Author:
Takahashi Tadahisa,Li Yuqing,Chen Weijian,Nyasha Mazvita R.,Ogawa Kazumi,Suzuki Kazuaki,Koide Masashi,Hagiwara Yoshihiro,Itoi Eiji,Aizawa Toshimi,Tsuchiya Masahiro,Suzuki Naoki,Aoki Masashi,Kanzaki Makoto
Abstract
AbstractThe physiological significance of skeletal muscle as a secretory organ is now well known but we can only speculate as to the existence of as-yet-unidentified myokines, especially those upregulated in response to muscle contractile activity. We first attempted to establish an “insert-chamber based in vitro exercise model” allowing the miniature but high cell-density culture state enabling highly developed contractile human myotubes to be readily obtained by applying electric pulse stimulation (EPS). By employing this in vitro exercise model, we identified R-spondin 3 (RSPO3) as a novel contraction-inducible myokine produced by cultured human myotubes. Contraction-dependent muscular RSPO3 mRNA upregulation was confirmed in skeletal muscles of mice subjected to sciatic nerve mediated in situ contraction as well as those of mice after 2 h of running. Pharmacological in vitro experiments demonstrated a relatively high concentration of metformin (millimolar range) to suppress the contraction-inducible mRNA upregulation of human myokines including RSPO3, interleukin (IL)-6, IL-8 and CXCL1. Our data also suggest human RSPO3 to be a paracrine factor that may positively participate in the myogenesis processes of myoblasts and satellite cells. Thus, the “insert chamber-based in vitro exercise model” is a potentially valuable research tool for investigating contraction-inducible biological responses of human myotubes usually exhibiting poorer contractility development even in the setting of EPS treatment.
Funder
Japan Society for the Promotion of Science
Japan Agency for Medical Research and Development
Ministry of Health, Labor and Welfare of Japan
a Grant-in-Aid for Challenging Exploratory Research
Publisher
Springer Science and Business Media LLC
Cited by
3 articles.
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