The role of proteasome in muscle wasting of experimental arthritis

Detalhes bibliográficos
Autor(a) principal: Teixeira, Vivian de Oliveira Nunes
Data de Publicação: 2023
Outros Autores: Bartikoski, Bárbara Jonson, Espírito Santo, Rafaela Cavalheiro do, Alabarse, Paulo Vinicius Gil, Ghannan, Khetam, Silva, Jordana Miranda de Souza, Filippin, Lidiane Isabel, Visioli, Fernanda, Martinez-Gamboa, Lorena, Feist, Eugen, Xavier, Ricardo Machado
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UFRGS
Texto Completo: http://hdl.handle.net/10183/274323
Resumo: Background Rheumatoid arthritis is an autoimmune infammatory disease that often leads patients to muscle impairment and physical disability. This study aimed to evaluate changes in the activity of proteasome system in skel‑ etal muscles of mice with collagen-induced arthritis (CIA) and treated with etanercept or methotrexate. Methods Male DBA1/J mice were divided into four groups (n=8 each): CIA-Vehicle (treated with saline), CIA-ETN (treated with etanercept, 5.5 mg/kg), CIA-MTX (treated with methotrexate, 35 mg/kg) and CO (healthy control group). Mice were treated two times a week for 6 weeks. Clinical score and hind paw edema were measured. Muscles were weighted after euthanasia and used to quantify proteasome activity, gene (MuRF-1, PMSα4, PSMβ5, PMSβ6, PSMβ7, PSMβ8, PSMβ9, and PSMβ10), and protein (PSMβ1, PSMβ5, PSMβ1i, PSMβ5i) expression of proteasome subunits. Results Both treatments slowed disease development, but only CIA-ETN maintained muscle weight compared to CIA-MTX and CIA-Vehicle groups. Etanercept treatment showed caspase-like activity of 26S proteasome similar to CO group, while CIA-Vehicle and CIA-MTX had higher activity compared to CO group (p: 0.0057). MuRF-1 mRNA expression was decreased after etanercept administration compared to CIA-Vehicle and CO groups (p: 0.002, p: 0.007, respectively). PSMβ8 and PSMβ9 mRNA levels were increased in CIA-Vehicle and CIA-MTX compared to CO group, while CIA-ETN presented no diference from CO. PMSβ6 mRNA expression was higher in CIA-Vehicle and CIA-MTX groups than in CO group. Protein levels of the PSMβ5 subunit were increased in CO group compared to CIA-Vehicle; after both etanercept and methotrexate treatments, PSMβ5 expression was higher than in CIA-Vehicle group and did not difer from CO group expression (p: 0.0025, p: 0.001, respectively). The infammation-induced subunit β1 (LMP2) was enhanced after methotrexate treatment compared to CO group (p: 0.043). Conclusions The results of CIA-Vehicle show that arthritis increases muscle proteasome activation by enhanced cas‑ pase-like activity of 26S proteasome and increased PSMβ8 and PSMβ9 mRNA levels. Etanercept treatment was able to maintain the muscle weight and to modulate proteasome so that its activity and gene expression were compared to CO after TNF inhibition. The protein expression of infammation-induced proteasome subunit was increased in muscle of CIA-MTX group but not following etanercept treatment. Thus, anti-TNF treatment may be an interesting approach to attenuate the arthritis-related muscle wasting.
