CD36 Mediates Both Cellular Uptake of Very Long Chain Fatty Acids and Their Intestinal Absorption in Mice

Drover, Victor A.; Nguyen, David; Bastie, Claire C.; Darlington, Yolanda F.; Abumrad, Nada A.; Pessin, Jeffrey E.; London, Erwin; Sahoo, Daisy; Phillips, Michael C.

doi:10.1074/jbc.m708086200

Cited by 138 publications

(123 citation statements)

References 31 publications

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“…Interestingly, micelle binding to both transporters was positively correlated to chain length and unsaturation. This is in line with the concept of longchain fatty acids being CD36 ligands ( 37 ). Moreover, accordingly to our SPR data showing that free OA and DHA were SR-BI ligands, mice overexpressing SR-BI at the A key fi nding is that these structures mimicking mixed micelles, i.e., including various lipids and lipid digestion products, are necessary for optimal binding to both lCD36 and lSR-BI.…”

Section: Discussionsupporting

confidence: 63%

Micellar lipid composition affects micelle interaction with class B scavenger receptor extracellular loops

Goncalves

Gontero

Nowicki

et al. 2015

Journal of Lipid Research

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International audienceScavenger receptors (SRs) like cluster determinant 36 (CD36) and SR class B type I (SR-BI) play a debated role in lipid transport across the intestinal brush border membrane. We used surface plasmon resonance to analyze real-time interactions between the extracellular protein loops and various ligands ranging from single lipid molecules to mixed micelles. Micelles mimicking physiological structures were necessary for optimal binding to both the extracellular loop of CD36 (lCD36) and the extracellular loop of SR-BI (lSR-BI). Cholesterol, phospholipid, and fatty acid micellar content significantly modulated micelle binding to and dissociation from the transporters. In particular, high phospholipid micellar concentrations inhibited micelle binding to both receptors (−53.8 and −74.4% binding at 0.32 mM compared with 0.04 mM for lCD36 and lSR-BI, respectively, P < 0.05). The presence of fatty acids was crucial for micelle interactions with both proteins (94.4 and 81.3% binding with oleic acid for lCD36 and lSR-BI, respectively, P < 0.05) and fatty acid type substitution within the micelles was the component that most impacted micelle binding to the transporters. These effects were partly due to subsequent modifications in micellar size and surface electric charge, and could be correlated to micellar vitamin D uptake by Caco-2 cells. Our findings show for the first time that micellar lipid composition and micellar properties are key factors governing micelle interactions with SRs

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Section: Discussionsupporting

confidence: 63%

Micellar lipid composition affects micelle interaction with class B scavenger receptor extracellular loops

Goncalves

Gontero

Nowicki

et al. 2015

Journal of Lipid Research

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“…mice on a C57BL/6 background were produced and characterized as described earlier ( 33 ( 36 ). As expected, 4 h after the gavage of a bolus containing radiolabeled cholesterol and sitostanol, much more cholesterol than sitostanol is present in the intestinal wall.…”

Section: Methodsmentioning

confidence: 99%

“…A weighed sample of liver was analyzed in a similar fashion. Plasma samples were prepared from the blood and analyzed for radioactive sterols by liquid scintillation counting and for cholesterol levels by an enzymatic assay ( 33 ).…”

Section: Methodsmentioning

confidence: 99%

“…The class B scavenger receptors cluster determinant 36 (CD36) ( 29 ) and scavenger receptor class B, type 1 (SR-BI) ( 30 ), which have established lipid transport capabilities, have been known for a decade or more to be located in the BBM and can potentially mediate cholesterol uptake into the BBM. Indeed, experiments with mice in which these genes are deleted have demonstrated that SR-BI is important for the absorption of ␤ -carotene ( 31 ) and vitamin E ( 32 ), and CD36 is important for the absorption of very long chain fatty acids ( 33 ). However, there is no effect on cholesterol absorption of deleting either SR-BI ( 31,34,35 ) or CD36 ( 36 ), although both receptors have been shown to facilitate the transport of cholesterol into cells ( 31,37,38 ).…”

Section: Real-time Pcrmentioning

confidence: 99%

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Influence of class B scavenger receptors on cholesterol flux across the brush border membrane and intestinal absorption

Nguyen

Drover

Knöpfel

et al. 2009

Journal of Lipid Research

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The effi ciency of absorption of dietary cholesterol in the small intestine affects plasma LDL cholesterol levels and thereby cardiovascular disease risk ( 1, 2 ). Consequently, there is great interest in understanding the mechanism of intestinal cholesterol absorption and inhibiting the process to reduce plasma cholesterol levels. Ezetimibe is such an inhibitor whose target is the protein NiemannPick C1-like 1 (NPC1L1) ( 3, 4 ); the importance of this protein in cholesterol absorption is refl ected by the fact that the absorption effi ciency is greatly reduced in mice lacking the gene encoding NPC1L1 ( 5, 6 ). Experiments with knockout and transgenic mice have variously demonstrated that acylCoA:cholesterol-acyltransferase-2 (ACAT-2) ( 7-9 ) and ATP binding cassette half transporters G5 and G8 (ABCG5/G8) ( 10-13 ) also play critical roles in the cholesterol absorption pathway. The above proteins are all involved in enterocyte cholesterol homeostasis ( 14, 15 ), but factors such as lipase activity and bile salt availability in the earlier digestive phase of the pathway are also critical (for recent reviews, see Refs. 14 and 16 ). Current understanding of the proteins and mechanisms controlling the uptake of cholesterol from the lumen of the small intestine into and across the brush border membrane (BBM) is relatively limited. Here, we distinguish between cholesterol uptake and cholesterol absorption, defi ning the former as the process of cholesterol transfer from the donor particle in the lumen of the small intestine to the BBM and the latter as the cascade of transport steps Press, May 19, 2009 DOI 10.1194 Abbreviations: ABCG5/G8, ATP binding cassette half transporters G5 and G8; ACAT-2, acylCoA:cholesterol-acyltransferase-2; BBM, brush border membrane; BBMV, brush border membrane vesicle; BSM, mixed bile salt micelle; CD36, cluster determinant 36; HFHC, high-fat/ high-cholesterol diet; NPC1L1, Niemann Pick C1-Like 1; SR-BI, scavenger receptor class B, type 1; SUV, small unilamellar vesicle; WT, wild type. Published, JLR Papers in

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“…FAT/CD36 in particular is important for very long-chain (VLC) FA (more than 18 carbon atoms) metabolism, since intestinal VLCFA uptake was completely abolished in CD36 2/2 mice [55]. Lobo et al [56] described that in humans, FAT/CD36 protein was restricted to duodenal and jejunal epithelium.…”

Section: Sterol and Lcfa Transportersmentioning

confidence: 99%

Fatty Acid- and Cholesterol Transporter Protein Expression along the Human Intestinal Tract

Masson¹,

Mensink²,

Namiot³

et al. 2010

Atherosclerosis Supplements

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CD36 Mediates Both Cellular Uptake of Very Long Chain Fatty Acids and Their Intestinal Absorption in Mice

Cited by 138 publications

References 31 publications

Micellar lipid composition affects micelle interaction with class B scavenger receptor extracellular loops

Micellar lipid composition affects micelle interaction with class B scavenger receptor extracellular loops

Influence of class B scavenger receptors on cholesterol flux across the brush border membrane and intestinal absorption

Fatty Acid- and Cholesterol Transporter Protein Expression along the Human Intestinal Tract

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