Β-GPA administration activates slow oxidative muscle signaling pathways and protects soleus muscle against the increased fatigue under 7-days of rat hindlimb suspension.

Archives of biochemistry and biophysics2023PMID: 37230367

View on PubMed DOI: 10.1016/j.abb.2023.109647

Animal StudyMOTS-C

Plain Language Summary

In rats with muscles unloaded by suspension (simulating weightlessness), a drug that depletes cellular energy stores (beta-GPA) unexpectedly protected the slow muscle fibers from the fatigue and fiber-type changes that normally accompany muscle disuse. This protection was linked to preserved activity of the mitochondria-derived peptide MOTS-c and other cellular energy sensors. The findings suggest that energy availability plays a key role in driving the muscle changes seen during inactivity.

Abstract

Unloading of slow-twitch muscles results in increased muscle fatigue and the mechanisms of this effect are poorly studied. We aimed to analyze the role of high-energy phosphates accumulation during the first week of rat hindlimb suspension plays in a fiber-type phenotype shift towards fast-type fatigable muscle fibers. Male Wistar rats were divided into 3 groups (n = 8): C - vivarium control; 7HS - 7-day hindlimb suspension; 7HB - 7-day hindlimb suspension with intraperitoneal injection of beta-guanidine propionic acid (β-GPA, 400 mg/kg b w). β-GPA is a competitive inhibitor of creatine kinase and it reduces concentrations of ATP and phosphocreatine. In the 7HB group, β-GPA treatment protected a slow-type signaling network in an unloaded soleus muscle, including MOTS-C, AMPK, PGC1 α and micro-RNA-499. These signaling effects resulted in a preserved soleus muscle fatigue resistance, slow-type muscle fibers percentage and mitochondrial DNA copy number under muscle unloading.

Authors

Sharlo, K A; Lvova, I D; Sidorenko, D A; Tyganov, S A; Sharlo, D T; Shenkman, B S