%, however, nearly no intracellular colocalization was found between decorin and caveolin-1. The combined use of filipin and chlorpromazine had an additive inhibitory effect on decorin endocytosis. Moreover, chlorpromazine diverted decorin from the chlorpromazine-sensitive pathway to an alternative uptake route. The CD44/hyaluronan pathway was excluded as an endocytic route for decorin. Our observations indicate that decorin is taken up by more than one endocytic pathway. Of note, lipid-raft-dependent EGFR signaling modulates decorin uptake, suggesting the presence of a potential feedback regulation mechanism for desensitization of signaling events mediated by decorin.

AB - Human skin fibroblasts efficiently internalize the matrikine decorin by receptor-mediated endocytosis, however, very little is known about its intracellular trafficking routes up to lysosomal degradation. In an in vitro system measuring uptake and degradation of [35S]sulfate-labeled decorin, endocytosis was blocked by 46% when clathrin assembly/disassembly was inhibited using chlorpromazine. Pharmacological inhibition of EGF receptor signaling caused 34% reduction of decorin uptake, whereas inhibition of the IGF receptor had no effect. Using confocal immunofluorescence microscopy, we determined that only about 5-10% of internalized decorin colocalized with the EGFR. Thus, uptake depends on EGFR signaling rather than trafficking along the same pathway. Decorin passes through early endosomes towards trafficking to lysosomes, since more than 50% of decorin colocalized with EEA1. Moreover, inhibition of endosomal fusion by wortmannin caused a profound inhibition of decorin endocytosis. Overexpression of the clathrin-binding Hrs protein, which has previously been shown to inibit EGFR degradation blocked the degradation of decorin. Cholesterol depletion by filipin inhibited uptake of decorin by 34%, however, nearly no intracellular colocalization was found between decorin and caveolin-1. The combined use of filipin and chlorpromazine had an additive inhibitory effect on decorin endocytosis. Moreover, chlorpromazine diverted decorin from the chlorpromazine-sensitive pathway to an alternative uptake route. The CD44/hyaluronan pathway was excluded as an endocytic route for decorin. Our observations indicate that decorin is taken up by more than one endocytic pathway. Of note, lipid-raft-dependent EGFR signaling modulates decorin uptake, suggesting the presence of a potential feedback regulation mechanism for desensitization of signaling events mediated by decorin.

UR - https://www.scopus.com/pages/publications/34247579085

U2 - 10.1016/j.biochi.2006.12.012

DO - 10.1016/j.biochi.2006.12.012

M3 - Journal articles

C2 - 17335953

AN - SCOPUS:34247579085

SN - 0300-9084

VL - 89

SP - 637

EP - 657

JO - Biochimie

JF - Biochimie

IS - 5

ER -

Endocytosis of the dermatan sulfate proteoglycan decorin utilizes multiple pathways and is modulated by epidermal growth factor receptor signaling

Abstract

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