Physical effects of cholesterol on arterial smooth muscle membranes: evidence of immiscible cholesterol domains and alterations in bilayer width during atherogenesis

Thomas N. Tulenko; Meng Chen; Pamela E. Mason; R. Preston Mason

Journal of Lipid Research (May 1998)

Physical effects of cholesterol on arterial smooth muscle membranes: evidence of immiscible cholesterol domains and alterations in bilayer width during atherogenesis

Thomas N. Tulenko,
Meng Chen,
Pamela E. Mason,
R. Preston Mason

Affiliations

Thomas N. Tulenko: To whom correspondence should be addressed.; Neurosciences Research Center, Allegheny University of the Health Sciences, MCP·Hahnemann School of Medicine, Allegheny Campus, Pittsburgh, PA 15212-4772
Meng Chen: Neurosciences Research Center, Allegheny University of the Health Sciences, MCP·Hahnemann School of Medicine, Allegheny Campus, Pittsburgh, PA 15212-4772
Pamela E. Mason: Department of Physiology, Allegheny University of the Health Sciences, MCP·Hahnemann School of Medicine, 2900 Queen Lane, Philadelphia, PA 19129
R. Preston Mason: To whom correspondence should be addressed.; Department of Physiology, Allegheny University of the Health Sciences, MCP·Hahnemann School of Medicine, 2900 Queen Lane, Philadelphia, PA 19129

Journal volume & issue: Vol. 39, no. 5
pp. 947 – 956

Abstract

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Small angle X-ray diffraction was used to examine arterial smooth muscle cell (SMC) plasma membranes isolated from control and cholesterol-fed (2%) atherosclerotic rabbits. A microsomal membrane enriched with plasma membrane obtained from animals fed cholesterol for up to 13 weeks showed a progressive elevation in the membrane unesterified (free) cholesterol:phospholipid (C/PL) mole ratio. Beyond 9 weeks of cholesterol feeding, X-ray diffraction patterns demonstrated a lateral immiscible cholesterol domain at 37°C with a unit cell periodicity of 34 Å coexisting within the liquid crystalline lipid bilayer. On warming, the immiscible cholesterol domain disappeared, and on cooling it reappeared, indicating that the immiscible cholesterol domain was fully reversible. These effects were reproduced in a model C/PL binary lipid system. In rabbits fed cholesterol for less than 9 weeks, lesser increases in membrane C/PL mole ratio were observed. X-ray diffraction analysis demonstrated an increase in membrane bilayer width that correlated with the C/PL mole ratio. This effect was also reproduced in a C/PL binar y lipid system. Taken together, these findings demonstrate that in vivo, feeding of cholesterol causes cholesterol–phospholipid interactions in the membrane bilayer that alter bilayer structure and organization. This interaction results in an increase in bilayer width peaking at a saturating membrane cholesterol concentration, beyond which lateral phase separation occurs resulting in the formation of separate cholesterol bilayer domains. These alterations in structure and organization in SMC plasma membranes may have significance in phenotypic modulation or aortic SMC during early atherogenesis.—Tulenko, T. N., M. Chen, P. E. Mason, and R. P. Mason. Physical effects of cholesterol on arterial smooth muscle membranes: evidence of immiscible cholesterol domains and alterations in bilayer width during atherogenesis. J. Lipid Res. 1998. 39: 947–956.

Published in Journal of Lipid Research

ISSN: 0022-2275 (Print); 1539-7262 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Science: Chemistry: Organic chemistry: Biochemistry
Website: https://www.journals.elsevier.com/journal-of-lipid-research

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