Abstract

Niacin (nicotinic acid) is one of the most effective hypolipidemic agents available. However, its use is greatly limited by side effects, the most prominent of which is intense flushing. We recently demonstrated that niacin induced vasodilation is mediated by a release of prostaglandin (PG) D2. An intriguing discovery was made that pretreatment with a very low dose of aspirin (40 mg) essentially totally inhibits niacin-induced release of PGD2 in vivo. We have obtained a considerable body of preliminary evidence that suggests strongly that tissue macrophages are the cellular source of niacin-induced release of PGD2 in vivo and that PG production by macrophages can be inhibited by very low doses of aspirin. Studies are now proposed to establish more definitively the cells that are activated by niacin in vivo. In particular, resident tissue macrophages isolated from various tissues of guinea pigs and humans will be studied. Experiments will then focus on identifying potential cellular mechanisms involved in niacin induced activation of arachidonic acid metabolism. Studies will then be carried out to determine the molecular basis for the unusual sensitivity of PG production in niacin responsive cells to inhibition by aspirin. Specifically we will address whether this enhanced sensitivity is related to (a) the cyclooxygenase(s) present in these cells, (b) the mechanism by which aspirin inhibits PG biosynthesis, or (c) the intracellular metabolic rate of aspirin. Finally, the effect of treatment of normal volunteers with pharmacologic doses of prednisone on niacin-induced release of eicosanoids in vivo will be determined. The finding that very low doses of aspirin can inhibit niacin-induced release of PGD2 in humans has important therapeutic implications for the use of niacin as a hypolipidemic agent. Further, these studies should provide valuable insights into cell-specific mechanisms involved in activation of arachidonic acid metabolism and factors that can influence the ability of certain pharmacologic agents to inhibit PG biosynthesis in specific cell types.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Specialized Center (P50)
Project #
2P50GM015431-26
Application #
3778183
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
26
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Salisbury-Ruf, Christi T; Bertram, Clinton C; Vergeade, Aurelia et al. (2018) Bid maintains mitochondrial cristae structure and function and protects against cardiac disease in an integrative genomics study. Elife 7:
Kong, Deping; Li, Juanjuan; Shen, Yujun et al. (2017) Niacin Promotes Cardiac Healing after Myocardial Infarction through Activation of the Myeloid Prostaglandin D2 Receptor Subtype 1. J Pharmacol Exp Ther 360:435-444
Teder, Tarvi; Boeglin, William E; Brash, Alan R (2017) Oxidation of C18 Hydroxy-Polyunsaturated Fatty Acids to Epoxide or Ketone by Catalase-Related Hemoproteins Activated with Iodosylbenzene. Lipids 52:587-597
Plewes, Katherine; Kingston, Hugh W F; Ghose, Aniruddha et al. (2017) Cell-free hemoglobin mediated oxidative stress is associated with acute kidney injury and renal replacement therapy in severe falciparum malaria: an observational study. BMC Infect Dis 17:313
Kudalkar, Shalley N; Kingsley, Philip J; Marnett, Lawrence J (2016) Assay of Endocannabinoid Oxidation by Cyclooxygenase-2. Methods Mol Biol 1412:205-15
Wu, Jing; Montaniel, Kim Ramil C; Saleh, Mohamed A et al. (2016) Origin of Matrix-Producing Cells That Contribute to Aortic Fibrosis in Hypertension. Hypertension 67:461-8
Wu, Jing; Saleh, Mohamed A; Kirabo, Annet et al. (2016) Immune activation caused by vascular oxidation promotes fibrosis and hypertension. J Clin Invest 126:50-67
Mashhadi, Zahra; Newcomer, Marcia E; Brash, Alan R (2016) The Thr-His Connection on the Distal Heme of Catalase-Related Hemoproteins: A Hallmark of Reaction with Fatty Acid Hydroperoxides. Chembiochem 17:2000-2006
Kong, Deping; Shen, Yujun; Liu, Guizhu et al. (2016) PKA regulatory II? subunit is essential for PGD2-mediated resolution of inflammation. J Exp Med 213:2209-26
Boutaud, Olivier; Sosa, I Romina; Amin, Taneem et al. (2016) Inhibition of the Biosynthesis of Prostaglandin E2 By Low-Dose Aspirin: Implications for Adenocarcinoma Metastasis. Cancer Prev Res (Phila) 9:855-865

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