The American Journal of Medicine (2006) 119, 198-202
Aspirin to Prevent Heart Attack and Stroke: What’s the Right Dose? James E. Dalen, MD, MPH Professor Emeritus, University of Arizona, Tucson ABSTRACT
Despite hundreds of clinical trials, the appropriate dose of aspirin to prevent myocardial infarction (MI)and stroke is uncertain. In the US, the doses most frequently recommended are 80, 160, or 325 mg per day. Because aspirin can cause major bleeding, the appropriate dose is the lowest dose that is effective inpreventing both MI and stroke because these two diseases frequently co-exist. Five randomized clinicaltrials have compared aspirin with placebo or no therapy for the prevention of stroke and MI. These trialsvaried with regard to the dose of aspirin, the duration of treatment, and, most important, the populationsselected for study varied in their baseline risk of stroke and MI. In men, 160 mg/day consistently loweredthe risk of MI. In women, doses of 50 mg, 75, and 100 mg/day did not significantly decrease the risk ofMI; therefore, the appropriate dose in women must exceed 100 mg/day. The appropriate dose for theprimary prevention of stroke in men and women has not been established. Doses of 75 and 100 mg/dayhave been ineffective in men and women. The appropriate dose must be at least 160 mg/day. The lowestdose to prevent recurrent MI or death in patients with stable coronary artery disease (CAD) is 75 mg/day. In acute MI the lowest dose is 160 mg/day. In patients with a history of stroke or transient ischemic attack(TIA), 50 mg/day has been shown to be effective in men and women. In acute stroke, 160 mg/day iseffective in preventing recurrent stroke or death. The risk of major bleeding with 160 mg/day is the sameas with 80 mg/day: 1 to 2 cases per 1000 patient years of treatment, and the risk of fatal bleeding is thesame with 80 and 160 mg/day. These studies indicate that the most appropriate dose for the primary andsecondary prevention of stroke and MI is 160 mg/day. 2006 Elsevier Inc. All rights reserved. KEYWORDS: Aspirin; Aspirin toxicity; Stroke prevention; Heart attack prevention; Primary prevention; Secondary prevention
In 1950, Lawrence Craven, a general practitioner in Glen-
The appropriate dose of aspirin should be sufficient to
dale, Calif, was the first to report that aspirin may prevent
prevent MI, as well as stroke, because these 2 diseases have
myocardial infraction (MI), and in 1956 he was the first to
the same risk factors and frequently co-exist. Ideally, the
report that aspirin may also prevent Now, more
appropriate dose would be effective for primary and sec-
than 50 years later, after hundreds of clinical trials, it has
ondary prevention, in women as well as in men.
been well established that Craven was correct; aspirin canprevent MI and stroke.However, the appropriate dose of
THE SEARCH FOR THE LOWEST EFFECTIVE DOSE
aspirin remains uncertain. The dose in clinical trials has
Because aspirin has significant side effects; principally
ranged from 50 to 1200 mg per day. Craven recommended
bleeding, especially gastrointestinal (GI) bleeding, many
a dose of 325 mg per day, although he noted that 325 mg 5
clinical trials have sought to determine the lowest effective
dose of aspirin to prevent MI and stroke.
The Antithrombotic Trialists’ Collaboration reviewed 287
studies involving 135 000 patients that compared antiplatelet
Requests for reprints should be addressed to James E. Dalen, MD,
therapy to They concluded that doses of 75 to 325
MPH, University of Arizona, 1840 East River Road, Suite 120, Tucson, AZ
mg of aspirin are effective and that there is no additional
benefit to doses higher than 325 mg per day. They also noted
0002-9343/$ -see front matter 2006 Elsevier Inc. All rights reserved. doi:10.1016/j.amjmed.2005.11.013
Aspirin to Prevent Heart Attack and Stroke
that 75 to 150 mg/day seems to be as effective as 325 mg and
Peto et randomized 5139 presumably healthy British
that the effects of doses less than 75 mg were less
male doctors (median age 60 years) to 500 mg of aspirin per
It is now widely accepted that the optimal dose is 325
day or no aspirin. After 6 years of follow-up, there was no
mg/day or However, there is no agreement whether the
significant difference in the incidence of MI or stroke in those
optimal dose is 80, 160, or 325 mg/day. Because the cost of
taking or not taking aspirin. It should be noted that many of
CLINICAL SIGNIFICANCE
● There is general agreement that the ap-
PRIMARY PREVENTION
average follow-up of 60.2 months,there was a significant 44% reduc-
● In randomized clinical trials, doses of
● In randomized clinical trials, the risk of
● These studies indicate that the most ap-
propriate dose of aspirin to prevent myo-
included only and the other two included men and
In the Hypertension Optimal Treatment (HOT) study,
Some studies selected participants with risk fac-
18 790 patients (8831 women) aged 50 or older with hyper-
tors for cardiovascular disease or who had
tension were randomized to receive 75 mg aspirin or pla-
Given the heterogeneity of these trials, the risk of MI and
After an average follow-up of 3.8 years, there was a
stroke in the participants in these 5 trials varied signifi-
nonsignificant decrease in the incidence of stroke in those
cantly. Therefore, it is not surprising that the results were
receiving The incidence of MI was significantly
reduced by 42% in men, whereas there was an insignificantreduction in MI of 19% in
In the WHS, 39 876 healthy women aged 45 years or older
Primary Prevention Trials: Prevention of MI
were randomized to a very low dose of aspirin: 100 mg every
other day or After 10 years of follow-up, there wasa significant 17% reduction in stroke in those treated with
aspirin. However, the reduction in stroke in women aged 65
and older was not significant. The incidence of MI was not
decreased in the total patient population. However, there was a
significant 34% decrease in MI in women age 65 or older. LOWEST DOSE FOR PRIMARY PREVENTION
ASA ϭ aspirin; WHS ϭ Women’s Health Study; HOT ϭ Hypertension
Optimal Treatment study; PPP ϭ Primary Prevention Project; PHS ϭPhysician’s Health Study; UK ϭ British physician study.
