Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy

Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy

Duchenne muscular dystrophy (DMD) is a devastating disease characterized by muscle wasting, loss of mobility and death in early adulthood. Satellite cells are muscle-resident stem cells responsible for the repair and regeneration of damaged muscles. One pathological feature of DMD is the progressive...

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Main Authors: Chunhui Jiang, Yefei Wen, Kazuki Kuroda, Kevin Hannon, Michael A. Rudnicki, Shihuan Kuang
Format: Article
Language:English
Published: The Company of Biologists 2014-08-01
Series:Disease Models & Mechanisms
Subjects:
Muscular dystrophy
Notch signaling
Stem cell
Online Access:http://dmm.biologists.org/content/7/8/997
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spelling doaj-4f7fee7af8f342bdb8449583b060ded12020-11-25T01:23:34ZengThe Company of BiologistsDisease Models & Mechanisms1754-84031754-84112014-08-0178997100410.1242/dmm.015917015917Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophyChunhui JiangYefei WenKazuki KurodaKevin HannonMichael A. RudnickiShihuan KuangDuchenne muscular dystrophy (DMD) is a devastating disease characterized by muscle wasting, loss of mobility and death in early adulthood. Satellite cells are muscle-resident stem cells responsible for the repair and regeneration of damaged muscles. One pathological feature of DMD is the progressive depletion of satellite cells, leading to the failure of muscle repair. Here, we attempted to explore the molecular mechanisms underlying satellite cell ablation in the dystrophin mutant mdx mouse, a well-established model for DMD. Initial muscle degeneration activates satellite cells, resulting in increased satellite cell number in young mdx mice. This is followed by rapid loss of satellite cells with age due to the reduced self-renewal ability of mdx satellite cells. In addition, satellite cell composition is altered even in young mdx mice, with significant reductions in the abundance of non-committed (Pax7+ and Myf5−) satellite cells. Using a Notch-reporter mouse, we found that the mdx satellite cells have reduced activation of Notch signaling, which has been shown to be necessary to maintain satellite cell quiescence and self-renewal. Concomitantly, the expression of Notch1, Notch3, Jag1, Hey1 and HeyL are reduced in the mdx primary myoblast. Finally, we established a mouse model to constitutively activate Notch signaling in satellite cells, and show that Notch activation is sufficient to rescue the self-renewal deficiencies of mdx satellite cells. These results demonstrate that Notch signaling is essential for maintaining the satellite cell pool and that its deficiency leads to depletion of satellite cells in DMD.http://dmm.biologists.org/content/7/8/997Muscular dystrophyNotch signalingStem cell
collection DOAJ
language English
format Article
sources DOAJ
author Chunhui Jiang
Yefei Wen
Kazuki Kuroda
Kevin Hannon
Michael A. Rudnicki
Shihuan Kuang
spellingShingle Chunhui Jiang
Yefei Wen
Kazuki Kuroda
Kevin Hannon
Michael A. Rudnicki
Shihuan Kuang
Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
Disease Models & Mechanisms
Muscular dystrophy
Notch signaling
Stem cell
author_facet Chunhui Jiang
Yefei Wen
Kazuki Kuroda
Kevin Hannon
Michael A. Rudnicki
Shihuan Kuang
author_sort Chunhui Jiang
title Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
title_short Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
title_full Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
title_fullStr Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
title_full_unstemmed Notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
title_sort notch signaling deficiency underlies age-dependent depletion of satellite cells in muscular dystrophy
publisher The Company of Biologists
series Disease Models & Mechanisms
issn 1754-8403
1754-8411
publishDate 2014-08-01
description Duchenne muscular dystrophy (DMD) is a devastating disease characterized by muscle wasting, loss of mobility and death in early adulthood. Satellite cells are muscle-resident stem cells responsible for the repair and regeneration of damaged muscles. One pathological feature of DMD is the progressive depletion of satellite cells, leading to the failure of muscle repair. Here, we attempted to explore the molecular mechanisms underlying satellite cell ablation in the dystrophin mutant mdx mouse, a well-established model for DMD. Initial muscle degeneration activates satellite cells, resulting in increased satellite cell number in young mdx mice. This is followed by rapid loss of satellite cells with age due to the reduced self-renewal ability of mdx satellite cells. In addition, satellite cell composition is altered even in young mdx mice, with significant reductions in the abundance of non-committed (Pax7+ and Myf5−) satellite cells. Using a Notch-reporter mouse, we found that the mdx satellite cells have reduced activation of Notch signaling, which has been shown to be necessary to maintain satellite cell quiescence and self-renewal. Concomitantly, the expression of Notch1, Notch3, Jag1, Hey1 and HeyL are reduced in the mdx primary myoblast. Finally, we established a mouse model to constitutively activate Notch signaling in satellite cells, and show that Notch activation is sufficient to rescue the self-renewal deficiencies of mdx satellite cells. These results demonstrate that Notch signaling is essential for maintaining the satellite cell pool and that its deficiency leads to depletion of satellite cells in DMD.
topic Muscular dystrophy
Notch signaling
Stem cell
url http://dmm.biologists.org/content/7/8/997
work_keys_str_mv AT chunhuijiang notchsignalingdeficiencyunderliesagedependentdepletionofsatellitecellsinmusculardystrophy
AT yefeiwen notchsignalingdeficiencyunderliesagedependentdepletionofsatellitecellsinmusculardystrophy
AT kazukikuroda notchsignalingdeficiencyunderliesagedependentdepletionofsatellitecellsinmusculardystrophy
AT kevinhannon notchsignalingdeficiencyunderliesagedependentdepletionofsatellitecellsinmusculardystrophy
AT michaelarudnicki notchsignalingdeficiencyunderliesagedependentdepletionofsatellitecellsinmusculardystrophy
AT shihuankuang notchsignalingdeficiencyunderliesagedependentdepletionofsatellitecellsinmusculardystrophy
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