Abstract

Cholesteryl ester-loaded macrophages (Mfs), or foam cells, which are prominent and important in atherosclerosis, form by the interaction of Mf with atherogenic lipoproteins (Lps), followed by stimulation of intracellular cholesterol esterification (CE'tion). That one type of atherogenic particle, b-VLDL, enters Mfs by unique cell-surface invaginations called STEMs (surface tubules for entry into Mfs) was recently discovered. The STEM pathway appears to be important in CE'tion and, remarkably, partial b-VLDL catabolism occurs in these cell-surface sites. Preliminary studies have revealed that another important class of atherogenic lipoproteins--retained & aggregated LDL--interacts with the Mf cell surface for an even longer time period than b-VLDL. This finding, together with the physiological importance and paucity of prior data regarding the interaction of retained & aggregated LDL with Mfs, provides a strong rationale for further study in this area. Thus, the overall objectives of this proposal are to first elucidate important cellular and biochemical events involved in the interaction of retained & aggregated LDL with Mfs and then to test specific hypotheses linking the cell-surface pathway involved with both b-VLDL (STEMs) and retained & aggregated LDL to the stimulation of intracellular CE'tion. To evaluate and refine these hypotheses, particularly as they relate to retained and aggregated LDL, fluorescence & electron microscopy and biochemical methods will be used in aim 1 to elucidate precisely how these lipoproteins interact with the Mf cell-surface and how they affect intracellular cholesterol metabolism. An important hypothesis to be tested is that CE'tion is stimulated during the period of prolonged cell-surface interaction.
In aim 2, the lipoprotein component(s) and the hydrolase(s) that are involved in the partial cell-surface catabolism known to occur with b-VLDL in STEMs and predicted to occur with retained & aggregated LDL will be identified.
Aim 3 will use the information obtained in the first two aims to address the roles of four processes that are hypothesized to link cell-surface events to intracellular CE'tion: (1) cell-surface catabolism as a facilitator of Lp-cholesterol transfer to cells; (2) direct transfer of the free cholesterol moiety of Lps to the Mf plasma membrane; (3) physical interactions between cholesterol and ACAT, including possible Lp-induced alterations in ACAT localization; and (4) signal transduction events involving changes in protein phosphorylation. The information gained from these studies may suggest new therapeutic strategies, directed at the level of the lesion foam cell, for further lowering the risk of atherosclerotic heart disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL057560-04
Application #
6165069
Study Section
Physiological Chemistry Study Section (PC)
Project Start
1997-03-15
Project End
2001-02-28
Budget Start
2000-03-01
Budget End
2001-02-28
Support Year
4
Fiscal Year
2000
Total Cost
$360,935
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
167204994
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Zhou, Alex-Xianghua; Wang, Xiaobo; Lin, Chyuan Sheng et al. (2015) C/EBP-Homologous Protein (CHOP) in Vascular Smooth Muscle Cells Regulates Their Proliferation in Aortic Explants and Atherosclerotic Lesions. Circ Res 116:1736-43
Tabas, Ira; Glass, Christopher K (2013) Anti-inflammatory therapy in chronic disease: challenges and opportunities. Science 339:166-72
Woo, Connie W; Kutzler, Lydia; Kimball, Scot R et al. (2012) Toll-like receptor activation suppresses ER stress factor CHOP and translation inhibition through activation of eIF2B. Nat Cell Biol 14:192-200
Moore, Kathryn J; Tabas, Ira (2011) Macrophages in the pathogenesis of atherosclerosis. Cell 145:341-55
Ouimet, Mireille; Franklin, Vivian; Mak, Esther et al. (2011) Autophagy regulates cholesterol efflux from macrophage foam cells via lysosomal acid lipase. Cell Metab 13:655-67
Shechtman, Caryn F; Henneberry, Annette L; Seimon, Tracie A et al. (2011) Loss of subcellular lipid transport due to ARV1 deficiency disrupts organelle homeostasis and activates the unfolded protein response. J Biol Chem 286:11951-9
Devlin, Cecilia; Pipalia, Nina H; Liao, Xianghai et al. (2010) Improvement in lipid and protein trafficking in Niemann-Pick C1 cells by correction of a secondary enzyme defect. Traffic 11:601-15
Thorp, Edward; Li, Gang; Seimon, Tracie A et al. (2009) Reduced apoptosis and plaque necrosis in advanced atherosclerotic lesions of Apoe-/- and Ldlr-/- mice lacking CHOP. Cell Metab 9:474-81
Haka, Abigail S; Grosheva, Inna; Chiang, Ethan et al. (2009) Macrophages create an acidic extracellular hydrolytic compartment to digest aggregated lipoproteins. Mol Biol Cell 20:4932-40
Manning-Tobin, Jennifer J; Moore, Kathryn J; Seimon, Tracie A et al. (2009) Loss of SR-A and CD36 activity reduces atherosclerotic lesion complexity without abrogating foam cell formation in hyperlipidemic mice. Arterioscler Thromb Vasc Biol 29:19-26

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