Efeitos de derivados do composto arylpyrazole (modulador seletivo do receptor de glicocorticóide) sobre a atrofia muscular esquelética.

Guilherme, João Paulo Limongi França

doi:10.11606/D.42.2012.tde-30012013-081433

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Master's Dissertation

DOI

https://doi.org/10.11606/D.42.2012.tde-30012013-081433

Document

Master's Dissertation

Author

Guilherme, João Paulo Limongi França (Catálogo USP)

Full name

João Paulo Limongi França Guilherme

Institute/School/College

Instituto de Ciências Biomédicas

Knowledge Area

Cell and Tissue Biology

Date of Defense

2012-09-25

Published

São Paulo, 2012

Supervisor

Moriscot, Anselmo Sigari (Catálogo USP)

Committee

Moriscot, Anselmo Sigari (President)
Lopes, Marilene Hohmuth
Silva, Magnus Régios Dias da

Title in Portuguese

Efeitos de derivados do composto arylpyrazole (modulador seletivo do receptor de glicocorticóide) sobre a atrofia muscular esquelética.

Keywords in Portuguese

Atrofia muscular
Hormônios glicocorticóides
Músculo esquelético

Abstract in Portuguese

Neste estudo, testamos dois novos moduladores seletivos do receptor de glicocorticóide, nomeados L5 e L7, em comparação com o dexametasona, sobre aspectos estruturais, funcionais e moleculares no músculo sóleo. Ratos Wistar foram tratados com doses progressivas de dexametasona, L5 e L7 em 1 ou 7 dias. A massa corporal e a ingestão alimentar apresentaram queda após o tratamento com dexametasona em todas as doses; os tratamentos com L5/L7 mostraram resposta semelhante aos controles. O peso do músculo foi diminuído pelo dexametasona, efeito não observado nos tratamentos com L5/L7. Apenas o tratamento com dexametasona causou uma diminuição na área de secção transversa dos tipos de fibra muscular analisada. A força tetânica do sóleo foi diminuída pela dexametasona, nos tratamentos com L5/L7 este parâmetro também não foi afetado. A expressão gênica de MAFbx/Atrogin-1 e MuRF-1 foi elevada pela dexametasona; por outro lado, L5/L7 não elevaram a expressão destes genes. Concluímos que o L5/L7, em contraste com o dexametasona, preveniu o músculo esquelético da atrofia.

Title in English

In vivo effects of two novel arylpyrazole glucocorticoid receptor modulators on skeletal muscle structure and function.

Keywords in English

Glucocorticoid hormones
Muscle atrophy
Skeletal muscle

Abstract in English

In this study, we have tested two new selective modulators named L5 and L7 along with dexamethasone in skeletal muscle structural, functional and molecular aspects. Male Wistar rats were treated with progressive doses of dexamethasone, L5 and L7 for 1 and 7 days. While body weight and food intake were decreased by the dexamethasone treatment in all doses, L5/L7 treatments induced gain in body weight similarly to controls. Muscle weight was decreased by dexamethasone, while L5/L7 were ineffective. Only the dexamethasone treatment caused a decrease in the analyzed cross sectional area of the skeletal muscle fiber types. Soleus tetanic force was decreased by the dexamethasone treatment, while L5/L7 treatments did not alter this parameter. MAFbx/Atrogin-1 and MuRF-1 gene expressions were elevated by dexamethasone; on the other hand, L5/L7 did not modulate any expression of those genes. We conclude that L5/L7, in contrast to dexamethasone, spare skeletal muscle from structural and functional loss, and molecular changes, reinforcing their role as a therapeutic device.

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Publishing Date

2013-03-15

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