Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome

Small Heat Shock Proteins (sHSPs) are molecular chaperones that transiently interact with other proteins, thereby assisting with quality control of proper protein folding and/or degradation. They are also recruited to protect cells from a variety of stresses in response to extreme heat, heavy metals...

Descripción completa

Detalles Bibliográficos
Autores principales: Grose, Julianne H., Langston, Kelsey, Wang, Xiaohui, Squires, Shayne, Mustafi, Soumyajit Banerjee, Hayes, Whitney, Neubert, Jonathan, Fischer, Susan K., Fasano, Matthew, Saunders, Gina Moore, Dai, Qiang, Christians, Elisabeth, Lewandowski, E. Douglas, Ping, Peipei, Benjamin, Ivor J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4605610/
https://www.ncbi.nlm.nih.gov/pubmed/26465331
http://dx.doi.org/10.1371/journal.pone.0133994
_version_ 1782395226946535424
author Grose, Julianne H.
Langston, Kelsey
Wang, Xiaohui
Squires, Shayne
Mustafi, Soumyajit Banerjee
Hayes, Whitney
Neubert, Jonathan
Fischer, Susan K.
Fasano, Matthew
Saunders, Gina Moore
Dai, Qiang
Christians, Elisabeth
Lewandowski, E. Douglas
Ping, Peipei
Benjamin, Ivor J.
author_facet Grose, Julianne H.
Langston, Kelsey
Wang, Xiaohui
Squires, Shayne
Mustafi, Soumyajit Banerjee
Hayes, Whitney
Neubert, Jonathan
Fischer, Susan K.
Fasano, Matthew
Saunders, Gina Moore
Dai, Qiang
Christians, Elisabeth
Lewandowski, E. Douglas
Ping, Peipei
Benjamin, Ivor J.
author_sort Grose, Julianne H.
collection PubMed
description Small Heat Shock Proteins (sHSPs) are molecular chaperones that transiently interact with other proteins, thereby assisting with quality control of proper protein folding and/or degradation. They are also recruited to protect cells from a variety of stresses in response to extreme heat, heavy metals, and oxidative-reductive stress. Although ten human sHSPs have been identified, their likely diverse biological functions remain an enigma in health and disease, and much less is known about non-redundant roles in selective cells and tissues. Herein, we set out to comprehensively characterize the cardiac-restricted Heat Shock Protein B-2 (HspB2), which exhibited ischemic cardioprotection in transgenic overexpressing mice including reduced infarct size and maintenance of ATP levels. Global yeast two-hybrid analysis using HspB2 (bait) and a human cardiac library (prey) coupled with co-immunoprecipitation studies for mitochondrial target validation revealed the first HspB2 “cardiac interactome” to contain many myofibril and mitochondrial-binding partners consistent with the overexpression phenotype. This interactome has been submitted to the Biological General Repository for Interaction Datasets (BioGRID). A related sHSP chaperone HspB5 had only partially overlapping binding partners, supporting specificity of the interactome as well as non-redundant roles reported for these sHSPs. Evidence that the cardiac yeast two-hybrid HspB2 interactome targets resident mitochondrial client proteins is consistent with the role of HspB2 in maintaining ATP levels and suggests new chaperone-dependent functions for metabolic homeostasis. One of the HspB2 targets, glyceraldehyde 3-phosphate dehydrogenase (GAPDH), has reported roles in HspB2 associated phenotypes including cardiac ATP production, mitochondrial function, and apoptosis, and was validated as a potential client protein of HspB2 through chaperone assays. From the clientele and phenotypes identified herein, it is tempting to speculate that small molecule activators of HspB2 might be deployed to mitigate mitochondrial related diseases such as cardiomyopathy and neurodegenerative disease.
format Online
Article
Text
id pubmed-4605610
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-46056102015-10-29 Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome Grose, Julianne H. Langston, Kelsey Wang, Xiaohui Squires, Shayne Mustafi, Soumyajit Banerjee Hayes, Whitney Neubert, Jonathan Fischer, Susan K. Fasano, Matthew Saunders, Gina Moore Dai, Qiang Christians, Elisabeth Lewandowski, E. Douglas Ping, Peipei Benjamin, Ivor J. PLoS One Research Article Small Heat Shock Proteins (sHSPs) are molecular chaperones that transiently interact with other proteins, thereby assisting with quality control of proper protein folding and/or degradation. They are also recruited to protect cells from a variety of