Nitrosative Redox Homeostasis and Antioxidant Response Defense in Disused Vastus lateralis Muscle in Long-Term Bedrest (Toulouse Cocktail Study)

Nitrosative Redox Homeostasis and Antioxidant Response Defense in Disused Vastus lateralis Muscle in Long-Term Bedrest (Toulouse Cocktail Study)

Increased oxidative stress by reactive oxygen species (ROS) and reactive nitrogen species (RNS) is a major determinant of disuse-induced muscle atrophy. Muscle biopsies (thigh vastus lateralis, VL) obtained from healthy male subjects enrolled in the Toulouse Cocktail bedrest (BR) study were used to...

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Veröffentlicht in:Antioxidants 2021-03, Vol.10 (3), p.378, Article 378
Hauptverfasser: Blottner, Dieter, Capitanio, Daniele, Trautmann, Gabor, Furlan, Sandra, Gambara, Guido, Moriggi, Manuela, Block, Katharina, Barbacini, Pietro, Torretta, Enrica, Py, Guillaume, Chopard, Angele, Vida, Imre, Volpe, Pompeo, Gelfi, Cecilia, Salanova, Michele
Format: Artikel
Sprache:eng
Schlagworte:
Aerospace medicine
antioxidant systems
Antioxidants
Atrophy
bedrest muscle disuse
Biochemistry & Molecular Biology
Biopsy
Chemistry, Medicinal
Confocal microscopy
Exercise
Food Science & Technology
GA-binding protein
Glycolysis
Homeostasis
Life Sciences
Life Sciences & Biomedicine
Local anesthesia
Mass spectrometry
Metabolism
Mitochondria
Musculoskeletal system
Myogenesis
Nitrogen
Oxidative phosphorylation
Oxidative stress
Pharmaceutical sciences
Pharmacology
Pharmacology & Pharmacy
Phosphorylation
Physical fitness
Placebos
Polyphenols
Protein folding
Protein synthesis
Proteins
Reactive nitrogen species
Reactive oxygen species
RNS in cell signaling
Ryanodine receptors
sarcopenia
Science & Technology
Scientific imaging
Selenium
Signal transduction
Skeletal muscle
skeletal muscle redox homeostasis
Tricarboxylic acid cycle
Vitamin E
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Zusammenfassung:Increased oxidative stress by reactive oxygen species (ROS) and reactive nitrogen species (RNS) is a major determinant of disuse-induced muscle atrophy. Muscle biopsies (thigh vastus lateralis, VL) obtained from healthy male subjects enrolled in the Toulouse Cocktail bedrest (BR) study were used to assess efficacy of an antioxidant cocktail (polyphenols, omega-3, vitamin E, and selenium) to counteract the increased redox homeostasis and enhance the antioxidant defense response by using label-free LC-MS/MS and NITRO-DIGE (nitrosated proteins), qPCR, and laser confocal microscopy. Label-free LC-MS/MS indicated that treatment prevented the redox homeostasis dysregulation and promoted structural remodeling (TPM3, MYH7, MYBPC, MYH1, MYL1, HRC, and LUM), increment of RyR1, myogenesis (CSRP3), and skeletal muscle development (MUSTN1, LMNA, AHNAK). These changes were absent in the Placebo group. Glycolysis, tricarboxylic acid cycle (TCA), oxidative phosphorylation, fatty acid beta-oxidation, and mitochondrial transmembrane transport were normalized in treated subjects. Proteins involved in protein folding were also normalized, whereas protein entailed in ion homeostasis decreased. NITRO-DIGE analysis showed significant protein nitrosylation changes for CAT, CA3, SDHA, and VDAC2 in Treatment vs. Placebo. Similarly, the nuclear factor erythroid 2-related factor 2 (Nrf-2) antioxidant response element (Nrf-2 ARE) signaling pathway showed an enhanced response in the Treatment group. Increased nitrosative redox homeostasis and decreased antioxidant defense response were found in post-BR control (Placebo, n = 10) vs. the antioxidant cocktail treated group (Treatment, n = 10). Taken together, increased nitrosative redox homeostasis and muscle deterioration during BR-driven physical inactivity were prevented, whereas decreased antioxidant nitrosative stress defense response was attenuated by Treatment suggesting positive effects of the nutritional intervention protocol in bedrest.
ISSN:2076-3921
2076-3921
DOI:10.3390/antiox10030378