Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.

Detalhes bibliográficos
Autor(a) principal: Festuccia, William Tadeu Lara
Data de Publicação: 2009
Outros Autores: Laplante, Mathieu, Brûlé, Sophie, Houde, Vanessa P., Achouba, Adel, Lachance, Dominic, Pedrosa, Maria Lúcia, Silva, Marcelo Eustáquio, Cota, Renata Guerra de Sá, Couet, Jacques, Arsenault, Marie, Marette, André, Deshaies, Yves
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UFOP
Texto Completo: http://www.repositorio.ufop.br/handle/123456789/4606
https://doi.org/10.1016/j.yjmcc.2009.04.011
Resumo: We investigated cardiac hypertrophy elicited by rosiglitazone treatment at the level of protein synthesis/ degradation, mTOR, MAPK and AMPK signalling pathways, cardiac function and aspects of carbohydrate/ lipid metabolism. Hearts of rats treated or not with rosiglitazone (15 mg/kg day) for 21 days were evaluated for gene expression, protein synthesis, proteasome and calpain activities, signalling pathways, and function by echocardiography. Rosiglitazone induced eccentric heart hypertrophy associated with increased expression of ANP, BNP, collagen I and III and fibronectin, reduced heart rate and increased stroke volume. Rosiglitazone robustly increased heart glycogen content (∼400%), an effect associated with increases in glycogenin and UDPG-PPL mRNA levels and glucose uptake, and a reduction in glycogen phosphorylase expression and activity. Cardiac triglyceride content, lipoprotein lipase activity and mRNA levels of enzymes involved in fatty acid oxidation were also reduced by the agonist. Rosiglitazone-induced cardiac hypertrophy was associated with an increase in myofibrillar protein content and turnover (increased synthesis and an enhancement of calpain-mediated myofibrillar degradation). In contrast, 26S β5 chymotryptic proteasome activity and mRNA levels of 20S β2 and β5 and 19S RPN 2 proteasome subunits along with the ubiquitin ligases atrogin and CHIP were all reduced by rosiglitazone. These morphological and biochemical changes were associated with marked activation of the key growth-promoting mTOR signalling pathway, whose pharmacological inhibition with rapamycin completely blocked cardiac hypertrophy induced by rosiglitazone. The study demonstrates that both arms of protein balance are involved in rosiglitazone-induced cardiac hypertrophy, and establishes the mTOR pathway as a novel important mediator therein.
id UFOP_f30f0c64be37b90d97794493971ca27a
oai_identifier_str oai:repositorio.ufop.br:123456789/4606
network_acronym_str UFOP
network_name_str Repositório Institucional da UFOP
repository_id_str 3233
spelling Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.Protein synthesisCalpain/calpastatinProteasomeGlycogenRapamycinWe investigated cardiac hypertrophy elicited by rosiglitazone treatment at the level of protein synthesis/ degradation, mTOR, MAPK and AMPK signalling pathways, cardiac function and aspects of carbohydrate/ lipid metabolism. Hearts of rats treated or not with rosiglitazone (15 mg/kg day) for 21 days were evaluated for gene expression, protein synthesis, proteasome and calpain activities, signalling pathways, and function by echocardiography. Rosiglitazone induced eccentric heart hypertrophy associated with increased expression of ANP, BNP, collagen I and III and fibronectin, reduced heart rate and increased stroke volume. Rosiglitazone robustly increased heart glycogen content (∼400%), an effect associated with increases in glycogenin and UDPG-PPL mRNA levels and glucose uptake, and a reduction in glycogen phosphorylase expression and activity. Cardiac triglyceride content, lipoprotein lipase activity and mRNA levels of enzymes involved in fatty acid oxidation were also reduced by the agonist. Rosiglitazone-induced cardiac hypertrophy was associated with an increase in myofibrillar protein content and turnover (increased synthesis and an enhancement of calpain-mediated myofibrillar degradation). In contrast, 26S β5 chymotryptic proteasome activity and mRNA levels of 20S β2 and β5 and 19S RPN 2 proteasome subunits along with the ubiquitin ligases atrogin and CHIP were all reduced by rosiglitazone. These morphological and biochemical changes were associated with marked activation of the key growth-promoting mTOR signalling pathway, whose pharmacological inhibition with rapamycin completely blocked cardiac hypertrophy induced by rosiglitazone. The study demonstrates that both arms of protein balance are involved in rosiglitazone-induced cardiac hypertrophy, and establishes the mTOR pathway as a novel important mediator therein.2015-03-12T18:50:42Z2015-03-12T18:50:42Z2009info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/articleapplication/pdfFESTUCCIA, W. T. L. et al. Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation. Journal of Molecular and Cellular Cardiology, v. 47, p. 85-95, 2009. Disponível em: <http://www.sciencedirect.com/science/article/pii/S0022282809001837>. Acesso em: 08 nov. 2014.0022-2828http://www.repositorio.ufop.br/handle/123456789/4606https://doi.org/10.1016/j.yjmcc.2009.04.011O periódico Journal of Molecular and Cellular Cardiology concede permissão para depósito deste artigo no Repositório Institucional da UFOP. Número da licença: 3530901251605.info:eu-repo/semantics/openAccessFestuccia, William Tadeu LaraLaplante, MathieuBrûlé, SophieHoude, Vanessa P.Achouba, AdelLachance, DominicPedrosa, Maria LúciaSilva, Marcelo EustáquioCota, Renata Guerra de SáCouet, JacquesArsenault, MarieMarette, AndréDeshaies, Yvesengreponame:Repositório Institucional da UFOPinstname:Universidade Federal de Ouro Preto (UFOP)instacron:UFOP2019-06-24T18:02:04Zoai:repositorio.ufop.br:123456789/4606Repositório InstitucionalPUBhttp://www.repositorio.ufop.br/oai/requestrepositorio@ufop.edu.bropendoar:32332019-06-24T18:02:04Repositório Institucional da UFOP - Universidade Federal de Ouro Preto (UFOP)false
dc.title.none.fl_str_mv Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
title Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
spellingShingle Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
Festuccia, William Tadeu Lara
Protein synthesis
Calpain/calpastatin
Proteasome
Glycogen
Rapamycin
title_short Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
title_full Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
title_fullStr Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
title_full_unstemmed Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
title_sort Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation.
author Festuccia, William Tadeu Lara
author_facet Festuccia, William Tadeu Lara
Laplante, Mathieu
Brûlé, Sophie
Houde, Vanessa P.
