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  4. Sphingolipids accumulate in aged muscle, and their reduction counteracts sarcopenia
 
research article

Sphingolipids accumulate in aged muscle, and their reduction counteracts sarcopenia

Laurila, Pirkka-Pekka  
•
Wohlwend, Martin  
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de Lima, Tanes Imamura  
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December 1, 2022
Nature Aging

Age-related muscle dysfunction and sarcopenia are major causes of physical incapacitation in older adults and currently lack viable treatment strategies. Here we find that sphingolipids accumulate in mouse skeletal muscle upon aging and that both genetic and pharmacological inhibition of sphingolipid synthesis prevent age-related decline in muscle mass while enhancing strength and exercise capacity. Inhibition of sphingolipid synthesis confers increased myogenic potential and promotes protein synthesis. Within the sphingolipid pathway, we show that accumulation of dihydroceramides is the culprit disturbing myofibrillar homeostasis. The relevance of sphingolipid pathways in human aging is demonstrated in two cohorts, the UK Biobank and Helsinki Birth Cohort Study in which gene expression-reducing variants of SPTLC1 and DEGS1 are associated with improved and reduced fitness of older individuals, respectively. These findings identify sphingolipid synthesis inhibition as an attractive therapeutic strategy for age-related sarcopenia and co-occurring pathologies.

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Type
research article
DOI
10.1038/s43587-022-00309-6
Web of Science ID

WOS:000916582800016

Author(s)
Laurila, Pirkka-Pekka  
Wohlwend, Martin  
de Lima, Tanes Imamura  
Luan, Peiling  
Herzig, Sebastien  
Zanou, Nadege
Crisol, Barbara
Bou-Sleiman, Maroun  
Porcu, Eleonora
Gallart-Ayala, Hector
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Date Issued

2022-12-01

Published in
Nature Aging
Volume

2

Issue

12

Start page

1159

End page
Subjects

Cell Biology

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Geriatrics & Gerontology

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Neurosciences

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Cell Biology

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Geriatrics & Gerontology

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Neurosciences & Neurology

•

resistance exercise

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increased ceramide

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stem-cells

•

performance

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inhibition

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metabolism

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strength

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mitochondrial

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polypharmacy

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senescence

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LISP  
Available on Infoscience
February 27, 2023
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/195299
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