Type 2 Diabetes Clinical Trial
Official title:
Simvastatin Reduces Plasma Osteoprotegerin in Type 2 Diabetic Patients With Microalbuminuria
Diabetes is associated with dyslipidaemia leading to generalized atherosclerosis,
cardiovascular disease (CVD) and nephropathy. Osteoprotegerin (OPG), a glycoprotein involved
in bone homeostasis, has been implicated in the pathogenesis leading up vessel
calcification. Furthermore, CVD in diabetics is associated with increased levels of OPG.
Aim: To investigate whether low dose simvastatin treatment (10-20 mg/day) reduces
circulating levels of OPG as well as adhesion molecules (VCAM-1; vascular cell adhesion
molecule-1, ICAM; intercellular cell adhesion molecule).
Type 2 diabetes is associated with an increased risk of macro- and microvascular
complications, resulting from a generalized injury to the vascular endothelium. The
pathophysiological mechanisms leading to cardio vascular disease (CVD) in diabetics are not
well defined. However, there is accumulating evidence, that damage to vascular smooth muscle
cells and endothelial cells partly occur through vessel shear stress, changes in nitric
oxide, and increased cytokine levels (i.e. TNF-α: tumour necrosis factor-α and IL-1:
interleukin-1). This ultimately results in sclerosis of the basal membrane caused by
endothelial cell proliferation and increased vascular permeability, allowing protein to leak
into the extra cellular matrix. Atherosclerotic lesions may also arise as a result of
accumulation of monocytes and macrophages containing oxidised LDL (foam cells) in the
arterial wall. This process is initiated by the expression of adhesion molecules (e.g.
VCAM-1; vascular cell adhesion molecule-1, ICAM; intercellular cell adhesion molecule) on
the luminal surface of vascular endothelial cells, allowing cellular attachment and
migration into the vascular wall.
Osteoprotegerin (OPG), a secreted basic glycoprotein and member of the TNF receptor
superfamily, is a soluble receptor activator of nuclear factor-κB (RANK) ligand (RANKL), and
TNF-related apoptosis inducing ligand (TRAIL), though with much lower affinity to TRAIL
compared to RANKL. OPG works as a decoy-receptor preventing the RANK-RANKL interaction,
thereby reducing the biological effect. The RANK-RANKL system induces osteoclast
differentiation and activation whereby bone absorption is promoted. Due to its properties as
a decoy receptor, OPG antagonizes this effect and inhibits bone loss. In addition to the
effects on osteoclasts, the RANK-RANKL system has been proposed to have cardiovascular
effects. Thus, activation of the RANK-RANKL system induces VCAM-1 synthesis, prolongs
endothelial cell survival, promotes angiogenesis, and reduces TNF-α levels. In contrast,
elevated levels of OPG are associated with the severity of CVD, although it is presently
unclear whether this association reflects a cause-effect relationship or is purely
coincidental.
Cholesterol-lowering therapy with statins reduces cardiovascular mortality and morbidity
risk in diabetics and non-diabetic subjects. According to recent studies, statins may have
additional, pleiotropic effects and may in fact stabilize atherosclerotic plaques.
Experimental data obtained in animal models indicate dose-dependent angiogenetic effects and
promotion of vascular structure formation. It is therefore of interest that recent, in vitro
studies by Ben-Tahl et al. and Rasmussen et al. suggest that statins may suppress OPG and
adhesion molecule production in humans. Thus, umbilical vein endothelial cells and smooth
vascular muscle cells incubated with simvastatin and stimulated with TNF-α and IL-1 secreted
less OPG than control cells. Under normal circumstances, exposure to cytokines (TNF-α and
IL-1) is a powerful stimulus to OPG production in vascular cells and these results therefore
seem to support the concept, that simvastatin may ameliorate some of the deleterious effects
of inflammation.
This study was conducted to examine the effect of simvastatin treatment on circulating OPG
and adhesion molecule levels in a group of type 2 diabetic patients at increased risk for
cardiovascular disease (CVD) due to persistent microalbuminuria. Since both OPG and adhesion
molecules are associated with CVD and potentially modifiable by statin treatment this could
help improve our understanding of potentially pleiotropic effects of statins in reducing
CVD.
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Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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