Hypercholesterolemia Clinical Trial
Official title:
A Stable-isotope Study in Healthy Normolipidemic Volunteers Comparing the Mechanisms of Action of Lifibrol and Pravastatin
Lifibrol is a new lipid-lowering drug which lowers cholesterol to an extent in the order of magnitude of the statins. The mechanism of action of this compound is different from the one of statins but remains unknown. The current study will investigate the mechanism of action using stable-isotope turnover methods. The study will be done in healthy male volunteers.
Elevated lipoprotein concentrations are a major risk factor for the development of
atherosclerotic cardiovascular disease. Effective reduction of low density lipoprotein
(LDL)-cholesterol concentrations has been shown to greatly reduce this risk. The most widely
used lipid-lowering agents are the 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase
inhibitors (statins), which have been shown to reduce morbidity and mortality from coronary
heart disease (CHD) in large prospective clinical trials. However, despite significant LDL-C
reduction approximately 70% of the events are still not avoided and the search for improved
or alternative lipid-modifying drug therapies continuous. HDL-C has been addressed as a
potential modifiable target for decreasing this residual risk, since a low HDL-C
concentration is an acknowledged independent risk factor for CHD. However, recent studies
showed that an increase in HDL-C concentrations was surprisingly not associated with a
decrease in atherosclerosis, but with a possible increase. Therefore it seems that not the
concentrations of HDL-C should be targeted but HDL function in reverse cholesterol
transport.
Lifibrol is a lipid-modifying drug which has been shown to improve HDL particle flux via
increased apoA-I production, while not having HDL-raising properties. Furthermore, it
decreases dose-dependently LDL-C by up to 40%. It is of major interest to clarify the,
apparently unique, mechanisms of action of a compound, whose LDL-lowering effects are
comparable in magnitude to the ones of statins.
The mechanisms of lifibrol's LDL-lowering effects are not completely clarified. There is
evidence suggesting that it increases hepatic LDL receptor expression by a
sterol-independent mechanism, i.e. not through a reduction in cholesterol synthesis, the
mechanism of action of statins. ApoB turnover studies have indicated that increased
catabolism of LDL rather than a decrease in hepatic apoB production may be responsible for
its cholesterol-lowering effects. Since apoB metabolism and cholesterol synthesis are
closely related, we designed a study to investigate the effects of lifibrol on the
metabolism of apoB-100-containing lipoproteins and on endogenous sterol synthesis in
parallel, using stable isotope methods. In addition, since lifibrol may inhibit cholesterol
synthesis at steps earlier than HMG-CoA reductase, we investigated [13C]acetate catabolism
analyzing 13CO2 appearance in breath. The HMG-CoA-reductase inhibitor pravastatin was used
as comparator, since its mode of action is well characterized. The principle questions
addressed were (i) whether lifibrol exerts its cholesterol-lowering effects through
decreased synthesis/enhanced catabolism of apoB-100-containing lipoproteins or through
inhibition of sterol de novo synthesis and (ii) whether these effects are interrelated.
;
Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Basic Science
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