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spelling Teixeira, Vivian de Oliveira NunesBartikoski, Bárbara JonsonEspírito Santo, Rafaela Cavalheiro doAlabarse, Paulo Vinicius GilGhannan, KhetamSilva, Jordana Miranda de SouzaFilippin, Lidiane IsabelVisioli, FernandaMartinez-Gamboa, LorenaFeist, EugenXavier, Ricardo Machado2024-03-28T06:24:11Z20232523-3106http://hdl.handle.net/10183/274323001199222Background Rheumatoid arthritis is an autoimmune infammatory disease that often leads patients to muscle impairment and physical disability. This study aimed to evaluate changes in the activity of proteasome system in skel‑ etal muscles of mice with collagen-induced arthritis (CIA) and treated with etanercept or methotrexate. Methods Male DBA1/J mice were divided into four groups (n=8 each): CIA-Vehicle (treated with saline), CIA-ETN (treated with etanercept, 5.5 mg/kg), CIA-MTX (treated with methotrexate, 35 mg/kg) and CO (healthy control group). Mice were treated two times a week for 6 weeks. Clinical score and hind paw edema were measured. Muscles were weighted after euthanasia and used to quantify proteasome activity, gene (MuRF-1, PMSα4, PSMβ5, PMSβ6, PSMβ7, PSMβ8, PSMβ9, and PSMβ10), and protein (PSMβ1, PSMβ5, PSMβ1i, PSMβ5i) expression of proteasome subunits. Results Both treatments slowed disease development, but only CIA-ETN maintained muscle weight compared to CIA-MTX and CIA-Vehicle groups. Etanercept treatment showed caspase-like activity of 26S proteasome similar to CO group, while CIA-Vehicle and CIA-MTX had higher activity compared to CO group (p: 0.0057). MuRF-1 mRNA expression was decreased after etanercept administration compared to CIA-Vehicle and CO groups (p: 0.002, p: 0.007, respectively). PSMβ8 and PSMβ9 mRNA levels were increased in CIA-Vehicle and CIA-MTX compared to CO group, while CIA-ETN presented no diference from CO. PMSβ6 mRNA expression was higher in CIA-Vehicle and CIA-MTX groups than in CO group. Protein levels of the PSMβ5 subunit were increased in CO group compared to CIA-Vehicle; after both etanercept and methotrexate treatments, PSMβ5 expression was higher than in CIA-Vehicle group and did not difer from CO group expression (p: 0.0025, p: 0.001, respectively). The infammation-induced subunit β1 (LMP2) was enhanced after methotrexate treatment compared to CO group (p: 0.043). Conclusions The results of CIA-Vehicle show that arthritis increases muscle proteasome activation by enhanced cas‑ pase-like activity of 26S proteasome and increased PSMβ8 and PSMβ9 mRNA levels. Etanercept treatment was able to maintain the muscle weight and to modulate proteasome so that its activity and gene expression were compared to CO after TNF inhibition. The protein expression of infammation-induced proteasome subunit was increased in muscle of CIA-MTX group but not following etanercept treatment. Thus, anti-TNF treatment may be an interesting approach to attenuate the arthritis-related muscle wasting.application/pdfengAdvances in rheumatology. São Paulo. Vol. 63 (2023), 14, 12 p.Artrite experimentalInibidores do fator de necrose tumoralAtrofia muscularExperimental arthritisMuscle wastingProteasomeTNF inhibitorThe role of proteasome in muscle wasting of experimental arthritisinfo:eu-repo/semantics/articleinfo:eu-repo/semantics/otherinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFRGSinstname:Universidade Federal do Rio Grande do Sul (UFRGS)instacron:UFRGSTEXT001199222.pdf.txt001199222.pdf.txtExtracted Texttext/plain50562http://www.lume.ufrgs.br/bitstream/10183/274323/2/001199222.pdf.txtab39a811f1e263aa9790e48318fabd07MD52ORIGINAL001199222.pdfTexto completo (inglês)application/pdf1540382http://www.lume.ufrgs.br/bitstream/10183/274323/1/001199222.pdfef1f7da32505348f9af24555f0101d83MD5110183/2743232024-03-29 06:19:29.754689oai:www.lume.ufrgs.br:10183/274323Repositório de PublicaçõesPUBhttps://lume.ufrgs.br/oai/requestopendoar:2024-03-29T09:19:29Repositório Institucional da UFRGS - Universidade Federal do Rio Grande do Sul (UFRGS)false
dc.title.pt_BR.fl_str_mv The role of proteasome in muscle wasting of experimental arthritis
title The role of proteasome in muscle wasting of experimental arthritis
spellingShingle The role of proteasome in muscle wasting of experimental arthritis
Teixeira, Vivian de Oliveira Nunes
Artrite experimental
Inibidores do fator de necrose tumoral
Atrofia muscular
Experimental arthritis
Muscle wasting
Proteasome
TNF inhibitor
title_short The role of proteasome in muscle wasting of experimental arthritis
title_full The role of proteasome in muscle wasting of experimental arthritis
title_fullStr The role of proteasome in muscle wasting of experimental arthritis
