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Abstract

Grant Number: 1R21AT003488-01A1

Project Title: Inhibition of Cholesterol Synthesis by Policosanol

PI Information: Name Email Title

PORTER, TODD D. tporter@email.uky.edu

Abstract: DESCRIPTION (provided by applicant): Over-the-counter botanicals and nutritional supplements have gained great popularity among the public as safe and effective means to treat chronic and acute diseases, and are widely viewed as safe alternatives to prescription medicines. Hypercholesterolemia is a widespread problem for which there is great interest in alternative medicines, and policosanol is a relatively new product derived from sugar cane that has gained considerable attention as a means to reduce blood cholesterol levels. This research will investigate a possible mechanism by which policosanol decreases blood cholesterol levels. Most current evidence indicates that this mixture of long-chain alcohols inhibits or suppresses HMG-CoA reductase activity, the regulatory step in cholesterol synthesis. To test this hypothesis, the effect of policosanol on HMG-CoA reductase activity will be evaluated in cultured hepatoma cells and in whole animals, and the mechanism by which policosanol inhibits this enzyme will be determined. Preliminary studies demonstrate that policosanol does not directly inhibit HMG-CoA reductase, indicating that intracellular activation/metabolism of policosanol, or the activation of a modulatory pathway, is necessary for the suppression of this key cholesterolgenic enzyme. Studies will test the hypothesis that peroxisomal metabolism of policosanol results in the activation of AMP-kinase, which then inactivates HMG-CoA reductase by phosphorylation. An alternative hypothesis, that policosanol is metabolized to a direct inhibitor of HMG-CoA reductase, will also be tested. HMG-CoA reductase expression and activity and AMP-kinase activity will be measured in hepatoma cells and in preparations from the livers of animals treated with policosanol. Finally, to determine if peroxisomal oxidation of policosanol is necessary, the ability of policosanol to inhibit cholesterol synthesis in mice that lack peroxisomal oxidation pathways will be determined. These studies should establish a solid, mechanistic understanding of how policosanol decreases cholesterol synthesis and lowers blood cholesterol levels, and may provide a basis for predicting how the use of this compound might interact, either favorably or unfavorably, with prescription Pharmaceuticals used for the treatment of hypercholesterolemia.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
HMG coA reductase, cholesterol
HTC cell, RNA interference, alcohol, alternative medicine, attention, blood, cell, conflict, culture, enzyme, fatty acid, hypercholesterolemia, intracellular, liver, medicine, metabolism, motivation, oxidation, phosphorylation, sterol, suppression, water

Institution: UNIVERSITY OF KENTUCKY

109 KINKEAD HALL

LEXINGTON, KY 405060057

Fiscal Year: 2007

Department: PHARMACEUTICAL SCIENCES

Project Start: 01-MAY-2007

Project End: 30-APR-2009

ICD: NATIONAL CENTER FOR COMPLEMENTARY & ALTERNATIVE MEDICINE

IRG: ZAT1

Grant Number:	1R21AT003488-01A1
Project Title:	Inhibition of Cholesterol Synthesis by Policosanol

PI Information:	Name	Email	Title
	PORTER, TODD D.	tporter@email.uky.edu

Institution:	UNIVERSITY OF KENTUCKY
	109 KINKEAD HALL
	LEXINGTON, KY 405060057
Fiscal Year:	2007
Department:	PHARMACEUTICAL SCIENCES
Project Start:	01-MAY-2007
Project End:	30-APR-2009
ICD:	NATIONAL CENTER FOR COMPLEMENTARY & ALTERNATIVE MEDICINE
IRG:	ZAT1