Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.

Muscles can be injured in different ways and the trauma and subsequent loss of function and physical capacity can impact significantly on the lives of patients through physical impairments and compromised quality of life. The relative success of muscle repair after injury will largely determine the...

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Main Authors: Jarrod E Church, Jennifer Trieu, Radhika Sheorey, Annabel Y-M Chee, Timur Naim, Dale M Baum, James G Ryall, Paul Gregorevic, Gordon S Lynch
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4084885?pdf=render
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spelling doaj-54c69962650f44dab05a344092e12d932020-11-25T02:29:57ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0197e10137910.1371/journal.pone.0101379Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.Jarrod E ChurchJennifer TrieuRadhika SheoreyAnnabel Y-M CheeTimur NaimDale M BaumJames G RyallPaul GregorevicGordon S LynchMuscles can be injured in different ways and the trauma and subsequent loss of function and physical capacity can impact significantly on the lives of patients through physical impairments and compromised quality of life. The relative success of muscle repair after injury will largely determine the extent of functional recovery. Unfortunately, regenerative processes are often slow and incomplete, and so developing novel strategies to enhance muscle regeneration is important. While the capacity to enhance muscle repair by stimulating β2-adrenoceptors (β-ARs) using β2-AR agonists (β2-agonists) has been demonstrated previously, the exact role β-ARs play in regulating the regenerative process remains unclear. To investigate β-AR-mediated signaling in muscle regeneration after myotoxic damage, we examined the regenerative capacity of tibialis anterior and extensor digitorum longus muscles from mice lacking either β1-AR (β1-KO) and/or β2-ARs (β2-KO), testing the hypothesis that muscles from mice lacking the β2-AR would exhibit impaired functional regeneration after damage compared with muscles from β1-KO or β1/β2-AR null (β1/β2-KO) KO mice. At 7 days post-injury, regenerating muscles from β1/β2-KO mice produced less force than those of controls but muscles from β1-KO or β2-KO mice did not exhibit any delay in functional restoration. Compared with controls, β1/β2-KO mice exhibited an enhanced inflammatory response to injury, which delayed early muscle regeneration, but an enhanced myoblast proliferation later during regeneration ensured a similar functional recovery (to controls) by 14 days post-injury. This apparent redundancy in the β-AR signaling pathway was unexpected and may have important implications for manipulating β-AR signaling to improve the rate, extent and efficacy of muscle regeneration to enhance functional recovery after injury.http://europepmc.org/articles/PMC4084885?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jarrod E Church
Jennifer Trieu
Radhika Sheorey
Annabel Y-M Chee
Timur Naim
Dale M Baum
James G Ryall
Paul Gregorevic
Gordon S Lynch
spellingShingle Jarrod E Church
Jennifer Trieu
Radhika Sheorey
Annabel Y-M Chee
Timur Naim
Dale M Baum
James G Ryall
Paul Gregorevic
Gordon S Lynch
Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
PLoS ONE
author_facet Jarrod E Church
Jennifer Trieu
Radhika Sheorey
Annabel Y-M Chee
Timur Naim
Dale M Baum
James G Ryall
Paul Gregorevic
Gordon S Lynch
author_sort Jarrod E Church
title Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
title_short Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
title_full Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
title_fullStr Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
title_full_unstemmed Functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
title_sort functional β-adrenoceptors are important for early muscle regeneration in mice through effects on myoblast proliferation and differentiation.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Muscles can be injured in different ways and the trauma and subsequent loss of function and physical capacity can impact significantly on the lives of patients through physical impairments and compromised quality of life. The relative success of muscle repair after injury will largely determine the extent of functional recovery. Unfortunately, regenerative processes are often slow and incomplete, and so developing novel strategies to enhance muscle regeneration is important. While the capacity to enhance muscle repair by stimulating β2-adrenoceptors (β-ARs) using β2-AR agonists (β2-agonists) has been demonstrated previously, the exact role β-ARs play in regulating the regenerative process remains unclear. To investigate β-AR-mediated signaling in muscle regeneration after myotoxic damage, we examined the regenerative capacity of tibialis anterior and extensor digitorum longus muscles from mice lacking either β1-AR (β1-KO) and/or β2-ARs (β2-KO), testing the hypothesis that muscles from mice lacking the β2-AR would exhibit impaired functional regeneration after damage compared with muscles from β1-KO or β1/β2-AR null (β1/β2-KO) KO mice. At 7 days post-injury, regenerating muscles from β1/β2-KO mice produced less force than those of controls but muscles from β1-KO or β2-KO mice did not exhibit any delay in functional restoration. Compared with controls, β1/β2-KO mice exhibited an enhanced inflammatory response to injury, which delayed early muscle regeneration, but an enhanced myoblast proliferation later during regeneration ensured a similar functional recovery (to controls) by 14 days post-injury. This apparent redundancy in the β-AR signaling pathway was unexpected and may have important implications for manipulating β-AR signaling to improve the rate, extent and efficacy of muscle regeneration to enhance functional recovery after injury.
url http://europepmc.org/articles/PMC4084885?pdf=render
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