Abstract

Macrophages (Mphi) loaded with free cholesterol (PC) and phospholipid (PL) are prominent in atherosclerotic lesions, and events associated with the necrosis of these cells appear to be a least partly responsible for lesion progression. The major goal of this proposal is to explore several hypotheses that relate lipid changes in Mphi wit foam cell necrosis and lesion progression. Preliminary studies have demonstrated that FC loading of cultured Mphi initially leads to an increase in cellular phosphatidylcholine (PC) due to stimulation of CTP:phosphocholine cytidylyltransferase (CT), which probably represents an adaptive response to av awed the toxicity of high PC:PL ratios. After long-term PC loading, however, the PL content of the cultured Mphi begins to decrease, and the cells subsequently show signs of toxicity. In this context, Aim #1 will explore several specific ideas regarding the molecular mechanisms responsible for the initial up-regulation of CT in FC-loaded Mphi.
In Aim #2, the biochemical and morphological properties associated with the toxicity of long-term FC-loaded Mphi in culture will be defined, and manipulations of PL metabolism in these cells will be used to explore several specific hypotheses relating Pl changes in these cells to cytotoxicity. These hypotheses are; (a) a toxic cellular FC:PL ratio, resulting from an eventual decrease in cellular pl mass, leads to Mphi toxicity and necrosis; (b) the generation of lysoPC, resulting from the exposure of the excess Mphi PL to phospholipase, leads to Mphi toxicity and necrosis; and (c) the generation of ceramide, resulting from the exposure of the excess Mphi sphingomyelin to sphingomyelinases, leads to Mphi apoptosis. The goal of Aim #3 is to explore these cytotoxicity hypotheses in a physiological setting using mouse models of atherosclerosis. First, lesion of atherosclerosis-susceptible apo E knockout (EO) mice will be carefully examined to determine if increases in FC:PL ratio, lysoPC, and/or ceramide precede the onset of lesion Mphi necrosis. Then, CT transgenic mice and Mphi-specific or heterozygous CT knockout mice will be created and crossed with EO mice to show that manipulations of PC metabolism can affect lesion necrosis and progression in vivo.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL054591-04
Application #
6273086
Study Section
Project Start
1998-07-01
Project End
1999-06-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
4
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Rockefeller University
Department
Type
DUNS #
071037113
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Fredman, Gabrielle; Kamaly, Nazila; Spolitu, Stefano et al. (2015) Targeted nanoparticles containing the proresolving peptide Ac2-26 protect against advanced atherosclerosis in hypercholesterolemic mice. Sci Transl Med 7:275ra20
Subramanian, Manikandan; Tabas, Ira (2014) Dendritic cells in atherosclerosis. Semin Immunopathol 36:93-102
Subramanian, Manikandan; Hayes, Crystal D; Thome, Joseph J et al. (2014) An AXL/LRP-1/RANBP9 complex mediates DC efferocytosis and antigen cross-presentation in vivo. J Clin Invest 124:1296-308
Libby, Peter; Tabas, Ira; Fredman, Gabrielle et al. (2014) Inflammation and its resolution as determinants of acute coronary syndromes. Circ Res 114:1867-79
Nagareddy, Prabhakara R; Murphy, Andrew J; Stirzaker, Roslynn A et al. (2013) Hyperglycemia promotes myelopoiesis and impairs the resolution of atherosclerosis. Cell Metab 17:695-708
Subramanian, Manikandan; Thorp, Edward; Hansson, Goran K et al. (2013) Treg-mediated suppression of atherosclerosis requires MYD88 signaling in DCs. J Clin Invest 123:179-88
Gautier, Emmanuel L; Westerterp, Marit; Bhagwat, Neha et al. (2013) HDL and Glut1 inhibition reverse a hypermetabolic state in mouse models of myeloproliferative disorders. J Exp Med 210:339-53
Rodríguez, José M; Wolfrum, Susanne; Robblee, Megan et al. (2013) Altered expression of Raet1e, a major histocompatibility complex class 1-like molecule, underlies the atherosclerosis modifier locus Ath11 10b. Circ Res 113:1054-64
Tabas, Ira; Glass, Christopher K (2013) Anti-inflammatory therapy in chronic disease: challenges and opportunities. Science 339:166-72
Rong, James X; Blachford, Courtney; Feig, Jonathan E et al. (2013) ACAT inhibition reduces the progression of preexisting, advanced atherosclerotic mouse lesions without plaque or systemic toxicity. Arterioscler Thromb Vasc Biol 33:4-12

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