A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes

Despite the identification of many susceptibility genes our knowledge of the underlying mechanisms responsible for complex disease remains limited. Here, we identified a type 2 diabetes disease module in endosomes, and validate it for functional relevance on selected nodes. Using hepatic Golgi/endos...

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Autores principales: Boutchueng-Djidjou, Martial, Belleau, Pascal, Bilodeau, Nicolas, Fortier, Suzanne, Bourassa, Sylvie, Droit, Arnaud, Elowe, Sabine, Faure, Robert L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6177195/
https://www.ncbi.nlm.nih.gov/pubmed/30300385
http://dx.doi.org/10.1371/journal.pone.0205180
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author Boutchueng-Djidjou, Martial
Belleau, Pascal
Bilodeau, Nicolas
Fortier, Suzanne
Bourassa, Sylvie
Droit, Arnaud
Elowe, Sabine
Faure, Robert L.
author_facet Boutchueng-Djidjou, Martial
Belleau, Pascal
Bilodeau, Nicolas
Fortier, Suzanne
Bourassa, Sylvie
Droit, Arnaud
Elowe, Sabine
Faure, Robert L.
author_sort Boutchueng-Djidjou, Martial
collection PubMed
description Despite the identification of many susceptibility genes our knowledge of the underlying mechanisms responsible for complex disease remains limited. Here, we identified a type 2 diabetes disease module in endosomes, and validate it for functional relevance on selected nodes. Using hepatic Golgi/endosomes fractions, we established a proteome of insulin receptor-containing endosomes that allowed the study of physical protein interaction networks on a type 2 diabetes background. The resulting collated network is formed by 313 nodes and 1147 edges with a topology organized around a few major hubs with Cdk2 displaying the highest collective influence. Overall, 88% of the nodes are associated with the type 2 diabetes genetic risk, including 101 new candidates. The Type 2 diabetes module is enriched with cytoskeleton and luminal acidification–dependent processes that are shared with secretion-related mechanisms. We identified new signaling pathways driven by Cdk2 and PTPLAD1 whose expression affects the association of the insulin receptor with TUBA, TUBB, the actin component ACTB and the endosomal sorting markers Rab5c and Rab11a. Therefore, the interactome of internalized insulin receptors reveals the presence of a type 2 diabetes disease module enriched in new layers of feedback loops required for insulin signaling, clearance and islet biology.
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spelling pubmed-61771952018-10-19 A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes Boutchueng-Djidjou, Martial Belleau, Pascal Bilodeau, Nicolas Fortier, Suzanne Bourassa, Sylvie Droit, Arnaud Elowe, Sabine Faure, Robert L. PLoS One Research Article Despite the identification of many susceptibility genes our knowledge of the underlying mechanisms responsible for complex disease remains limited. Here, we identified a type 2 diabetes disease module in endosomes, and validate it for functional relevance on selected nodes. Using hepatic Golgi/endosomes fractions, we established a proteome of insulin receptor-containing endosomes that allowed the study of physical protein interaction networks on a type 2 diabetes background. The resulting collated network is formed by 313 nodes and 1147 edges with a topology organized around a few major hubs with Cdk2 displaying the highest collective influence. Overall, 88% of the nodes are associated with the type 2 diabetes genetic risk, including 101 new candidates. The Type 2 diabetes module is enriched with cytoskeleton and luminal acidification–dependent processes that are shared with secretion-related mechanisms. We identified new signaling pathways driven by Cdk2 and PTPLAD1 whose expression affects the association of the insulin receptor with TUBA, TUBB, the actin component ACTB and the endosomal sorting markers Rab5c and Rab11a. Therefore, the interactome of internalized insulin receptors reveals the presence of a type 2 diabetes disease module enriched in new layers of feedback loops required for insulin signaling, clearance and islet biology. Public Library of Science 2018-10-09 /pmc/articles/PMC6177195/ /pubmed/30300385 http://dx.doi.org/10.1371/journal.pone.0205180 Text en © 2018 Boutchueng-Djidjou et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Boutchueng-Djidjou, Martial
Belleau, Pascal
Bilodeau, Nicolas
Fortier, Suzanne
Bourassa, Sylvie
Droit, Arnaud
Elowe, Sabine
Faure, Robert L.
A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes
title A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes
title_full A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes
title_fullStr A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes
title_full_unstemmed A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes
title_short A type 2 diabetes disease module with a high collective influence for Cdk2 and PTPLAD1 is localized in endosomes
title_sort type 2 diabetes disease module with a high collective influence for cdk2 and ptplad1 is localized in endosomes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6177195/
https://www.ncbi.nlm.nih.gov/pubmed/30300385
http://dx.doi.org/10.1371/journal.pone.0205180
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