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  4. Iron accumulation causes impaired myogenesis correlated with MAPK signaling pathway inhibition by oxidative stress

Iron accumulation causes impaired myogenesis correlated with MAPK signaling pathway inhibition by oxidative stress

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Use this link to cite this item : https://repo.lib.tokushima-u.ac.jp/113746
ID 113746
Author
Ikeda, Yasumasa Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Satoh, Akiho Tokushima University
Horinouchi, Yuya Tokushima University
Hamano, Hirofumi Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Watanabe, Hiroaki Tokushima University
Imao, Mizuki Tokushima University
Imanishi, Masaki Tokushima University Tokushima University Educator and Researcher Directory
Zamami, Yoshito Tokushima University KAKEN Search Researchers
Takechi, Kenshi Tokushima University
Izawa-Ishizawa, Yuki Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Miyamoto, Licht Tokushima University KAKEN Search Researchers
Hirayama, Tasuku Gifu Pharmaceutical University
Nagasawa, Hideko Gifu Pharmaceutical University
Ishizawa, Keisuke Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Aihara, Ken-ichi Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Tsuchiya, Koichiro Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Tamaki, Toshiaki Tokushima University Tokushima University Educator and Researcher Directory KAKEN Search Researchers
Keywords
muscle regeneration
muscle differentiation
p38MAPK
ERK1/2
iron
myogenesis
oxidative stress
mitogen-activated protein kinases(MAPKs)
Content Type
Journal Article
Description
Skeletal muscle atrophy is caused by disruption in the homeostatic balance of muscle degeneration and regeneration under various pathophysiological conditions. We have previously reported that iron accumulation induces skeletal muscle atrophy via a ubiquitin ligase-dependent pathway. However, the potential effect of iron accumulation on muscle regeneration remains unclear. To examine the effect of iron accumulation on myogenesis, we used a mouse model with cardiotoxin (CTX)-induced muscle regeneration in vivo and C2C12 mice myoblast cells in vitro. In mice with iron overload, the skeletal muscles exhibited increased oxidative stress and decreased expression of satellite cell markers. Following CTX-induced muscle injury, these mice also displayed delayed muscle regeneration with a decrease in the size of regenerating myofibers, reduced expression of myoblast differentiation markers, and decreased phosphorylation of mitogen-activated protein kinase signaling pathways. In vitro, iron overload also suppressed the differentiation of C2C12 myoblast cells, but the suppression could be reversed by superoxide scavenging using tempol. Excess iron inhibits myogenesis via oxidative stress, leading to an imbalance in skeletal muscle homeostasis.
Journal Title
The FASEB Journal
ISSN
15306860
08926638
NCID
AA1066874X
Publisher
Federation of American Societies for Experimental Biology|John Wiley & Sons
Volume
33
Issue
8
Start Page
9551
End Page
9564
Published Date
2019-05-30
Remark
This is the peer reviewed version of the following article: Ikeda, Y., Satoh, A., Horinouchi, Y., Hamano, H., Watanabe, H., Imao, M., Imanishi, M., Zamami, Y., Takechi, K., Izawa‐Ishizawa, Y., Miyamoto, L., Hirayama, T., Nagasawa, H., Ishizawa, K., Aihara, K.‐I., Tsuchiya, K. and Tamaki, T. (2019), Iron accumulation causes impaired myogenesis correlated with MAPK signaling pathway inhibition by oxidative stress. Faseb, 33: 9551-9564, which has been published in final form at https://doi.org/10.1096/fj.201802724RR. This article may be used for non-commercial purposes in accordance with Wiley Terms and Conditions for Use of Self-Archived Versions.
EDB ID
351099
DOI (Published Version)
10.1096/fj.201802724RR
URL ( Publisher's Version )
https://doi.org/10.1096/fj.201802724RR
FullText File
faseb_33_8_9551.pdf 1.94 MB
language
eng
TextVersion
Author
departments
Medical Sciences
University Hospital
Pharmaceutical Sciences
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