Sphingomyelinase activity promotes atrophy and attenuates force in human muscle fibres and is elevated in heart failure patients.

Karl OlssonArthur J ChengMamdoh Al-AmeriNicolas TardifMichael MelinOlav RooyackersJohanna T LannerHåkan WesterbladThomas GustafssonJoseph D BrutonTommy R Lundberg

Published in: Journal of cachexia, sarcopenia and muscle (2022)

The present findings implicate activation of skeletal muscle SMase as a mechanism underlying human heart failure-related loss of muscle mass and function. Moreover, our findings strengthen the idea that SMase activation may underpin disease-related loss of muscle mass and function in other clinical conditions, acting as a common patophysiological mechanism for the myopathy often reported in diseases associated with a systemic inflammatory response.

Keyphrases

skeletal muscle
endothelial cells
heart failure
inflammatory response
induced pluripotent stem cells
pluripotent stem cells
type diabetes
metabolic syndrome
lipopolysaccharide induced
atrial fibrillation
adipose tissue