HOPE trial
Last reviewed 02/2023
Original HOPE study (1):
- designed to investigate the effects of taking an ACE inhibitor ramipril and/or vitamin E for at least 4 years, on a wide range of vascular endpoints
- total of 9541 patients (men and women) older than 55 years took part in study
- patients were included if they were at high risk of cardiovascular events due to history of diabetes, previous ischaemic heart disease, peripheral vascular disease or stroke
- treatment benefits of ramipril were seen across all patient groups - these benefits occurred within 3 to 4 months of starting treatment with ramipril
- results revealed that the combined reduction in myocardial infarction, cardiovascular death and stroke at 5 years was 22 % in the ramipril treatment group; there was a 17% reduction in all cause mortality in the ramipril treatment group; no effect on stated endpoints occurred with patients treated with vitamin E
- the study investigators do not attribute treatment benefits accrued with ramipril to be because of an impact on blood pressure - the baseline blood pressure had a mean level of 139/79 mmHg - by the end of the trial there had only been a small further decline
HOPE follow-up study (2):
- a follow-up study based on the HOPE study population has been undertaken
- 4,528 patients agreed to further follow-up (median follow-up period
2.6 years)
- rates of use of angiotensin-converting-enzyme inhibitors (ACEIs) in the 2 groups (72% ramipril versus 68% placebo) were similar after the end of the trial
- during the post-trial follow-up, patients allocated to ramipril
had a 19% further lower relative risk (RR) of myocardial infarction
(MI), a 16% lower RR of revascularization, and a 34% lower RR of a
new diagnosis of diabetes
- RR reductions in vascular events were observed during and after the active phase of the trial, regardless of baseline risk (RR of 0.76, 0.89, and 0.83 for low-, medium-, and high-risk patients, respectively) or ancillary treatments (RR of 0.90 for aspirin, 0.76 for beta-blockers, and 0.84 for lipid-lowering medication)
- the study authors noted that the benefits of ramipril observed during
the active period of the HOPE trial were maintained during post-trial
follow-up for cardiovascular death, stroke, and hospitalisation for heart
failure
- additional reductions in MI, revascularization, and the development of diabetes were observed during the follow-up phase despite similar rates ACEI use in the 2 randomized groups
- benefits associated with ACEI use were consistent regardless of patient risk or ancillary treatments
- the benefits observed in the study extension data indicate that the 4.5 years of initial, "earlier" use of ramipril therapy provided a longer-term protective effect compared with later initiation
- during the follow-up period, there was not observed an additional
treatment effect for stroke
- blood pressure was similar during the post-trial follow-up and suggests that an important mechanism by which strokes may have been reduced during the blinded part of the study (where there was a modest difference in blood pressure of 3/2 mm Hg) was blood pressure lowering
- the study authors concluded that ACE inhibitor therapy should be used in most patients with vascular disease or diabetes and additional CV risk factors
- 4,528 patients agreed to further follow-up (median follow-up period
2.6 years)
Vitamin E in the prevention of cardiovascular disease:
- study evidence (1,3) has provided no evidence of benefit of vitamin E supplementation in the prevention of the development cardiovascular disease
Vitamin C supplementation in the prevention of cardiovascular disease:
- in a large, long-term trial of male physicians, neither vitamin E nor vitamin C supplementation reduced the risk of major cardiovascular events (3)
Homocysteine lowering therapy and stroke risk (4)
- HOPE 2 investigators have analyzed stroke outcomes among participants of
the HOPE 2 trial that randomized 5522 adults with known cardiovascular disease
to a daily combination of 2.5 mg of folic acid, 50 mg of vitamin B6, and 1
mg of vitamin B12, or matching placebo, for 5 years
- among 5522 participants, stroke occurred in 258 (4.7%) individuals during a mean of 5 years of follow-up. The geometric mean homocysteine concentration decreased by 2.2 micromol/L in the vitamin therapy group and increased by 0.80 micromol/L in the placebo group
- the incidence rate of stroke was 0.88 per 100 person-years in the vitamin therapy group and 1.15 per 100 person-years in the placebo group - the hazard ratio [HR], 0.75; 95% (CI, 0.59-0.97) was significant
- vitamin therapy also significantly reduced the risk of nonfatal stroke (HR, 0.72; 95% CI, 0.54-0.95) but did not impact on neurological deficit at 24 hours (P=0.45) or functional dependence at discharge or at 7 days (OR, 0.95; 95% CI, 0.57-1.56)
- this study data suggests that homocysteine lowering therapy may have a role in lowering stroke risk
- a meta-analysis has suggested that folic acid reduces risk of stroke (5)
Reference:
- 1. New England Journal of Medicine 2000; 342: 145-53.
- 2. Bosch J et al. Long-term effects of ramipril on cardiovascular events and on diabetes: results of the HOPE study extension.Circulation. 2005 Aug 30;112(9):1339-4
- 3. Sesso HD et al.Vitamins E and C in the prevention of cardiovascular disease in men: the Physicians' Health Study II randomized controlled trial. JAMA. 2008 Nov 12;300(18):2123-33.
- 4. Saposnik G et al.; Heart Outcomes Prevention Evaluation 2 Investigators. Homocysteine-lowering therapy and stroke risk, severity, and disability: additional findings from the HOPE 2 trialStroke. 2009 Apr;40(4):1365-72.
- 5) Wang X et al.Efficacy of folic acid supplementation in stroke prevention: a meta-analysis.Lancet. 2007 ;369:1876-82.
evidence in cardiovascular (CV) medicine