CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis

Glucose transporter 4 (GLUT4) is sequestered inside muscle and fat and then released by vesicle traffic to the cell surface in response to postprandial insulin for blood glucose clearance. Here, we map the biogenesis of this GLUT4 traffic pathway in humans, which involves clathrin isoform CHC22. We...

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Autores principales: Camus, Stéphane M., Camus, Marine D., Figueras-Novoa, Carmen, Boncompain, Gaelle, Sadacca, L. Amanda, Esk, Christopher, Bigot, Anne, Gould, Gwyn W., Kioumourtzoglou, Dimitrios, Perez, Franck, Bryant, Nia J., Mukherjee, Shaeri, Brodsky, Frances M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Rockefeller University Press 2019
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7039200/
https://www.ncbi.nlm.nih.gov/pubmed/31863584
http://dx.doi.org/10.1083/jcb.201812135
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author Camus, Stéphane M.
Camus, Marine D.
Figueras-Novoa, Carmen
Boncompain, Gaelle
Sadacca, L. Amanda
Esk, Christopher
Bigot, Anne
Gould, Gwyn W.
Kioumourtzoglou, Dimitrios
Perez, Franck
Bryant, Nia J.
Mukherjee, Shaeri
Brodsky, Frances M.
author_facet Camus, Stéphane M.
Camus, Marine D.
Figueras-Novoa, Carmen
Boncompain, Gaelle
Sadacca, L. Amanda
Esk, Christopher
Bigot, Anne
Gould, Gwyn W.
Kioumourtzoglou, Dimitrios
Perez, Franck
Bryant, Nia J.
Mukherjee, Shaeri
Brodsky, Frances M.
author_sort Camus, Stéphane M.
collection PubMed
description Glucose transporter 4 (GLUT4) is sequestered inside muscle and fat and then released by vesicle traffic to the cell surface in response to postprandial insulin for blood glucose clearance. Here, we map the biogenesis of this GLUT4 traffic pathway in humans, which involves clathrin isoform CHC22. We observe that GLUT4 transits through the early secretory pathway more slowly than the constitutively secreted GLUT1 transporter and localize CHC22 to the ER-to-Golgi intermediate compartment (ERGIC). CHC22 functions in transport from the ERGIC, as demonstrated by an essential role in forming the replication vacuole of Legionella pneumophila bacteria, which requires ERGIC-derived membrane. CHC22 complexes with ERGIC tether p115, GLUT4, and sortilin, and downregulation of either p115 or CHC22, but not GM130 or sortilin, abrogates insulin-responsive GLUT4 release. This indicates that CHC22 traffic initiates human GLUT4 sequestration from the ERGIC and defines a role for CHC22 in addition to retrograde sorting of GLUT4 after endocytic recapture, enhancing pathways for GLUT4 sequestration in humans relative to mice, which lack CHC22.
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spelling pubmed-70392002020-07-06 CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis Camus, Stéphane M. Camus, Marine D. Figueras-Novoa, Carmen Boncompain, Gaelle Sadacca, L. Amanda Esk, Christopher Bigot, Anne Gould, Gwyn W. Kioumourtzoglou, Dimitrios Perez, Franck Bryant, Nia J. Mukherjee, Shaeri Brodsky, Frances M. J Cell Biol Research Articles Glucose transporter 4 (GLUT4) is sequestered inside muscle and fat and then released by vesicle traffic to the cell surface in response to postprandial insulin for blood glucose clearance. Here, we map the biogenesis of this GLUT4 traffic pathway in humans, which involves clathrin isoform CHC22. We observe that GLUT4 transits through the early secretory pathway more slowly than the constitutively secreted GLUT1 transporter and localize CHC22 to the ER-to-Golgi intermediate compartment (ERGIC). CHC22 functions in transport from the ERGIC, as demonstrated by an essential role in forming the replication vacuole of Legionella pneumophila bacteria, which requires ERGIC-derived membrane. CHC22 complexes with ERGIC tether p115, GLUT4, and sortilin, and downregulation of either p115 or CHC22, but not GM130 or sortilin, abrogates insulin-responsive GLUT4 release. This indicates that CHC22 traffic initiates human GLUT4 sequestration from the ERGIC and defines a role for CHC22 in addition to retrograde sorting of GLUT4 after endocytic recapture, enhancing pathways for GLUT4 sequestration in humans relative to mice, which lack CHC22. Rockefeller University Press 2019-12-19 /pmc/articles/PMC7039200/ /pubmed/31863584 http://dx.doi.org/10.1083/jcb.201812135 Text en © 2019 Camus et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Camus, Stéphane M.
Camus, Marine D.
Figueras-Novoa, Carmen
Boncompain, Gaelle
Sadacca, L. Amanda
Esk, Christopher
Bigot, Anne
Gould, Gwyn W.
Kioumourtzoglou, Dimitrios
Perez, Franck
Bryant, Nia J.
Mukherjee, Shaeri
Brodsky, Frances M.
CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis
title CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis
title_full CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis
title_fullStr CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis
title_full_unstemmed CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis
title_short CHC22 clathrin mediates traffic from early secretory compartments for human GLUT4 pathway biogenesis
title_sort chc22 clathrin mediates traffic from early secretory compartments for human glut4 pathway biogenesis
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7039200/
https://www.ncbi.nlm.nih.gov/pubmed/31863584
http://dx.doi.org/10.1083/jcb.201812135
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