Cardiovascular Diseases Clinical Trial
To assess the influence of HDL-subclasses with coronary disease progression, and to identify factors influencing HDL subclasses at baseline and over time.
BACKGROUND:
The Stanford Coronary Risk Intervention Project was a four-year randomized clinical trial
that showed that risk reduction through lifestyle change and lipid-lowering medications
significantly reduced the rate of narrowing of the minimum diameter of coronary artery
segments with angiographically visible lesions in 119 patients versus 127 controls who
received usual physician care. In collaboration with this trial, Dr. Ronald Krauss measured
high-density lipoprotein (HDL) subclasses by gradient gel electrophoresis. HDL may be
divided into two HDL2 and three HDL3 subclasses that are approximated by their estimated
particle diameters: HDL3c (7.2-7.8 nm), HDL3b (7.8-8.2 nm), HDL3a (8.2- 8.8 nm), HDL2a
(8.8-9.7 nm) and HDL2b (9.7-12.9 nm). The HDL- distribution can also be characterized by the
diameter of the predominant peak, which may lie in either the HDL3b or HDL3a interval. Case
control and angiographic studies suggest that coronary heart disease risk is increased when
HDL2b is reduced relative to HDL3c and HDL3b. See also Study 27.
DESIGN NARRATIVE:
Using data from the Stanford Coronary Risk Intervention Project (SCRIP), the following
specific questions were examined : 1. Did the risk reduction program change specific HDtL
subclasses as compared to controls? 2. Did the HDL gradient gel profile characterize men
most likely to benefit from multifactor risk reduction? 3. Did HDL-subclasses change
significantly in patients that reduced fat intake, reduced body weight, or who took one or
more of the following medications: colestipol, nicotinic acid, clofibrate, probucol,
gemfibrozil, fenofibrate, lovastatin, guar gum or fish oils? 4. What were the
cross-sectional associations of HDL-subclasses with adiposity, fasting and post-load insulin
and glucose, diet and medications at baseline? Preliminary analyses suggested that: 1)
During the trial, men in the treatment group increased HDL2b; 2) the special intervention
was most effective in reducing coronary disease progression in subjects with a baseline
predominant HDL-peak diameter below the median; 3) HDL- subclasses were more strongly
influenced by diet and adiposity than by drugs during the trial; 4) carbohydrates, alcohol
and caffeine were associated with specific subclasses at baseline.
The study completion date listed in this record was obtained from the "End Date" entered in
the Protocol Registration and Results System (PRS) record.
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