Ceramide down-regulates System A amino acid transport and protein synthesis in rat skeletal muscle cells

ABSTRACT Skeletal muscle is a major insulin target tissue and has a prominent role in the control of body amino acid economy, being the principal store of free and protein‐bound amino acids and a dominant locus for amino acid metabolism. Interplay between diverse stimuli (e.g., hormonal/nutritional/...

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Bibliographic Details
Published in:The FASEB journal 2005-03, Vol.19 (3), p.461-463
Main Authors: Hyde, Russell, Hajduch, Eric, Powell, Darren J, Taylor, Peter M, Hundal, Harinder S
Format: Article
Language:English
Subjects:
Amino Acid Transport System A - antagonists & inhibitors
Amino Acid Transport System A - drug effects
Amino Acid Transport System A - metabolism
Amino Acid Transport Systems - analysis
Amino Acid Transport Systems - antagonists & inhibitors
Amino Acid Transport Systems - physiology
Amino Acids - analysis
Amino Acids - metabolism
Animals
Cell Line
Cell Membrane - chemistry
Ceramides - pharmacology
Glucose - metabolism
insulin
Me-AIB
Muscle Cells - drug effects
Muscle Cells - metabolism
Muscle Fibers, Skeletal - drug effects
Muscle Fibers, Skeletal - metabolism
Muscle Proteins - biosynthesis
Muscle, Skeletal - chemistry
Muscle, Skeletal - drug effects
Muscle, Skeletal - metabolism
PKB/Akt
Protein Kinases - metabolism
rapamycin
Rats
Signal Transduction - drug effects
SNAT2
TOR Serine-Threonine Kinases
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Summary:ABSTRACT Skeletal muscle is a major insulin target tissue and has a prominent role in the control of body amino acid economy, being the principal store of free and protein‐bound amino acids and a dominant locus for amino acid metabolism. Interplay between diverse stimuli (e.g., hormonal/nutritional/mechanical) modulates muscle insulin action to serve physiological need through the action of factors such as intramuscular signaling molecules. Ceramide, a product of sphingolipid metabolism and cytokine signaling, has a potent contra‐insulin action with respect to the transport and deposition of glucose in skeletal muscle, although ceramide effects on muscle amino acid turnover have not previously been documented. Here, membrane permeant C2‐ceramide is shown to attenuate the basal and insulin‐stimulated activity of the Na+‐dependent System A amino acid transporter in rat muscle cells (L6 myotubes) by depletion of the plasma membrane abundance of SNAT2 (a System A isoform). Concomitant with transporter down‐regulation, ceramide diminished both intramyocellular amino acid abundance and the phosphorylation of translation regulators lying downstream of mTOR. The physiological outcome of ceramide signaling in this instance is a marked reduction in cellular protein synthesis, a result that is likely to represent an important component of the processes leading to muscle wasting in catabolic conditions.
ISSN:0892-6638
1530-6860
DOI:10.1096/fj.04-2284fje