Probing Red Cell Membrane Cholesterol Movement with Cyclodextrin

Steck, Theodore L.; Ye, Jin; Lange, Yvonne

doi:10.1016/s0006-3495(02)73972-6

Cited by 233 publications

(210 citation statements)

References 55 publications

(84 reference statements)

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“…4 shows that apoA1 and HDL failed to induce Abcg5/g8 specific efflux. A similar result was observed for methyl-b-cyclodextrin, which in contrast to apoA1 or HDL does not interact with proteins but takes up cholesterol directly from the membrane [22]. Since this cholesterol acceptor is very potent and may overrule the importance of Abcg5/g8 we have used limiting amounts of the acceptor and carried out kinetic studies.…”

Section: Resultssupporting

confidence: 65%

The sterol transporting heterodimer ABCG5/ABCG8 requires bile salts to mediate cholesterol efflux

et al. 2007

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The ATP binding cassette transporters ABCG5 and ABCG8 are indispensable for hepatobiliary cholesterol transport. In this study, we investigated the specificity of the heterodimer for cholesterol acceptors. Dog gallbladder epithelial cells were mono-or double-transfected with lentiviral mouse Abcg5 and Abcg8 vectors. Double-transfected cells showed increased efflux to different bile salt (BS) species, while mono-transfected cells did not show enhanced efflux. The efflux was initiated at micellar concentrations and addition of phosphatidylcholine increased efflux. Cholesterol secretion was highly BS dependent, whereas other cholesterol acceptors such as ApoAI, HDL or methyl-b-cyclodextrin did not elicit Abcg5/g8 dependent cholesterol secretion.

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Section: Resultssupporting

confidence: 65%

The sterol transporting heterodimer ABCG5/ABCG8 requires bile salts to mediate cholesterol efflux

et al. 2007

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“…MBCD depletes cholesterol from plasma membranes by sequestering cholesterol in its hydrophobic pocket (27). This effect is rapid.…”

Section: Modeling the Effect Of Diabetes On Neurons By Cholesterol Dementioning

confidence: 99%

Effect of Cholesterol Reduction on Receptor Signaling in Neurons

Fukui¹,

Ferris²,

Kahn

2015

Journal of Biological Chemistry

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Background: Cholesterol synthesis is decreased in the brain in diabetes. Results: Cholesterol depletion in neuron-derived cells results in impaired insulin/IGF-1 and neurotrophin signaling and altered apoptosis. Conclusion: Reduction of cellular cholesterol in diabetes causes defects in signal transduction and function in neuron-derived cells. Significance: Reduced brain cholesterol could contribute to the higher prevalence of cognitive dysfunction and Alzheimer disease in diabetes.

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“…While the lateral and transverse distributions of cholesterol are apparently each in rapid diffusional equilibrium, the tendencies of the sterol population at each leaflet to project into the neighboring aqueous space do not come to equilibrium but rather remain different from one another. The transfer of membrane cholesterol to aqueous acceptors such as cyclodextrin appears to depend on this bobbing motion (6). In particular, it is during these transient projections that sterol molecules are captured by collision with the acceptors.…”

Section: Discussionmentioning

confidence: 99%

“…Cholesterol equilibrates rapidly between the two leaflets of the PM bilayer; however, its transbilayer distribution is debated (6). The transverse distribution of the PM PLs is asymmetrical, with a preponderance of PC and SM in the exofacial leaflet and anionic PL, mostly PE and PS, in the cytoplasmic leaflet (7).…”

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confidence: 99%

Scrambling of Phospholipids Activates Red Cell Membrane Cholesterol

Lange

Steck

2007

Biochemistry

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Cholesterol is predicted to associate more strongly with the outer than the inner leaflet of plasma membrane bilayers based on the relative in vitro affinities of their phospholipids. Complex formation with the high affinity species (especially saturated sphingomyelins) is said to reduce the chemical activity (escape potential or fugacity) of the sterol. We therefore tested the hypothesis that scrambling the sidedness of plasma membrane phospholipids of intact cells will increase the chemical activity of outer surface cholesterol. Upon activating the plasma membrane scramblase in intact human red cells by introducing ionomycin to raise cytoplasmic Ca ++ , phosphatidylserine became exposed and, concomitantly, the chemical activity of exofacial cholesterol was increased. (This was gauged by its susceptibility to cholesterol oxidase and its rate of transfer to cyclodextrin.) Similar behavior was observed in human fibroblasts. Two other treatments known to activate cell surface cholesterol (namely, exposure to glutaraldehyde and to low ionic strength buffer) also brought phosphatidylserine to the cell surface but by a Ca ++ -independent mechanism. Given that phospholipid scrambling is important in blood coagulation and apoptosis, the concomitant activation of cell surface cholesterol could contribute to these and other pathophysiological signaling processes.It has been observed that increasing the cholesterol in the mammalian PM 1 beyond the physiological level evokes a sharp rise in its susceptibility to attack by CO and in its transfer both to extracellular cyclodextrin and the endoplasmic reticulum (1,2). These findings have been explained by the following hypothesis (2,3): Cholesterol forms complexes of varied strength and stoichiometry with different bilayer PLs. The complexed sterol has a lower chemical activity (escape potential or fugacity) than uncomplexed (free) cholesterol; for example, that added in excess of the binding capacity of the PL. It is the high chemical activity of the uncomplexed sterol that accounts for its increased interaction with CO and cyclodextrin. Physiologically, the high fugacity of excess cholesterol provides a homeostatic mechanism that keeps the PM sterol level near the capacity of its PL partners, ~0.8 mol per mol phospholipid (4). [Note that the concept of cholesterol chemical activity of interest here differs distinctly from that of active cholesterol, which refers to the attributes of biologically functional sterols (5).] † This work was supported in part by National Institutes of Health grant HL 28448.* To whom correspondence should be addressed at ‡ Dept. of Pathology, Rush University Medical Center, 1653 West Congress Parkway, Chicago, IL 60612. Tel: 312-942-5256; Fax: 312-563-3115; E-mail: ylange@rush.edu. 1 The abbreviations used are: CO, cholesterol oxidase; DIDS, 4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid; ER, endoplasmic reticulum; HBS, 150 mM NaCl-5 mM histidine, pH 7.5; MBCD, methyl-β-cyclodextrin; PBS, 150 mM NaCl-5 mM NaPi, pH 7.5; PC, phosphatidylc...

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Probing Red Cell Membrane Cholesterol Movement with Cyclodextrin

Cited by 233 publications

References 55 publications

The sterol transporting heterodimer ABCG5/ABCG8 requires bile salts to mediate cholesterol efflux

The sterol transporting heterodimer ABCG5/ABCG8 requires bile salts to mediate cholesterol efflux

Effect of Cholesterol Reduction on Receptor Signaling in Neurons

Scrambling of Phospholipids Activates Red Cell Membrane Cholesterol

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