Coronary Heart Disease Clinical Trial
Official title:
Effect of Rosuvastatin Therapy on HDL2 Level and Antiatherosclerotic Reverse Cholesterol Transport Process in Chinses CAD Patients With Hyperlipidemia
In many large trials, reducing low density lipoprotein (LDL) levels with rosuvastatin
decreased the incidence of major cardiovascular events,but little attention to the effects
of rosuvastatin on HDL level,especially on HDL subtype.
Epidemiological evidence strongly favors the notion that the risk of cardiovascular disease
(CVD) is inversely related to the plasma high-density lipoprotein (HDL) cholesterol
concentration.
HDL can be subdivided into large-sized (HDL2a, HDL2b) and small-sized subclasses (preb1-HDL,
HDL3c, HDL3b, HDL3a) and preb2-HDL. Some studies indicate that only large HDL2a and HDL2b
particles make HDLs possess anti-atherogenic functions.
The investigators assume that rosuvastatin could play the role of anti-atherosclerosis
though the levels of HDL2a、HDL2b increased.
Elevated LDL-C and lowered HDL-C are important risk factors for cardiovascular disease.
Raising HDL-C is an attractive approach for reducing the residual risk of cardiovascular
events that persist in many patients receiving low-density LDL-C -lowering therapy with
statins. From previous studies, it is concluded that compared to atorvastatin, rosuvastatin
could significantly increase HDL-C levels from baseline. However, which benefits the
elevated HDL-C will bring to these patients who receive statin lowing LDL-C therapy are
still unknown. Despite strong evidence that HDL-C levels predict atherosclerotic events,
attempts at using an HDL-based treatment strategy as a therapeutic target have not yet been
successful at the present time. However, on the basis of an enormous amount of basic
scientific and clinical investigation, the International Atherosclerosis Society and US
National Lipid Association still believe that there are a considerable number of reasons
supporting the need to continue to investigate the therapeutic effect of modulating HDL
structure and function.
It has long been known that a low level of HDL cholesterol is a powerful independent
predictor of increased cardiovascular risk, even among patients with LDL cholesterol levels
below 70 mg/dl. In fact, a 1 mg/dl (0.026 mM) increment in HDL-C levels was associated with
a significant decrease in the risk of coronary heart disease (CAD) of 2% in men and 3% in
women. HDL-C has been proposed to have several anti-atherosclerotic properties, including
the ability to mediate reverse cholesterol transport (RCT), antioxidant capacity,
anti-inflammatory properties, nitric oxide-promoting activity, and an ability to transport
proteins with their own intrinsic biological activities. RCT describes the metabolism and an
important antiatherogenic function of HDL, namely, the HDL-mediated efflux of cholesterol
from cells of the arterial wall and its subsequent delivery to the liver and steroidogenic
organs, thus preventing atherosclerosis. HDL particles are responsible for RCT, as critical
acceptors of cholesterol from lipid-laden macrophages and thereby play an important role in
the maintenance of net cholesterol balance in the arterial wall and in the reduction of
pro-inflammatory responses by lipid-rich macrophages. The antiatherogenic properties of HDL
have been primarily ascribed to RCT. Khera et al. recently reported that HDL efflux capacity
was inversely and significantly correlated with carotid intima-media thickness (CIMT). A
one-standard deviation increase in HDL efflux capacity predicted a 30% reduction in the odds
for CAD. Although cholesterol efflux from macrophages represents only a small portion of
total RCT, the cholesterol efflux from macrophage foam cells is probably the most relevant
step with respect to preventing or reversing atherosclerosis. HDL can be separated into two
major parts, i.e., pre β-(further distinguished into preβ1-, preβ2-,preβ3-HDL) and
a-HDL(separated into 5 distinct subclasses HDL3c 3b 3a 2a 2b). It has been postulated that
RCT indeed was the metabolic process that nascent preβ-HDL converted to mature a-HDL,
following the route of preβ1-HDL→preβ2-HDL→preβ3-HDL→HDL3→HDL2[13].
The effect of HDL-C on plaque formation is complex, since HDL particles are highly
heterogeneous, and exist as a spectrum of small, intermediate and large particles that
differ in lipid and protein content. So the increase in plasma HDL-C does not necessarily
reflect an increase in reverse cholesterol transport (RCT). Former studies from cholesteryl
ester transfer protein(CETP) modulators and inhibitors such as dalcetrapib have limited
efficacy to be still on the way may attributed to their concentration only on raising total
HDL-C level and undesirable side effects. Results obtained in some studies, have shown that
HDL quality (HDL subpopulations), rather than quantity (total HDL concentration), should be
the target of future pharmacological therapies. A number of investigations have reported
that, with the increase of plasma LDL-C or the decrease of plasma HDL-C concentrations or
elevated TC(total cholesterol), or in some CAD patients with hyperlipidemia, or patients of
CAD with diabetes, there was a general shift toward smaller-sized HDL (HDL3), which, in
turn, indicates that reverse cholesterol transport might be weakened and HDL maturation
might be abnormal. Significantly lower larger-sized HDL-HDL2 in CAD patients with
hyperlipidemia compared with control patients, and this inverse relationship between HDL-C,
HDL2, and CAD is particularly strong in men with type 2 diabetes mellitus. In type 2
diabetes patients, the difference between HDL2 in the myocardial infarction (MI) and non-MI
group persists after adjustment for physical activity, alcohol intake, obesity, duration of
diabetes, and glycemic control. Moreover, HDL2 deficiency has also been demonstrated to be a
primary alteration in myocardial infarction patients even without other significant risk
factors. The tendency that small-sized HDL3b, and HDL3a levels were significantly higher,
and the large-sized HDL2a and HDL2b levels were significantly lower were also detected in
ACS(acute coronary syndrome) patients. From articles on Chinese patients with elevate TC or
LDL-C/HDL-C ratio, there was also a general shift toward smaller-sized HDL particles, which
implied that the maturation process of HDL was blocked. Overall, accumulate evidences have
demonstrated that in patients with CAD/CAD comorbid with diabetes/elevated TC levels, HDL
maturation was hampered in the stage of the transformation of small-sized HDL3 to larger
sized HDL2. HDL2 levels have inverse associations with the risk of acute myocardial
infarction and thus to be protective factors in ischemic heart disease. It has also
demonstrated that patients with high HDL2 level were better protected from atherosclerosis.
It has been demonstrate that atorvastatin 20 mg/d treatment for 8 weeks could result in a
favorable modification of HDL subfraction phenotype. Treated with atorvastatin 20mg/d
significantly increased the cholesterol concentration of large HDL particles and decreased
the cholesterol concentration of small HDL particles although without changes of serum HDL-C
level in patients with atherosclerosis. However, there are still lack of evidence on the
effect of rosuvastatin treatment for HDL maturation(for the step of transformation of HDL3
to HDL2)and RCT process in CAD and Chinese patients. It has been demonstrated that Low HDL
cholesterol is frequently associated with low HDL2b and high HDL cholesterol frequently
associated with high HDL2b. As the investigators discussed above, compared to atorvastatin,
rosuvastatin could significantly decrease LDL-C level and increase HDL-C level from
baseline. So besides the basic effect of lowing LDL-C, it has a strong possibility that
rosuvastatin therapy on CAD patients with hyperlipidemia could reverse the aberrant HDL
maturation process via elevating lager HDL2 level, and then restore the RCT process to the
normal to prevent atherosclerosis.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Subject), Primary Purpose: Prevention
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