Hypertension Clinical Trial
To determine if the combined incidence of nonfatal myocardial infarction and coronary heart disease death differs between diuretic-based and each of three alternative antihypertensive pharmacological treatments. Also, to determine, in a subset of this population, if lowering serum cholesterol with a HMG CoA reductase inhibitor in older adults reduces all-cause mortality compared to a control group receiving usual care. Conducted in conjunction with the Department of Veterans' Affairs.
BACKGROUND:
An estimated 58 million people in the United States have elevated blood pressure (systolic
blood pressure (SBP) of 140 mmHg or greater and/or diastolic blood pressure (DBP) of 90 mmHg
or greater on initial examination) or are taking antihypertensive medication. Perhaps
one-half to two-thirds of these have sustained hypertension.
Despite the known etiologic relationship of hypertension to coronary heart disease,
large-scale randomized clinical trials in mild to moderate hypertension have failed to
demonstrate conclusively that antihypertensive drug treatment, largely based on
thiazide-like diuretics, reduces the occurrence of coronary heart disease death or non-fatal
myocardial infarction. The pooled results of nine such trials, using primarily thiazide-like
diuretics and involving over 43,000 subjects, suggest a 9 percent benefit, with 95 percent
confidence limits consistent with a 19 percent benefit or 1 percent adverse outcome. This
observed treatment effect compares with a maximum predicted effect on coronary heart disease
of approximately 23 percent for an equivalent blood pressure difference, as derived from
epidemiologic data. In contrast, the observed beneficial effect on stroke in these trials,
36 percent, is almost exactly that which would be predicted from epidemiologic data. A more
recent overview of 14 trials in participants with all levels of hypertension estimated a
somewhat larger benefit of 14 percent. While this may be an over-estimate of benefit, these
overviews do not include the strongly positive results of the Systolic Hypertension in the
Elderly Program (SHEP), in which diuretic-based treatment reduced stroke incidence by 36
percent and major coronary heart disease events by 27 percent.
In the early 1980s, two new classes of antihypertensive agents, the calcium antagonists and
ACE inhibitors, were developed and licensed for use in chronic antihypertensive therapy.
These agents cost more than older agents such as diuretics and beta-blockers, and evidence
was limited that might justify their use despite the increased cost. The 1988 Joint National
Committee on Detection, Evaluation, and Treatment of High Blood Pressure recommended
beta-blockers, calcium antagonists, ACE-inhibitors, and diuretics as equally acceptable
first-line therapy. All four classes of drugs have been found to control diastolic blood
pressure as single agents in 50 percent or more of patients with mild hypertension.
Of these drug classes, only beta-blockers have been compared directly to diuretics in
large-scale, long-term clinical trials in hypertension. Three such trials completed in
Europe in 1985-1986 showed approximate equivalence of effects on morbidity and mortality in
diuretic- and beta-blocker-based regimens. Pooled analysis of these trials yields a 6
percent lower coronary heart disease mortality from beta-blockers. These data are in
contrast to the recent Medical Research Council (MRC) Trial in the Elderly, in which
patients treated with a thiazide diuretic had significantly lower rates of coronary heart
disease compared to beta-blocker treatment or placebo, both by about 45 percent.
Circulating levels of cholesterol, specifically cholesterol associated with the low-density
lipoprotein (LDL) fraction, have been established as a major etiologic factor in coronary
heart disease in observational epidemiologic studies, in metabolic, pathologic, and genetic
studies in humans and selected animal models, and in randomized clinical trials. The
clinical trials that have demonstrated a reduction in coronary heart disease incidence from
lowering LDL-cholesterol levels have been conducted primarily in middle-aged men with
hypercholesterolemia or established coronary heart disease. Experimental evidence for the
efficacy of cholesterol lowering in older men is confined to the analysis of small subgroups
of clinical trials and is lacking for women of any age. The paucity of clinical trial data
led the National Cholesterol Education Program's Expert Panel on Detection, Evaluation, and
Treatment of High Blood Cholesterol in Adults in their 1987 Guidelines to allow for
considerable physician judgement regarding the elderly.
DESIGN NARRATIVE:
Patients were recruited through office-based practices and hypertension clinics which were
reimbursed by the Clinical Trials Center on a per-patient basis. Six hundred patients were
entered into the vanguard or feasibility phase and a total of 42,448 were entered into the
full-scale trial. The primary hypothesis of the antihypertensive trial was that the combined
incidence of fatal coronary heart disease and nonfatal myocardial infarction would be lower
in hypertensive patients randomized to amlodipine (a calcium antagonist), lisinopril (an
angiotensin-converting enzyme (ACE) inhibitor), or doxazosin (an alpha adrenergic blocker)
as compared to those randomized to chlorthalidone (a thiazide-like diuretic). Secondary
endpoints were total cardiovascular mortality, major morbidity, all-cause mortality, and
health-related quality of life.
The primary hypothesis of the cholesterol-lowering trial was that mortality from all causes
would be lower in the subset of hypertensive patients with LDL cholesterol levels between
120 and 189 mg/dl (between 100 and 159 mg/dl for those with known coronary heart disease)
who were randomized to receive pravastatin (a HMG CoA reductase inhibitor) plus the National
Cholesterol Education Program Step I cholesterol-lowering diet than those randomized to
receive usual care plus diet. Secondary endpoints were the combined incidence of nonfatal
myocardial infarction and coronary heart disease death, major non-cardiovascular heart
disease morbidity and mortality, and health-related quality of life.
Recruitment for the feasibility phase began in February 1994. The clinical phase of the
feasibility study ended in September 1994. Recruitment for the full-scale trial began in
October 1994 and ended in January, 1998. The mean follow-up was 4.9 years. There were over
600 clinics in 47 states, Puerto Rico, Virgin Islands and Canada.
;
Allocation: Randomized, Primary Purpose: Prevention
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