To develop an effective treatment for muscle recovery, costimuli effect of cyclic stretch and hypoxia on the recovery of oxidative damaged skeletal muscle cells is investigated. C2C12 myoblast cells are differentiated into myotube in culture dish followed by seeding the myotubes in the microfluidic device for further growth. Hydrogen peroxide is used to induce oxidative stress on myotubes for mimicking intracellular muscle damage. Afterward, the damaged myotubes are recovered in either normoxia or hypoxia environment with or without cyclic stretch, to elucidate the effect of the stretch and hypoxia on recovery. For analysis, reactive oxygen species, 8‐hydroxydeoxyguanosine, and myosin heavy chain are chosen as recovery indicators and it is shown that cyclic stretch and hypoxia facilitate the recovery of muscle to the greatest extent when both cyclic stretch and hypoxia are applied. To investigate the mechanism of the stretch and hypoxia intervened recovery, hypoxia inducible factor‐1α (HIF‐1α), peroxiredoxin 2, glutathione peroxidase 1, and catalase are selected as candidates for the key factor of recovery acceleration. There is evidence that HIF‐1α and antioxidants contributed to stretch‐/hypoxia‐induced recovery, and HIF‐1α is speculated to play the most important role. Hence, the stretch and hypoxia triggered pathways of cellular recovery are suggested.
Increased Recovery Rate of Damaged Muscle
Hyung‐Soon Park, Jessie S. John, and colleagues demonstrate how the combination of cyclic stretch and hypoxic conditions leads to an increased recovery rate of damaged muscle in article numer 2100465, by activating the reactive oxygen species recovery‐related pathways as found in the microfluidic‐based muscle damage model. Also, Hypoxia Inducible Factor 1‐alpha (HIF1‐α) plays a causal role in the stretch‐/hypoxia‐enhanced recovery.
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