Abstract
AbstractAndrogens exert their effects primarily by binding to the androgen receptor (AR), a ligand-dependent nuclear receptor. While androgens have anabolic effects on skeletal muscle, previous studies reported that AR functions in myofibers to regulate skeletal muscle quality, rather than skeletal muscle mass. Therefore, the anabolic effects of androgens are exerted via extra-myofiber cells or tissues. In this context, the cellular and molecular mechanisms of AR in mesenchymal progenitors, which play a crucial role in maintaining skeletal muscle homeostasis, remain largely unknown. In this study, we demonstrated expression of AR in mesenchymal progenitors and found that targeted AR ablation in mesenchymal progenitors reduced limb muscle mass in mature adult, but not young or aged, male mice, although fatty infiltration of muscle was not affected. The absence of AR in mesenchymal progenitors led to remarkable perineal muscle hypotrophy, regardless of age, due to abnormal regulation of transcripts associated with apoptosis and proteolysis. Additionally, we revealed that AR in mesenchymal progenitors regulates the expression of insulin-like growth factor 1, which can increase skeletal muscle mass in a paracrine manner. These findings indicate that the anabolic effects of androgens indirectly regulate skeletal muscle mass via, at least in part, AR signaling in mesenchymal progenitors.
Publisher
Cold Spring Harbor Laboratory
Cited by
1 articles.
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