Neurobiol Lipids 1, 1 (10 July 2002) find out how to cite this article

Mike A Simmonds

Department of Pharmacology, School of Pharmacy, 29/39 Brunswick Square London WC1N 1AX UK,
email: mike.simmonds01@btopenworld.com ; mikesimmonds@neurobiologyoflipids.org

Published online: 10 July, 2002 | Article readership
Copyright © 2002 M A Simmonds, Licensee Neurobiology of Lipids

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FIRST PARAGRAPH CHOLESTEROL AND CELL MEMBRANE STRUCTURE CHOLESTEROL AS A STEROIDAL PRECURSOR MODULATION OF MEMBRANE PROTEINS

MANIPULATION OF MEMBRANE CHOLESTEROL IN VIVO CHOLESTEROL AND NEURODEGENERATION PROSPECT WEB ENHANCED REFERENCES

Although cholesterol gets a bad press as a cause of vascular disease, it is, of course, an essential component of all mammalian cells.  In neurobiology, three quite different roles of cholesterol can be discerned: as a structural component of the plasma membranes of neurones and glia; as the precursor for a cascade of steroidal hormones and mediators affecting both genomic and non-genomic processes in neurones; and as a direct modulator of the functions of certain plasma membrane proteins..

In the early 1980s, there was a flurry of activity involving a variety of membrane proteins.  Interpretations of the protein/lipid interactions observed were strongly influenced by the considerable body of in-depth work that had been published on the biophysical properties of lipid bilayers and biological membranes.  Thus, membrane fluidity was the prime mechanism considered for lipid modulation of protein function.  However, several authors who manipulated membrane cholesterol levels to achieve changes in fluidity recognised the possibility that cholesterol itself might exert additional direct effects.  Examples include studies on adenylate cyclase [4], GABA uptake transporters [5] and the nicotinic acetylcholine receptor of Torpedo [6].

Continued interest in this aspect of nicotinic acetylcholine receptor regulation [7, 8] further strengthened the evidence in support of distinctive influences by membrane fluidity and direct cholesterol-protein interactions, including the dependence of the latter on specific phospholipids.  In the meantime, other receptor proteins were studied with regard to mechanisms of modulation by membrane cholesterol, including the visual pigment rhodopsin [9], oxytocin and cholecystokinin receptors [10] and the GABA_A receptor [11, 12, 13].  A recent analogous study on multidrug resistance P-glycoprotein [14] demonstrated a wider applicability of the phenomenon.

The free cholesterol in cells is located almost entirely in the plasma membrane. It has proved quite easy to manipulate the cholesterol content in vitro and a variety of methods is described in the foregoing references.  It has also been concluded that, in well-perfused tissues in vivo other than the central nervous system, the free cholesterol content would exchange completely with circulating free cholesterol within about 1 day [15].  Not surprisingly, therefore, lowering of circulating cholesterol levels in hypercholesterolaemic patients by treatment with pravastatin has been shown to result in decreases in erythrocyte and platelet membrane cholesterol contents [16].  Moreover, these changes were associated with an increase in Na⁺ pump activity in these membranes.  Although the wider implications of these observations for the functioning of other cell types were pointed out by the authors, there appear to be no related reports in the literature to date.

With regard to the central nervous system, whole brain levels of cholesterol are found to be quite stable.  The turnover is very low, the source of new cholesterol being synthesis in the brain rather than circulating plasma cholesterol, for which a blood/brain barrier may operate [17, 18].  Myelin contains a substantial proportion of the brain cholesterol and may account for the stable level overall. It is possible, however, that the fraction of cholesterol present in grey matter may be more labile.  For example, mice fed a diet containing 5% cholesterol for 8 weeks, which resulted in a 200% increase in serum cholesterol, were found to have no significant increase in whole brain cholesterol but they did show a significant 20% increase in cholesterol measured in frontal cortex, which has less white matter than the brain as a whole [19].  Increases in brain cholesterol as a result of atherogenic diets have also been reported for rabbits, in which the regional increases were correlated with increases in beta-amyloid immunoreactivity [20], and for rats, in which there was an associated fall in brain Ca²⁺-ATPase activity [21].

A more subtle effect has been seen in mice on a chronic ethanol diet.  Although there was no consistent change in brain cholesterol content, there was a significant shift in the assymetric distribution of cholesterol between cytofacial and exofacial leaflets of synaptic plasma membranes.  In control mice, 88% of the membrane cholesterol was present in the cytofacial leaflet whereas in the ethanol-treated mice this was reduced to 72% [22].  A corresponding increase in fluidity of the cytofacial leaflet and decrease in fluidity of the exofacial leaflet was found in the ethanol-treated compared with the control mice [23].  A similar redistribution of synaptic plasma membrane cholesterol has been seen with ageing in mice [24].

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This article should be cited in the following way: Simmonds MA. The emerging neurobiology of cholesterol. Neurobiol. Lipids  Vol.1, 1 (2002), Published online July 10, 2002, Available at: http://neurobiologyoflipids.org/content/1/1/ Please note: Because Neurobiology of Lipids is published online only,  the articles are identified with an article number rather than with traditional (printed) page numbers

 

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