Metabolic Syndrome Clinical Trial
Official title:
The Effects of Ezetimibe on Postprandial Hyperlipidemia and Endothelial Dysfunction in Patients With the Metabolic Syndrome.
In the present study the investigators are researching the effects of the cholesterol absorption inhibitor ezetimibe on postprandial lipemia and postprandial endothelial function in patients with the metabolic syndrome. The lipid-lowering effect of high-dose statin monotherapy on fasting lipids is equal to the combination therapy of low-dose statin and ezetimibe.
In patients at high risk for future cardiovascular events, more intensive LDL cholesterol
lowering with high doses statin therapy provides greater protection against death or major
cardiovascular events than does a standard regimen. Intensive LDL cholesterol lowering can
be achieved by high dose statin treatment or with combination therapy of lower doses statin
and ezetimibe. However, it is unclear whether this combination therapy results in the same
or more beneficial effects on cardiovascular prognosis.
The metabolic syndrome is a cluster of several vascular risk factors (as abdominal obesity,
high blood pressure, hypertriglyceridemia, low HDL cholesterol and high fasting glucose).
The underlying pathophysiology is still not fully clarified, but insulin resistance seems to
be a main characteristic of this syndrome. Subjects with the metabolic syndrome are at
increased risk for the development of cardiovascular morbidity and mortality and type II
diabetes. The prevalence of the metabolic syndrome is high in patients with clinical
manifestations of vascular diseases and is associated with more vascular damage in these
patients.
Insulin resistance is linked to endothelial dysfunction and decreased nitric oxide
bioavailability by several mechanisms including, inflammation (as reflected by elevated high
sensitive C Reactive Protein (hs-CRP) plasma levels), disruption of insulin receptor
signalling cascades, increased production of cytokines and activation of the renin
angiotensin system. However, other studies do not support an association between insulin
resistance and endothelial function, so this mechanism seems controversial.
In the postprandial state, insulin resistance is associated with hyperlipidemia.
Postprandial hyperlipidemia may be an important determinant of endothelial dysfunction as
well. Remnants of chylomicron and very low density lipoprotein metabolism impair endothelial
dependent vasodilatation. In line with the hypothesis that endothelial function can be used
as a surrogate endpoint for cardiovascular morbidity, therapeutic modulation of
(postprandial) endothelial function may potentially contribute to prevention of
cardiovascular disease in patients with the metabolic syndrome.
Statin therapy modulates (postprandial) endothelial function but it is not known whether
this is an indirect effect of lipid-lowering or a direct vascular effect of statins
influencing the stability and bioavailability of NOS.
AIMS In the present study we propose to investigate the effects of the cholesterol
absorption inhibitor ezetimibe on postprandial lipemia and (postprandial) endothelial
function in patients with the metabolic syndrome. High-dose statin monotherapy has the same
lipid-lowering effect (on fasting lipids) as the combination therapy of low dose statin and
ezetimibe. The latter may reduce postprandial lipemia more effectively and may therefore
have beneficial effects on postprandial endothelial dysfunction.
Ezetimibe is unlikely to have a direct vascular effect and therefore any observed change in
vascular function is due to a change in postprandial lipemia. As secondary objective of the
study, this enables us to differentiate between direct and indirect effects of statin
therapy on postprandial endothelial function comparing modulation of postprandial
endothelial function by monotherapy simvastatin with combination therapy of simvastatin and
ezetimibe.
Hypothesis With comparable reduction in fasting plasma lipids, combination therapy of
low-dose statin and ezetimibe reduces postprandial lipemia better than high-dose statin
monotherapy. This leads to better postprandial endothelial function in patients with the
metabolic syndrome.
Objectives
1. To determine the effects of combination therapy of low-dose statin and ezetimibe on
postprandial hyperlipidemia compared to high-dose statin monotherapy.
2. To determine the effects of combination therapy of low-dose statin and ezetimibe on
postprandial endothelial (dys-)function compared to high-dose statin monotherapy.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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