As shown in the lowest reported dose to prevent
myocardial infarction in women, 50 mg/day (100 mg QOD),
was reported by the WHS, but it was limited to women aged
‡Stroke data for men and women combined.
65 years or In the total group of women aged 45 and
The American Journal of Medicine, Vol 119, No 3, March 2006
older, there was an insignificant 2% increase in myocardial
SECONDARY PREVENTION OF MI
infarction. These findings in the WHS were not consistent
The Swedish Angina Pectoris Aspirin Trial (SAPAT) ran-
with the results in women in other trials. In the HOT trial,
domized 2035 patients (977 women) with stable angina
a daily dose of 75 mg in women age 50ϩ with hypertension
pectoris to aspirin 75 mg/day versus None of the
resulted in an insignificant decrease in MI of In the
patients had a history of prior MI. All patients also received
Primary Prevention 100 mg per day resulted in an
sotalol. After a median follow-up of 50 months the inci-
insignificant decrease in MI of 31% in men and women
dence of MI and sudden death was a significant 34% lower
aged 50 years and older who had at least one major cardio-
in those treated with aspirin plus sotalol, compared with
those receiving sotalol plus placebo. In addition, there was
The combined results of these studies indicate that the
a 25% reduction in stroke that was not statistically signifi-
lowest effective dose of aspirin to prevent MI in women
aged 50 or older is more than 100 mg per day.
In a Veterans Administration (VA) study of 1266 men
In men, the lowest effective dose to prevent MI was
with unstable angina, 325 mg of aspirin daily significantly
reported in the HOT Men aged 50 or older with
decreased the risk of MI or sudden death by 51% in those
hypertension had a significant 42% reduction in MI with a
taking In the Relationship between Insulin Sensi-
daily dose of 75 mg. However, in the PPP trial 100 mg of
tivity and Cardiovascular disease risk (RISC) study of 796
aspirin resulted in a statistically insignificant 31% reduction
men with unstable angina, there was a significant 31%
in In the U.S. physicians 325 mg of aspirin
reduction in MI or sudden death after a daily dose of 75 mg
QOD led to a significant 44% reduction in MI in men aged
50 or older. Given these data, the lowest effective dose for
In the Second International Study of Infarct Survival
the primary prevention of MI in men age 50 and older is 160mg/day.
(ISIS-2) 17 187 patients with acute MI were ran-domized to 165 mg per day of aspirin for 1 month versusplacebo. Recurrent MI was significantly reduced by 45%,
LOWEST DOSE FOR PRIMARY PREVENTION
and vascular death was significantly decreased by 23%. OF STROKE
These studies indicate that the lowest effective dose to
As shown in the lowest reported effective dose for
prevent MI or sudden death in patients with stable coronary
the primary prevention of stroke, 50 mg/day, was reported
artery disease (CAD) or unstable angina is 75 mg/day. In
by the This dose resulted in a statistically significant
patients with acute myocardial infarction (AMI), the lowest
reduction in stroke of However, in women aged 65 or
effective dose to prevent recurrent MI or death is 160 mg
older, a reduction in stroke of 22% was not statistically
significant. As with the case of MI, these findings from theWHS are inconsistent with the other primary prevention
SECONDARY PREVENTION OF STROKE
trials. In the HOT Trial, 75 mg per day in men and women
The European Stroke Prevention Study (ESPS) randomized
led to a statistically insignificant decrease in stroke of
6602 patients with a history of stroke or TIA to 1 of 4
In the PPP trial, 100 mg per day led to an insignificant 33%
regimens: aspirin 50 mg/day, dipyridamole 400 mg/day,
reduction in These studies indicate that the appro-
dypridamole plus aspirin, or After 2 years of
priate dose of aspirin for the primary prevention of stroke in
treatment, the incidence of stroke in those taking aspirin was
women aged 50 or older is more than 100 mg per day.
