| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5587895 | Growth Hormone & IGF Research | 2017 | 12 Pages |
Abstract
The mere IGF-1 partial deficiency is per se associated with hepatic mitochondrial dysfunction sensitive to IGF-1 replacement therapy. Results in this work prove that IGF-1 is involved in hepatic mitochondrial protection, because it is able to reduce free radical production, oxidative damage and apoptosis. All these IGF-1 actions are mediated by the modulation of the expression of genes encoding citoprotective and antiapoptotic proteins.
Keywords
MMPIUGRMDAMMPTSDHBCCCPHSPsRCRIGF-1GSHPxANTRT-qPCRREEOXPHOSATRPCCROSUCPsHydrogen peroxideatractylosideOxidative damageResting energy expendituremitochondrial membrane permeability transitioninsulin-like growth factor-1adenine nucleotide translocatorUncoupling proteinsCellular protectionstandard error of meanRh-123Free radicalsRhodamine-123electron transport chainSODMetabolic syndromeSuperoxide dismutasesuccinate dehydrogenaseOxidative phosphorylationFluorescencemalondialdehydeMETSProtein carbonyl contentintrauterine growth restrictionSEMnot significantMitochondriarespiratory control ratioheterozygousH2O2ETcArbitrary Unitreverse transcription polymerase chain reactionMitochondrial membrane potentialHeat shock proteinscarbonyl cyanide m-chlorophenyl hydrazinecontrol groupglutathione peroxidaseReactive oxygen species
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Authors
M. Olleros Santos-Ruiz, M.C. Sádaba, I. MartÃn-Estal, U. Muñoz, C. Sebal Neira, I. Castilla-Cortázar,