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DOI: 10.1055/a-1331-7021
Role of Dkk2 in the Muscle/bone Interaction of Androgen-Deficient Mice
Funding: This study was partly supported by a grant from Kindai Research Enhancement Grant (21st Century Joint Research Enhancement Grant) to H.K., Grants-in-Aid for Scientific Research (C:20K09514) to H.K. and (C:19K07310) to N.K., and a Grant-in-Aid for Scientific Research on Innovative Areas (grant number 15H05935, “Living in Space”) from the Ministry of Education, Culture, Sports, Science, and Technology of Japan to H.K.
Abstract
Androgen deficiency is known to cause both osteoporosis and sarcopenia. Myokines, humoral factors secreted from the skeletal muscles, have recently been getting attention as the key factors related to the interactions between muscle and bone. Dickkopf (Dkk) 2 is known as an inhibitor of canonical Wnt/β-catenin signaling, and Wnt/β-catenin signaling is crucial for the maintenance of muscle and bone. The present study was therefore performed to investigate the roles of Dkk2 in the alterations of muscle and bone of androgen-deficient mice with orchidectomy (ORX). ORX significantly enhanced Dkk2 mRNA levels, but not other Dkks and secreted frizzled related proteins, in the soleus muscles of mice. Moreover, ORX enhanced serum Dkk2 levels, but not Dkk2 mRNA levels in the tibial bone tissues, the white adipose tissues and liver of mice. In simple regression analyses, serum Dkk2 levels were negatively related to trabecular bone mineral density at the tibias in mice employed in the experiments. In vitro experiments, testosterone suppressed Dkk2 mRNA levels in mouse muscle C2C12 cells. In conclusion, we showed that androgen deficiency enhances Dkk2 expression and secretion in the muscles of mice. Dkk2 might be involved in androgen deficiency-induced muscle wasting and osteopenia as a myokine linking muscle to bone.
Publication History
Received: 22 July 2020
Received: 27 November 2020
Accepted: 07 December 2020
Article published online:
22 December 2020
© 2020. Thieme. All rights reserved.
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