FAT/CD36 is localized in sarcolemma and in vesicle-like structures in subsarcolemma regions but not in mitochondria

Jeppesen, Jacob; Mogensen, Martin; Prats, Clara; Sahlin, Kent; Madsen, Klavs; Kiens, Bente

doi:10.1194/jlr.m003756

Cited by 29 publications

(26 citation statements)

References 59 publications

(59 reference statements)

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“…Bezaire and colleagues put forth the notion that fatty acid transporters FAT/CD and FATP1 are involved in the transfer of FAs into the mitochondria possibly by direct binding to the mitochondrial membrane (66, 96). This work is recently disputed by Jeppesen et al (315). Regardless of whether these proteins bind directly to mitochondria, at least in the case of FATP, skeletal muscle-specific overexpression in mice promoted increased skeletal muscle fatty acid uptake and oxidation specifically, but did not predispose animals to diet-induced insulin resistance (274).…”

Section: Mechanisms Of Insulin Resistancementioning

confidence: 94%

Metabolic Syndrome and Insulin Resistance: Underlying Causes and Modification by Exercise Training

Roberts

Hevener

Barnard

2013

Comprehensive Physiology

450

425

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Metabolic syndrome (MS) is a collection of cardiometabolic risk factors that includes obesity, insulin resistance, hypertension, and dyslipidemia. Although there has been significant debate regarding the criteria and concept of the syndrome, this clustering of risk factors is unequivocally linked to an increased risk of developing type 2 diabetes and cardiovascular disease. Regardless of the true definition, based on current population estimates, nearly 100 million have MS. It is often characterized by insulin resistance, which some have suggested is a major underpinning link between physical inactivity and MS. The purpose of this review is to: (i) provide an overview of the history, causes and clinical aspects of MS, (ii) review the molecular mechanisms of insulin action and the causes of insulin resistance, and (iii) discuss the epidemiological and intervention data on the effects of exercise on MS and insulin sensitivity.

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Section: Mechanisms Of Insulin Resistancementioning

confidence: 94%

Metabolic Syndrome and Insulin Resistance: Underlying Causes and Modification by Exercise Training

Roberts

Hevener

Barnard

2013

Comprehensive Physiology

450

425

View full text Add to dashboard Cite

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“…Because we could not isolate mitochondrial membrane fractions on top of nuclear fractions from the small amount of hindlimb muscles that we had, we could not determine whether CD36 protein content was altered in mitochondrial membranes. Indeed, it has been suggested by some (18,19), but not others (23), that mitochondrial membrane CD36 content is an important factor in the regulation of FA oxidation. Because of the methodological limitations described above, we cannot contribute data to this debate.…”

Section: Discussionmentioning

confidence: 99%

AMPKα₂deficiency uncovers time dependency in the regulation of contraction-induced palmitate and glucose uptake in mouse muscle

Abbott

Bogachus²,

Turcotte

2011

Journal of Applied Physiology

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Abbott MJ, Bogachus LD, Turcotte LP. AMPK␣2 deficiency uncovers time dependency in the regulation of contraction-induced palmitate and glucose uptake in mouse muscle. J Appl Physiol 111: 125-134, 2011. First published May 5, 2011 doi:10.1152/japplphysiol.00807.2010.-AMP-activated protein kinase (AMPK) is a fuel sensor in skeletal muscle with multiple downstream signaling targets that may be triggered by increases in intracellular Ca 2ϩ concentration ([Ca 2ϩ ]). The purpose of this study was to determine whether increases in intracellular [Ca 2ϩ ] induced by caffeine act solely via AMPK␣ 2 and whether AMPK␣2 is essential to increase glucose uptake, fatty acid (FA) uptake, and FA oxidation in contracting skeletal muscle. Hindlimbs from wild-type (WT) or AMPK␣ 2 dominant-negative (DN) transgene mice were perfused during rest (n ϭ 11), treatment with 3 mM caffeine (n ϭ 10), or muscle contraction (n ϭ 11). Time-dependent effects on glucose and FA uptake were uncovered throughout the 20-min muscle contraction perfusion period (P Ͻ 0.05). Glucose uptake rates did not increase in DN mice during muscle contraction until the last 5 min of the protocol (P Ͻ 0.05). FA uptake rates were elevated at the onset of muscle contraction and diminished by the end of the protocol in DN mice (P Ͻ 0.05). FA oxidation rates were abolished in the DN mice during muscle contraction (P Ͻ 0.05). The DN transgene had no effect on caffeine-induced FA uptake and oxidation (P Ͼ 0.05). Glucose uptake rates were blunted in caffeine-treated DN mice (P Ͻ 0.05). The DN transgene resulted in a greater use of intramuscular triglycerides as a fuel source during muscle contraction. The DN transgene did not alter caffeine-or contraction-mediated changes in the phosphorylation of Ca 2ϩ /calmodulin-dependent protein kinase I or ERK1/2 (P Ͼ 0.05). These data suggest that AMPK␣ 2 is involved in the regulation of substrate uptake in a time-dependent manner in contracting muscle but is not necessary for regulation of FA uptake and oxidation during caffeine treatment. ERK1/2; muscle contraction; caffeine; calcium/calmodulin-dependent protein kinase kinase; acetyl-CoA carboxylase EVIDENCE SUGGESTS THAT MULTIPLE cellular signals regulate the changes in substrate metabolism with muscle contraction, including the AMP-activated protein kinase (AMPK) signaling cascade (2, 34, 35, 52). During states of low energy, such as muscle contraction or exercise, it is widely accepted that liver kinase B1 (LKB1) acts as an upstream AMPK kinase that phosphorylates and activates AMPK and initiates a multitude of signaling events to maintain energy homeostasis (39 -41). Although strong evidence indicates that the LKB1-AMPK cascade is a key signaling pathway that regulates changes in glucose uptake, fatty acid (FA) uptake, and FA oxidation in contracting skeletal muscle (16,25,54,56), data also show that AMPK may not be the sole signal mediating contractioninduced changes in glucose uptake, FA uptake, and FA oxidation (35,36,56).Along with AMPK, mounting data suggest that increas...

