Abstract

: There is a large body of evidence suggesting that oxidative modifications of low-density lipoproteins (LDL) contribute significantly to the initiation and/or progression of atherosclerosis. Although numerous studies of the oxidation of LDL lipids have been published, far less is known about the oxidative modification of the apoprotein. The greater chemical diversity of the apoprotein than of the LDL lipids offers the opportunity for greater biomarker specificity for distinguishing contributions of specific mechanisms of oxidation. The first Specific Aim of the present proposal is to test the hypothesis that oxidations of LDL in vitro by methods that are candidate mechanisms for oxidation of LDL in vivo produce modifications of the apoprotein (apo B-100) that are sufficiently distinguishable to be empIoyed as biomarkers for oxidation of LDL in vivo by the respective mechanisms. In our studies to date we have observed clear differences in products of apoB-1 00 oxidation formed in oxidation of LDL in vitro by Cu2+, HOCl, and myeloperoxidase (MPO). We propose to investigate similarly the oxidation of LDL in vitro by Fe2+-catalyzed oxidation, nitration (NO and ONOOdonors, MPO or eosinophil peroxidase aboutPO] plus NO2-), and oxidation mediated by cultured cells, including endothelial cells, vascular smooth muscle cells and monocytes. These studies will employ isolation methods based on high performance liquid chromatography (HPLC) and structural characterization methods based on mass spectrometry. The second Specific Aim of this proposal is to test the hypothesis that subfractions of circulating LDL isolated from some individuals will exhibit specific modifications apoB-1 00 oxidation that will reflect a limited subset of the products of oxidation of LDL in vitro characterized in Specific Aim 1. The third Specific Aim of this proposal is to test the hypothesis that LDL isolated from atheromatous material will exhibit a limited subset of the products of apoprotein oxidation that were characterized in Specific Aim i. Our results to date provide very strong support for the working hypotheses upon which we base this application. The goal of the studies proposed is to develop a means of distinguishing the specific mechanisms of LDL oxidation that are suspected to contribute to the oxidation of LDL in vivo and to atherogenesis. The longer-term goals of this research are to create the basis for more mechanistically specific therapeutic efforts to retard the initiation and progression of atherosclerosis and to develop biomarkers of these distinct mechanisms of oxidation to monitor efficacies of these therapeutic interventions. Finally, the studies we propose are not limited in relevance to atherosclerosis or even to oxidation of LDL, but the concepts and methods developed in these studies are readily applicable to a wide range of important human diseases for which unspecified oxidative processes are proposed to contribute.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL063364-02
Application #
6527210
Study Section
Pathology A Study Section (PTHA)
Program Officer
Applebaum-Bowden, Deborah
Project Start
2001-09-10
Project End
2005-08-31
Budget Start
2002-09-01
Budget End
2003-08-31
Support Year
2
Fiscal Year
2002
Total Cost
$288,375
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Biochemistry
Type
Schools of Medicine
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Stancel, Nicole; Chen, Chih-Chieh; Ke, Liang-Yin et al. (2016) Interplay between CRP, Atherogenic LDL, and LOX-1 and Its Potential Role in the Pathogenesis of Atherosclerosis. Clin Chem 62:320-7
Chu, Chih-Sheng; Ke, Liang-Yin; Chan, Hua-Chen et al. (2016) Four Statin Benefit Groups Defined by The 2013 ACC/AHA New Cholesterol Guideline are Characterized by Increased Plasma Level of Electronegative Low-Density Lipoprotein. Acta Cardiol Sin 32:667-675
Ke, Liang-Yin; Chan, Hua-Chen; Chen, Chih-Chieh et al. (2016) Enhanced Sphingomyelinase Activity Contributes to the Apoptotic Capacity of Electronegative Low-Density Lipoprotein. J Med Chem 59:1032-40
Chang, Chiz-Tzung; Wang, Guei-Jane; Kuo, Chin-Chi et al. (2016) Electronegative Low-density Lipoprotein Increases Coronary Artery Disease Risk in Uremia Patients on Maintenance Hemodialysis. Medicine (Baltimore) 95:e2265
Shen, Ming-Yi; Chen, Fang-Yu; Hsu, Jing-Fang et al. (2016) Plasma L5 levels are elevated in ischemic stroke patients and enhance platelet aggregation. Blood 127:1336-45
Chen, Wei-Yu; Chen, Fang-Yu; Lee, An-Sheng et al. (2015) Sesamol reduces the atherogenicity of electronegative L5 LDL in vivo and in vitro. J Nat Prod 78:225-33
Chang, Kuan-Cheng; Lee, An-Sheng; Chen, Wei-Yu et al. (2015) Increased LDL electronegativity in chronic kidney disease disrupts calcium homeostasis resulting in cardiac dysfunction. J Mol Cell Cardiol 84:36-44
Hsu, Jing-Fang; Chou, Tzu-Chieh; Lu, Jonathan et al. (2014) Low-density lipoprotein electronegativity is a novel cardiometabolic risk factor. PLoS One 9:e107340
Lee, An-Sheng; Chen, Wei-Yu; Chan, Hua-Chen et al. (2014) Gender disparity in LDL-induced cardiovascular damage and the protective role of estrogens against electronegative LDL. Cardiovasc Diabetol 13:64
Ke, Liang-Yin; Stancel, Nicole; Bair, Henry et al. (2014) The underlying chemistry of electronegative LDL's atherogenicity. Curr Atheroscler Rep 16:428

Showing the most recent 10 out of 30 publications