Irisin treatment improves healing of dystrophic skeletal muscle

Background: Irisin is an exercise induced myokine that is shown to promote browning of adipose tissue and hence, increase energy expenditure. Furthermore, our unpublished results indicate that Irisin improves myogenic differentiation and induces skeletal muscle hypertrophy. Since exercise induced sk...

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Main Authors: Reza, Musarrat Maisha, Sim, Chu Ming, Subramaniyam, Nathiya, Ge, Xiaojia, Sharma, Mridula, Kambadur, Ravi, McFarlane, Craig
Other Authors: School of Biological Sciences
Format: Article
Language:English
Published: 2018
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Online Access:https://hdl.handle.net/10356/88450
http://hdl.handle.net/10220/44623
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-884502023-02-28T17:02:34Z Irisin treatment improves healing of dystrophic skeletal muscle Reza, Musarrat Maisha Sim, Chu Ming Subramaniyam, Nathiya Ge, Xiaojia Sharma, Mridula Kambadur, Ravi McFarlane, Craig School of Biological Sciences Skeletal Muscle Dystrophy Background: Irisin is an exercise induced myokine that is shown to promote browning of adipose tissue and hence, increase energy expenditure. Furthermore, our unpublished results indicate that Irisin improves myogenic differentiation and induces skeletal muscle hypertrophy. Since exercise induced skeletal muscle hypertrophy improves muscle strength, we wanted to investigate if ectopic injection of Irisin peptide improves skeletal muscle function in a mouse model of muscular dystrophy. This utility of Irisin peptide is yet to be studied in animal models. Methods: In order to test this hypothesis, we expressed and purified recombinant murine Irisin peptide from E. coli. Three- to six-week-old male mdx mice were injected IP with either vehicle (dialysis buffer) or Irisin recombinant peptide for two or four weeks, three times-a-week. Results: Irisin injection increased muscle weights and enhanced grip strength in mdx mice. Improved muscle strength can be attributed to the significant hypertrophy observed in the Irisin injected mdx mice. Moreover, Irisin treatment resulted in reduced accumulation of fibrotic tissue and myofiber necrosis in mdx mice. In addition, Irisin improved sarcolemmal stability, which is severely compromised in mdx mice. Conclusion: Irisin injection induced skeletal muscle hypertrophy, improved muscle strength and reduced necrosis and fibrotic tissue in a murine dystrophy model. These results demonstrate the potential therapeutic value of Irisin in muscular dystrophy. ASTAR (Agency for Sci., Tech. and Research, S’pore) NMRC (Natl Medical Research Council, S’pore) Published version 2018-03-27T07:58:15Z 2019-12-06T17:03:35Z 2018-03-27T07:58:15Z 2019-12-06T17:03:35Z 2017 Journal Article Reza, M. M., Sim, C. M., Subramaniyam, N., Ge, X., Sharma, M., Kambadur, R., & McFarlane, C. (2017). Irisin treatment improves healing of dystrophic skeletal muscle. Oncotarget, 8(58), 98553-98566. https://hdl.handle.net/10356/88450 http://hdl.handle.net/10220/44623 10.18632/oncotarget.21636 en Oncotarget © 2017 Reza et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. 14 p. application/pdf
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic Skeletal Muscle
Dystrophy
spellingShingle Skeletal Muscle
Dystrophy
Reza, Musarrat Maisha
Sim, Chu Ming
Subramaniyam, Nathiya
Ge, Xiaojia
Sharma, Mridula
Kambadur, Ravi
McFarlane, Craig
Irisin treatment improves healing of dystrophic skeletal muscle
description Background: Irisin is an exercise induced myokine that is shown to promote browning of adipose tissue and hence, increase energy expenditure. Furthermore, our unpublished results indicate that Irisin improves myogenic differentiation and induces skeletal muscle hypertrophy. Since exercise induced skeletal muscle hypertrophy improves muscle strength, we wanted to investigate if ectopic injection of Irisin peptide improves skeletal muscle function in a mouse model of muscular dystrophy. This utility of Irisin peptide is yet to be studied in animal models. Methods: In order to test this hypothesis, we expressed and purified recombinant murine Irisin peptide from E. coli. Three- to six-week-old male mdx mice were injected IP with either vehicle (dialysis buffer) or Irisin recombinant peptide for two or four weeks, three times-a-week. Results: Irisin injection increased muscle weights and enhanced grip strength in mdx mice. Improved muscle strength can be attributed to the significant hypertrophy observed in the Irisin injected mdx mice. Moreover, Irisin treatment resulted in reduced accumulation of fibrotic tissue and myofiber necrosis in mdx mice. In addition, Irisin improved sarcolemmal stability, which is severely compromised in mdx mice. Conclusion: Irisin injection induced skeletal muscle hypertrophy, improved muscle strength and reduced necrosis and fibrotic tissue in a murine dystrophy model. These results demonstrate the potential therapeutic value of Irisin in muscular dystrophy.
author2 School of Biological Sciences
author_facet School of Biological Sciences
Reza, Musarrat Maisha
Sim, Chu Ming
Subramaniyam, Nathiya
Ge, Xiaojia
Sharma, Mridula
Kambadur, Ravi
McFarlane, Craig
format Article
author Reza, Musarrat Maisha
Sim, Chu Ming
Subramaniyam, Nathiya
Ge, Xiaojia
Sharma, Mridula
Kambadur, Ravi
McFarlane, Craig
author_sort Reza, Musarrat Maisha
title Irisin treatment improves healing of dystrophic skeletal muscle
title_short Irisin treatment improves healing of dystrophic skeletal muscle
title_full Irisin treatment improves healing of dystrophic skeletal muscle
title_fullStr Irisin treatment improves healing of dystrophic skeletal muscle
title_full_unstemmed Irisin treatment improves healing of dystrophic skeletal muscle
title_sort irisin treatment improves healing of dystrophic skeletal muscle
publishDate 2018
url https://hdl.handle.net/10356/88450
http://hdl.handle.net/10220/44623
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