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Inhibition of Activin/Myostatin signalling induces skeletal muscle hypertrophy but impairs mouse testicular development

Authors :
Danielle Vaughan
Olli Ritvos
Robert Mitchell
Oliver Kretz
Maciej Lalowski
Helge Amthor
David Chambers
Antonios Matsakas
Arja Pasternack
Henry Collins-Hooper
Randy Ballesteros
Tobias B. Huber
Bernd Denecke
Darius Widera
Abir Mukherjee
Ketan Patel
Source :
European Journal of Translational Myology (2020)
Publication Year :
2020
Publisher :
PAGEPress Publications, 2020.

Abstract

Numerous approaches are being developed to promote post-natal muscle growth based on attenuating Myostatin/Activin signalling for clinical uses such as the treatment neuromuscular diseases, cancer cachexia and sarcopenia. However there have been concerns about the effects of inhibiting Activin on tissues other than skeletal muscle. We intraperitoneally injected mice with the Activin ligand trap, sActRIIB, in young, adult and a progeric mouse model. Treatment at any stage in the life of the mouse rapidly increased muscle mass. However at all stages of life the treatment decreased the weights of the testis. Not only were the testis smaller, but they contained fewer sperm compared to untreated mice. We found that the hypertrophic muscle phenotype was lost after the cessation of sActRIIB treatment but abnormal testis phenotype persisted. In summary, attenuation of Myostatin/Activin signalling inhibited testis development. Future use of molecules based on a similar mode of action to promote muscle growth should be carefully profiled for adverse side-effects on the testis. However the effectiveness of sActRIIB as a modulator of Activin function provides a possible therapeutic strategy to alleviate testicular seminoma development.

Details

Language :
English
ISSN :
20377452 and 20377460
Database :
Directory of Open Access Journals
Journal :
European Journal of Translational Myology
Publication Type :
Academic Journal
Accession number :
edsdoj.09e0948256164d728487d1212eb609fd
Document Type :
article
Full Text :
https://doi.org/10.4081/ejtm.2019.8737