Achouba, Adel
Lachance, Dominic
Pedrosa, Maria Lúcia
Silva, Marcelo Eustáquio
Cota, Renata Guerra de Sá
Couet, Jacques
Arsenault, Marie
Marette, André
Deshaies, Yves
author_role author
author2 Laplante, Mathieu
Brûlé, Sophie
Houde, Vanessa P.
Achouba, Adel
Lachance, Dominic
Pedrosa, Maria Lúcia
Silva, Marcelo Eustáquio
Cota, Renata Guerra de Sá
Couet, Jacques
Arsenault, Marie
Marette, André
Deshaies, Yves
author2_role author
author
author
author
author
author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Festuccia, William Tadeu Lara
Laplante, Mathieu
Brûlé, Sophie
Houde, Vanessa P.
Achouba, Adel
Lachance, Dominic
Pedrosa, Maria Lúcia
Silva, Marcelo Eustáquio
Cota, Renata Guerra de Sá
Couet, Jacques
Arsenault, Marie
Marette, André
Deshaies, Yves
dc.subject.por.fl_str_mv Protein synthesis
Calpain/calpastatin
Proteasome
Glycogen
Rapamycin
topic Protein synthesis
Calpain/calpastatin
Proteasome
Glycogen
Rapamycin
description We investigated cardiac hypertrophy elicited by rosiglitazone treatment at the level of protein synthesis/ degradation, mTOR, MAPK and AMPK signalling pathways, cardiac function and aspects of carbohydrate/ lipid metabolism. Hearts of rats treated or not with rosiglitazone (15 mg/kg day) for 21 days were evaluated for gene expression, protein synthesis, proteasome and calpain activities, signalling pathways, and function by echocardiography. Rosiglitazone induced eccentric heart hypertrophy associated with increased expression of ANP, BNP, collagen I and III and fibronectin, reduced heart rate and increased stroke volume. Rosiglitazone robustly increased heart glycogen content (∼400%), an effect associated with increases in glycogenin and UDPG-PPL mRNA levels and glucose uptake, and a reduction in glycogen phosphorylase expression and activity. Cardiac triglyceride content, lipoprotein lipase activity and mRNA levels of enzymes involved in fatty acid oxidation were also reduced by the agonist. Rosiglitazone-induced cardiac hypertrophy was associated with an increase in myofibrillar protein content and turnover (increased synthesis and an enhancement of calpain-mediated myofibrillar degradation). In contrast, 26S β5 chymotryptic proteasome activity and mRNA levels of 20S β2 and β5 and 19S RPN 2 proteasome subunits along with the ubiquitin ligases atrogin and CHIP were all reduced by rosiglitazone. These morphological and biochemical changes were associated with marked activation of the key growth-promoting mTOR signalling pathway, whose pharmacological inhibition with rapamycin completely blocked cardiac hypertrophy induced by rosiglitazone. The study demonstrates that both arms of protein balance are involved in rosiglitazone-induced cardiac hypertrophy, and establishes the mTOR pathway as a novel important mediator therein.
publishDate 2009
dc.date.none.fl_str_mv 2009
2015-03-12T18:50:42Z
2015-03-12T18:50:42Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
format article
status_str publishedVersion
dc.identifier.uri.fl_str_mv FESTUCCIA, W. T. L. et al. Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation. Journal of Molecular and Cellular Cardiology, v. 47, p. 85-95, 2009. Disponível em: <http://www.sciencedirect.com/science/article/pii/S0022282809001837>. Acesso em: 08 nov. 2014.
0022-2828
http://www.repositorio.ufop.br/handle/123456789/4606
https://doi.org/10.1016/j.yjmcc.2009.04.011
identifier_str_mv FESTUCCIA, W. T. L. et al. Rosiglitazone-induced heart remodelling is associated with enhanced turnover of myofibrillar protein and mTOR activation. Journal of Molecular and Cellular Cardiology, v. 47, p. 85-95, 2009. Disponível em: <http://www.sciencedirect.com/science/article/pii/S0022282809001837>. Acesso em: 08 nov. 2014.
0022-2828
url http://www.repositorio.ufop.br/handle/123456789/4606
https://doi.org/10.1016/j.yjmcc.2009.04.011
dc.language.iso.fl_str_mv eng
language eng
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.source.none.fl_str_mv reponame:Repositório Institucional da UFOP
instname:Universidade Federal de Ouro Preto (UFOP)
instacron:UFOP
instname_str Universidade Federal de Ouro Preto (UFOP)
instacron_str UFOP
institution UFOP
reponame_str Repositório Institucional da UFOP
collection Repositório Institucional da UFOP
repository.name.fl_str_mv Repositório Institucional da UFOP - Universidade Federal de Ouro Preto (UFOP)
repository.mail.fl_str_mv repositorio@ufop.edu.br
_version_ 1813002863221145600

Registros relacionados