stresses in response to extreme heat, heavy metals, and oxidative-reductive stress. Although ten human sHSPs have been identified, their likely diverse biological functions remain an enigma in health and disease, and much less is known about non-redundant roles in selective cells and tissues. Herein, we set out to comprehensively characterize the cardiac-restricted Heat Shock Protein B-2 (HspB2), which exhibited ischemic cardioprotection in transgenic overexpressing mice including reduced infarct size and maintenance of ATP levels. Global yeast two-hybrid analysis using HspB2 (bait) and a human cardiac library (prey) coupled with co-immunoprecipitation studies for mitochondrial target validation revealed the first HspB2 “cardiac interactome” to contain many myofibril and mitochondrial-binding partners consistent with the overexpression phenotype. This interactome has been submitted to the Biological General Repository for Interaction Datasets (BioGRID). A related sHSP chaperone HspB5 had only partially overlapping binding partners, supporting specificity of the interactome as well as non-redundant roles reported for these sHSPs. Evidence that the cardiac yeast two-hybrid HspB2 interactome targets resident mitochondrial client proteins is consistent with the role of HspB2 in maintaining ATP levels and suggests new chaperone-dependent functions for metabolic homeostasis. One of the HspB2 targets, glyceraldehyde 3-phosphate dehydrogenase (GAPDH), has reported roles in HspB2 associated phenotypes including cardiac ATP production, mitochondrial function, and apoptosis, and was validated as a potential client protein of HspB2 through chaperone assays. From the clientele and phenotypes identified herein, it is tempting to speculate that small molecule activators of HspB2 might be deployed to mitigate mitochondrial related diseases such as cardiomyopathy and neurodegenerative disease. Public Library of Science 2015-10-14 /pmc/articles/PMC4605610/ /pubmed/26465331 http://dx.doi.org/10.1371/journal.pone.0133994 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Grose, Julianne H.
Langston, Kelsey
Wang, Xiaohui
Squires, Shayne
Mustafi, Soumyajit Banerjee
Hayes, Whitney
Neubert, Jonathan
Fischer, Susan K.
Fasano, Matthew
Saunders, Gina Moore
Dai, Qiang
Christians, Elisabeth
Lewandowski, E. Douglas
Ping, Peipei
Benjamin, Ivor J.
Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome
title Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome
title_full Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome
title_fullStr Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome
title_full_unstemmed Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome
title_short Characterization of the Cardiac Overexpression of HSPB2 Reveals Mitochondrial and Myogenic Roles Supported by a Cardiac HspB2 Interactome
title_sort characterization of the cardiac overexpression of hspb2 reveals mitochondrial and myogenic roles supported by a cardiac hspb2 interactome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4605610/
https://www.ncbi.nlm.nih.gov/pubmed/26465331
http://dx.doi.org/10.1371/journal.pone.0133994
work_keys_str_mv AT grosejulianneh characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT langstonkelsey characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT wangxiaohui characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT squiresshayne characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT mustafisoumyajitbanerjee characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT hayeswhitney characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT neubertjonathan characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT fischersusank characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT fasanomatthew characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT saundersginamoore characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT daiqiang characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT christianselisabeth characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT lewandowskiedouglas characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT pingpeipei characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome
AT benjaminivorj characterizationofthecardiacoverexpressionofhspb2revealsmitochondrialandmyogenicrolessupportedbyacardiachspb2interactome

Ejemplares similares