(325 mg and 500 either increased or failed
In the Chinese Acute Stroke Trial (CAST), 21 106 with
to significantly decrease the incidence of stroke. The appro-
acute ischemic stroke were randomized to aspirin, 160 mg/
priate dose of aspirin for the primary prevention of stroke in
day or After 4 weeks, the incidence of recurrent
stroke or death in those receiving aspirin was a significant
Three randomized trials have compared aspirin in doses
10% lower than those receiving placebo.
These 2 studies indicate that aspirin, 50 mg/day, can
preventing strokes in patients with atrial fibrillation (AF).
significantly reduce the rate of recurrent stroke in patients
The incidence of stroke was reduced in each trial, but the
with a history of stroke or TIA. In patients with acute
decrease was statistically significant in only one, the Stroke
ischemic stroke, 160 mg/day of aspirin can significantly
Prevention in Atrial Fibrillation trial (SPAF In the
reduce the rate of recurrent stroke or death.
SPAF I trial, 325 mg of aspirin per day resulted in a
summarizes the lowest effective dose to signif-
significant 42% reduction in stroke as compared with pla-
icantly reduce MI and stroke in varying patient populations.
cebo. It should be noted that a trial comparing 150 to 160
The dose varies from 50 to 160 mg/day (with the exception
mg of aspirin/day with placebo in patients with AF has not
of primary stroke prevention in men, and the prevention of
stroke in patients with AF). These findings are consistent
These data indicate that the lowest effective dose of
with the report of the Antithrombotic Trialists that 75 to 150
aspirin to prevent stroke in patients with AF is 325 mg/day.
Aspirin to Prevent Heart Attack and Stroke
Stroke/death in men/women with acute stroke
WHS ϭ Women’s Health Study; HOT ϭ Hypertension Optimal Treat-
MI ϭ myocardial infarction; AF ϭ atrial fibrillation; CAD ϭ coro-
ment study; PPP ϭ Primary Prevention Project; PHS ϭ Physician’s
nary artery disease; AMI ϭ acute mycardial infarction; HX ϭ history of;
Health Study; UK ϭ British physician study.
randomized controlled studies during 368 750 patient years
BLEEDING COMPLICATIONS OF ASPIRIN
of therapy. There were actually more fatal bleeds in the
The incidence of peptic ulcer is increased during aspirin
placebo patients than in those taking doses of aspirin rang-
therapy. In the the incidence in those treated with
ing from 100 mg QOD to 500 mg per day. The absence of
aspirin was 2.7%, compared with 2.1% in controls. In the
an increase in fatal bleeding in these 5 randomized clinical
PHS the incidence in those taking aspirin (1.4%)
trials is in stark contrast to predictions of excess deaths due
was not significantly greater than placebo (1.2%). In the
to major GI hemorrhage predicted from epidemiological
British Physician the incidence in those taking as-
pirin was 2.5% versus 1.6% in the controls . There was noconsistent relationship between the dose of aspirin and the
ARE BLEEDING COMPLICATIONS RELATED TO
incidence of peptic ulcer in these studies. The aspirin dose
THE DOSE OF ASPIRIN?
in the PHS was 3 times greater than in the WHS, yet the
As noted in and there seems to be no relationship
incidence of peptic ulcer was lower in the PHS and was not
between aspirin dose and the incidence of major bleeding or
significantly greater than those taking a
fatal bleeding in the 5 primary prevention trials.
The risk of major bleeding, in most cases GI bleeding, is
clearly increased with aspirin therapy, as shown in
meta-analyses of 287 studies of antiplatelet therapy versus
However, the excess risk of major bleeding with aspirin in
control in 135 000 patients. The risk of a major extracranial
these studies was modest, ranging from 0.19 to 1.6 cases per
bleed with daily aspirin doses ranging from Ͻ75 mg to 325
1000 patient-years. This is consistent with the rate of 2 per
mg is shown in There was no significant difference
1000 patient-years reported by the Antithrombotic Trial-
in the relative risk of a major extracranial bleed in those
The excess rate of major bleeding was not related to
receiving Ͻ75 mg versus those receiving 160 to 325 mg per
the dose of aspirin in these 5 trials. The rate was higher in
the HOT which prescribed 75 mg/day, than in the
Serebruany et reported a similar meta-analysis of the
bleeding complications in 50 randomized controlled trials of
indicates the number of patients with fatal bleed-
antiplatelet agents involving 338 191 patients. They classi-
ing during aspirin therapy compared with placebo in 5
fied major bleeding as intracranial bleeding, overt bleedingwith a decrease in hemoglobin Ͼ5 g/dL, or a decreasedhematocrit Ͼ15%.
Their findings, as shown in are consistent with
those of the Antithrombotic There was no signif-
icant difference in the incidence of major bleeding between
ASA ϭ aspirin; WHS ϭ Women’s Health Study; HOT ϭ Hypertension
Optimal Treatment study; PPP ϭ Primary Prevention Project; PHS ϭ
Physician’s Health Study; UK ϭ British physician study
The American Journal of Medicine, Vol 119, No 3, March 2006
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CONCLUSIONS
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