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“…In addition increased mitochondrial CD36 content paralleled upregulation of FA oxidation [70-72]. Association of CD36 with mitochondria could not be observed in one study that used both biochemical fractionation and imaging and tested co-localization of CD36 with the mitochondrial protein MitoNeet [73]. This discrepancy might reflect the possibility that CD36 association with the mitochondria is dynamically regulated and could reflect a CD36 pool in mitochondria-associated membranes.…”

Section: Sarcolemmal Cd36 Targets Fas To Metabolic Sitesmentioning

confidence: 99%

CD36 actions in the heart: Lipids, calcium, inflammation, repair and more?

Abumrad

Goldberg

2016

Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biolog

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CD36 is a multifunctional immuno-metabolic receptor with many ligands. One of its physiological functions in the heart is the high-affinity uptake of long-chain fatty acids (FAs) from albumin and triglyceride rich lipoproteins. CD36 deletion markedly reduces myocardial FA uptake in rodents and humans. The protein is expressed on endothelial cells and cardiomyocytes and at both sites is likely to contribute to FA uptake by the myocardium. CD36 also transduces intracellular signaling events that influence how the FA is utilized and mediate metabolic effects of FA in the heart. CD36 mediated signaling regulates AMPK activation in a way that adjusts oxidation to FA uptake. It also impacts remodeling of myocardial phospholipids and eicosanoid production, effects exerted via influencing intracellular calcium (iCa2+) and the activation of phospholipases. Under excessive FA supply CD36 contributes to lipid accumulation, inflammation and dysfunction. However, it is also important for myocardial repair after injury via its contribution to immune cell clearance of apoptotic cells. This review describes recent progress regarding the multiple actions of CD36 in the heart and highlights those areas requiring future investigation.

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FAT/CD36 is localized in sarcolemma and in vesicle-like structures in subsarcolemma regions but not in mitochondria

Cited by 29 publications

References 59 publications

Metabolic Syndrome and Insulin Resistance: Underlying Causes and Modification by Exercise Training

Metabolic Syndrome and Insulin Resistance: Underlying Causes and Modification by Exercise Training

AMPKα₂deficiency uncovers time dependency in the regulation of contraction-induced palmitate and glucose uptake in mouse muscle

CD36 actions in the heart: Lipids, calcium, inflammation, repair and more?

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FAT/CD36 is localized in sarcolemma and in vesicle-like structures in subsarcolemma regions but not in mitochondria

Cited by 29 publications

References 59 publications

Metabolic Syndrome and Insulin Resistance: Underlying Causes and Modification by Exercise Training

Metabolic Syndrome and Insulin Resistance: Underlying Causes and Modification by Exercise Training

AMPKα2deficiency uncovers time dependency in the regulation of contraction-induced palmitate and glucose uptake in mouse muscle

CD36 actions in the heart: Lipids, calcium, inflammation, repair and more?

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AMPKα₂deficiency uncovers time dependency in the regulation of contraction-induced palmitate and glucose uptake in mouse muscle