title_full_unstemmed The role of proteasome in muscle wasting of experimental arthritis
title_sort The role of proteasome in muscle wasting of experimental arthritis
author Teixeira, Vivian de Oliveira Nunes
author_facet Teixeira, Vivian de Oliveira Nunes
Bartikoski, Bárbara Jonson
Espírito Santo, Rafaela Cavalheiro do
Alabarse, Paulo Vinicius Gil
Ghannan, Khetam
Silva, Jordana Miranda de Souza
Filippin, Lidiane Isabel
Visioli, Fernanda
Martinez-Gamboa, Lorena
Feist, Eugen
Xavier, Ricardo Machado
author_role author
author2 Bartikoski, Bárbara Jonson
Espírito Santo, Rafaela Cavalheiro do
Alabarse, Paulo Vinicius Gil
Ghannan, Khetam
Silva, Jordana Miranda de Souza
Filippin, Lidiane Isabel
Visioli, Fernanda
Martinez-Gamboa, Lorena
Feist, Eugen
Xavier, Ricardo Machado
author2_role author
author
author
author
author
author
author
author
author
author
dc.contributor.author.fl_str_mv Teixeira, Vivian de Oliveira Nunes
Bartikoski, Bárbara Jonson
Espírito Santo, Rafaela Cavalheiro do
Alabarse, Paulo Vinicius Gil
Ghannan, Khetam
Silva, Jordana Miranda de Souza
Filippin, Lidiane Isabel
Visioli, Fernanda
Martinez-Gamboa, Lorena
Feist, Eugen
Xavier, Ricardo Machado
dc.subject.por.fl_str_mv Artrite experimental
Inibidores do fator de necrose tumoral
Atrofia muscular
topic Artrite experimental
Inibidores do fator de necrose tumoral
Atrofia muscular
Experimental arthritis
Muscle wasting
Proteasome
TNF inhibitor
dc.subject.eng.fl_str_mv Experimental arthritis
Muscle wasting
Proteasome
TNF inhibitor
description Background Rheumatoid arthritis is an autoimmune infammatory disease that often leads patients to muscle impairment and physical disability. This study aimed to evaluate changes in the activity of proteasome system in skel‑ etal muscles of mice with collagen-induced arthritis (CIA) and treated with etanercept or methotrexate. Methods Male DBA1/J mice were divided into four groups (n=8 each): CIA-Vehicle (treated with saline), CIA-ETN (treated with etanercept, 5.5 mg/kg), CIA-MTX (treated with methotrexate, 35 mg/kg) and CO (healthy control group). Mice were treated two times a week for 6 weeks. Clinical score and hind paw edema were measured. Muscles were weighted after euthanasia and used to quantify proteasome activity, gene (MuRF-1, PMSα4, PSMβ5, PMSβ6, PSMβ7, PSMβ8, PSMβ9, and PSMβ10), and protein (PSMβ1, PSMβ5, PSMβ1i, PSMβ5i) expression of proteasome subunits. Results Both treatments slowed disease development, but only CIA-ETN maintained muscle weight compared to CIA-MTX and CIA-Vehicle groups. Etanercept treatment showed caspase-like activity of 26S proteasome similar to CO group, while CIA-Vehicle and CIA-MTX had higher activity compared to CO group (p: 0.0057). MuRF-1 mRNA expression was decreased after etanercept administration compared to CIA-Vehicle and CO groups (p: 0.002, p: 0.007, respectively). PSMβ8 and PSMβ9 mRNA levels were increased in CIA-Vehicle and CIA-MTX compared to CO group, while CIA-ETN presented no diference from CO. PMSβ6 mRNA expression was higher in CIA-Vehicle and CIA-MTX groups than in CO group. Protein levels of the PSMβ5 subunit were increased in CO group compared to CIA-Vehicle; after both etanercept and methotrexate treatments, PSMβ5 expression was higher than in CIA-Vehicle group and did not difer from CO group expression (p: 0.0025, p: 0.001, respectively). The infammation-induced subunit β1 (LMP2) was enhanced after methotrexate treatment compared to CO group (p: 0.043). Conclusions The results of CIA-Vehicle show that arthritis increases muscle proteasome activation by enhanced cas‑ pase-like activity of 26S proteasome and increased PSMβ8 and PSMβ9 mRNA levels. Etanercept treatment was able to maintain the muscle weight and to modulate proteasome so that its activity and gene expression were compared to CO after TNF inhibition. The protein expression of infammation-induced proteasome subunit was increased in muscle of CIA-MTX group but not following etanercept treatment. Thus, anti-TNF treatment may be an interesting approach to attenuate the arthritis-related muscle wasting.
publishDate 2023
dc.date.issued.fl_str_mv 2023
dc.date.accessioned.fl_str_mv 2024-03-28T06:24:11Z
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
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dc.identifier.uri.fl_str_mv http://hdl.handle.net/10183/274323
dc.identifier.issn.pt_BR.fl_str_mv 2523-3106
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dc.language.iso.fl_str_mv eng
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dc.relation.ispartof.pt_BR.fl_str_mv Advances in rheumatology. São Paulo. Vol. 63 (2023), 14, 12 p.
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eu_rights_str_mv openAccess
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