The role of intramuscular lipid in insulin resistance
- 16 July 2003
- journal article
- review article
- Published by Wiley in Acta Physiologica Scandinavica
- Vol. 178 (4) , 373-383
- https://doi.org/10.1046/j.1365-201x.2003.01162.x
Abstract
There is interest in how altered lipid metabolism could contribute to muscle insulin resistance. Many animal and human states of insulin resistance have increased muscle triglyceride content, and there are now plausible mechanistic links between muscle lipid accumulation and insulin resistance, which go beyond the classic glucose–fatty acid cycle. We postulate that muscle cytosolic accumulation of the metabolically active long‐chain fatty acyl CoAs (LCACoA) is involved, leading to insulin resistance and impaired insulin signalling or impaired enzyme activity (e.g. glycogen synthase or hexokinase) either directly or via chronic translocation/activation of mediators such as a protein kinase C (particularly PKC θ and ɛ). Ceramides and diacylglycerols (DAGs) have also been implicated in forms of lipid‐induced muscle insulin resistance. Dietary lipid‐induced muscle insulin resistance in rodents is relatively easily reversed by manipulations that lessen cytosolic lipid accumulation (e.g. diet change, exercise or fasting). PPAR agonists (both γ and α) also lower muscle LCACoA and enhance insulin sensitivity. Activation of AMP‐activated protein kinase (AMPK) by AICAR leads to muscle enhancement (especially glycolytic muscle) of insulin sensitivity, but involvement of altered lipid metabolism is less clear cut. In rodents there are similarities in the pattern of muscle lipid accumulation/PKC translocation/altered insulin signalling/insulin resistance inducible by 3–5‐h acute free fatty acid elevation, 1–4 days intravenous glucose infusion or several weeks of high‐fat feeding. Recent studies extend findings and show relevance to humans. Muscle cytosolic lipids may accumulate either by increased fatty acid flux into muscle, or by reduced fatty acid oxidation. In some circumstances muscle insulin resistance may be an adaptation to optimize use of fatty acids when they are the predominant available energy fuel. The interactions described here are fundamental to optimizing therapy of insulin resistance based on alterations in muscle lipid metabolism.Keywords
This publication has 117 references indexed in Scilit:
- Leptin Activates Cardiac Fatty Acid Oxidation Independent of Changes in the AMP-activated Protein Kinase-Acetyl-CoA Carboxylase-Malonyl-CoA AxisJournal of Biological Chemistry, 2002
- Leptin stimulates fatty-acid oxidation by activating AMP-activated protein kinaseNature, 2002
- Insulin receptor phosphorylation, insulin receptor substrate-1 phosphorylation, and phosphatidylinositol 3-kinase activity are decreased in intact skeletal muscle strips from obese subjects.Journal of Clinical Investigation, 1995
- Analysis of Acyl Coenzyme A Binding to the Transcription Factor FadR and Identification of Amino Acid Residues in the Carboxyl Terminus Required for Ligand BindingPublished by Elsevier ,1995
- Impaired free fatty acid utilization by skeletal muscle in non-insulin-dependent diabetes mellitus.Journal of Clinical Investigation, 1994
- Mechanisms of fatty acid-induced inhibition of glucose uptake.Journal of Clinical Investigation, 1994
- Effect of fatty acids and their acyl-CoA esters on protein kinase C activity in fibroblasts: Possible implications in fatty acid oxidation defectsBiochimica et Biophysica Acta (BBA) - Molecular Cell Research, 1994
- Interaction between glucose and free fatty acid metabolism in human skeletal muscle.Journal of Clinical Investigation, 1993
- Palmitoyl‐CoA and the acyl‐CoA thioester of the carcinogenic peroxisome‐proliferator ciprofibrate potentiate diacylglycerol‐activated protein kinase C by decreasing the phosphatidylserine requirement of the enzymeEuropean Journal of Biochemistry, 1990
- THE GLUCOSE FATTY-ACID CYCLE ITS ROLE IN INSULIN SENSITIVITY AND THE METABOLIC DISTURBANCES OF DIABETES MELLITUSPublished by Elsevier ,1963