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Loss of ARNT in skeletal muscle limits muscle regeneration in aging.

Citation
Endo, Y., et al. “Loss Of Arnt In Skeletal Muscle Limits Muscle Regeneration In Aging.”. Faseb Journal : Official Publication Of The Federation Of American Societies For Experimental Biology, pp. 16086-16104.
Center Joslin Diabetes Center
Author Yori Endo, Kodi Baldino, Bin Li, Yuteng Zhang, Dharaniya Sakthivel, Michael MacArthur, Adriana C Panayi, Peter Kip, Daniel J Spencer, Ravi Jasuja, Debalina Bagchi, Shalender Bhasin, Kristo Nuutila, Ronald L Neppl, Amy J Wagers, Indranil Sinha
Keywords aging, hypoxia signaling, muscle regeneration
Abstract

The ability of skeletal muscle to regenerate declines significantly with aging. The expression of aryl hydrocarbon receptor nuclear translocator (ARNT), a critical component of the hypoxia signaling pathway, was less abundant in skeletal muscle of old (23-25 months old) mice. This loss of ARNT was associated with decreased levels of Notch1 intracellular domain (N1ICD) and impaired regenerative response to injury in comparison to young (2-3 months old) mice. Knockdown of ARNT in a primary muscle cell line impaired differentiation in vitro. Skeletal muscle-specific ARNT deletion in young mice resulted in decreased levels of whole muscle N1ICD and limited muscle regeneration. Administration of a systemic hypoxia pathway activator (ML228), which simulates the actions of ARNT, rescued skeletal muscle regeneration in both old and ARNT-deleted mice. These results suggest that the loss of ARNT in skeletal muscle is partially responsible for diminished myogenic potential in aging and activation of hypoxia signaling holds promise for rescuing regenerative activity in old muscle.

Year of Publication
2020
Journal
FASEB journal : official publication of the Federation of American Societies for Experimental Biology
Volume
34
Issue
12
Number of Pages
16086-16104
Date Published
12/2020
ISSN Number
1530-6860
DOI
10.1096/fj.202000761RR
Alternate Journal
FASEB J
PMID
33064329
PMCID
PMC7756517
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