NADPH oxidase 2 is necessary for chronic intermittent hypoxia-induced sternohyoid muscle weakness in adult male mice.

Sarah E DrummondDavid P BurnsSarah El MaghraniOscar ZieglerVincent HealyKen D O'Halloran

Published in: Experimental physiology (2022)

). Profound sternohyoid muscle dysfunction following exposure to CIH was entirely prevented by apocynin co-treatment or NOX2 deletion. Exposure to CIH increased sternohyoid muscle NOX enzyme activity, with no alteration to the gene or protein expression of NOX subunits. There was no evidence of overt oxidative stress, muscle regeneration, inflammation or atrophy following exposure to CIH. We suggest that NOX-dependent CIH-induced upper airway muscle weakness increases vulnerability to upper airway obstruction. Our results have implications for human obstructive sleep apnoea syndrome and point to antioxidant intervention, potentially targeting NOX2 blockade, as a therapeutic strategy.

Keyphrases

oxidative stress
skeletal muscle
reactive oxygen species
diabetic rats
stem cells
endothelial cells
gene expression
dna damage
climate change
depressive symptoms
young adults
drug induced
intellectual disability
dna methylation
obstructive sleep apnea
induced apoptosis
smoking cessation
sleep apnea