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(Circulation. 1997;96:2751-2753.)
© 1997 American Heart Association, Inc.
Articles |
Key Words: AHA Medical/Scientific Statements aspirin myocardial infarction prevention cardiovascular disease
| Introduction |
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| Acute Myocardial Infarction |
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To achieve an immediate clinical antithrombotic effect, an initial minimum loading dose of 162 mg should be used in acute MI. If an enteric-coated aspirin is the only preparation available, the first tablet should be chewed or crushed before administration. In 1996 the US Food and Drug Administration (FDA)4 proposed a professional labeling indication for aspirin in patients with acute MI: an initial dose of 160 to 162.5 mg to be continued daily for at least 30 days.
Despite its clear benefits in this clinical setting, aspirin as a treatment for acute MI remains underused. In 1993 in a national registry of more than 1000 large US hospitals, only 77% of patients with acute MI received aspirin.5 In a survey of treatment of Medicare patients in the early 1990's, only 61% of a sample of acute MI patients aged 65 and older were taking aspirin within 2 days of hospitalization.6 Increased administration of aspirin to virtually all patients with acute MI would save an additional 5000 to 10 000 lives in the United States each year.7
| Secondary Prevention |
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The most widely tested regimen in the secondary prevention trials was medium-dose aspirin (75 to 325 mg/d), and in the overall analyses there was no evidence that either higher doses of aspirin or any other antiplatelet regimen was more effective than daily aspirin in this dose range. In the trials of stroke and TIA, higher doses (650 to 1300 mg/d) were used, but in trials of post-MI patients, lower doses (75 to 325 mg/d) appeared equally beneficial in reducing risks of subsequent stroke.9 Therefore, daily aspirin therapy at a dose of at least 75 to 325 mg should be strongly considered for all such patients at elevated risk of subsequent vascular events. For patients with TIA or stroke, at least 75 to 325 mg a day is indicated,10 and doses from 650 to 1300 mg/d may be more beneficial11 but will produce more side effects.12 13
Since publication of the 1994 Antiplatelet Trialists' Collaboration overview, several additional trials have compared other antiplatelet agents with aspirin. In the TASS study,14 those receiving ticlopidine (500 mg/d) had a 21% decrease in all types of stroke at 3 years compared with those receiving aspirin (1300 mg/d). The occurrence of neutropenia in almost 1% of patients receiving ticlopidine as well as its additional expense may limit its clinical use. Clopidogrel (75 mg/d) was compared with aspirin (325 mg/d) in a randomized trial of 19 185 patients with recent ischemic stroke, MI, or peripheral arterial disease.15 Annual rates of the composite outcome of ischemic stroke, MI, and vascular death were 5.83% and 5.32% in the aspirin and clopidogrel groups, respectively (p=0.043), with no major differences reported in the safety of the two regimens.
In the 1980s the FDA approved professional labeling indications for aspirin in patients with prior MI and unstable angina16 as well as for men with prior TIAs.17 In January 1997, at a joint meeting of the FDA Nonprescription Drugs and Cardiovascular and Renal Drugs Advisory Committees, members voted to recommend that the FDA expand the professional labeling indication to include women as well as men with prior TIAs and patients with prior occlusive stroke or chronic stable angina.
| Primary Prevention |
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Additional data in primary prevention are needed for complete assessment of aspirin's benefit-to-risk ratio in apparently healthy persons. Specifically such data would allow clinicians to weigh the clear benefit of aspirin on MI against any risks, including a possible increase in hemorrhagic stroke. Such evidence will be provided by the Women's Health Study,19 an ongoing trial of administration of low-dose aspirin among approximately 40 000 US female healthcare professionals. Pending the results of this trial, any policy recommendation concerning aspirin in the primary prevention of cardiovascular disease would be premature. The US Preventive Services Task Force20 has issued a similar statement, concluding that there is insufficient evidence to recommend for or against routine aspirin prophylaxis in primary prevention and that any use should be an individual clinical judgment. While awaiting definitive data from the Women's Health Study, aspirin therapy in primary prevention may be warranted for patients at risk of MI. However, such use must at present be based on an individual clinical judgment by healthcare providers that takes into account a patient's particular cardiovascular risk profile, the demonstrated benefits of aspirin on reducing risk of a first MI, and known as well as unknown side effects.
| Summary |
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| Footnotes |
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A single reprint is available by calling 800-242-8721 (US only) or writing the American Heart Association, Public Information, 7272 Greenville Avenue, Dallas, TX 75231-4596. Ask for reprint No. 71-0129. To purchase additional reprints: up to 999 copies, call 800-611-6083 (US only) or fax 413-665-2671; 1000 or more copies, call 214-706-1466, fax 214-691-6342, or
| References |
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Fuster V, Dyken ML, Vokonas PS, Hennekens C. Aspirin as a
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3. ISIS-2 (Second International Study of Infarct Survival) Collaborative Group. Randomised trial of intravenous streptokinase, oral aspirin, both, or neither among 17,187 cases of suspected acute myocardial infarction: ISIS-2. Lancet. 1988;2:349-360.[Medline] [Order article via Infotrieve]
4. US Food and Drug Administration. Internal analgesic, antipyretic, and antirheumatic drug products for over-the-counter human use: proposed amendment to the tentative final monograph. Federal Register. June 13, 1996;61:30002.
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Rogers WJ, Bowlby LJ, Chandra NC, French WJ, Gore JM, Lambrew
CT, Rubison RM, Tiefenbrunn HJ, Weaver WD. Treatment of myocardial
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Krumholz HM, Radford MJ, Ellerbeck EF, Hennen J, Meehan TP,
Petrillo M, Wang Y, Kresowik TF, Jencks SF. Aspirin in the treatment of
acute myocardial infarction in elderly Medicare beneficiaries: patterns
of use and outcomes. Circulation. 1995;92:2841-2847.
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Hennekens CH, Jonas MA, Buring JE. The benefits of aspirin in
acute myocardial infarction: still a well-kept secret in the US.
Arch Intern Med. 1994;154:37-39.
8.
Antiplatelet Trialists Collaboration. Collaborative
overview of randomized trials of antiplatelet treatment, I:
prevention of vascular death, MI and stroke by prolonged
antiplatelet therapy in different categories of patients. Br
Med J. 1994;308:235-246.
9.
Hennekens CH, Buring JE, Sandercock P, Collins R, Peto R.
Aspirin and other antiplatelet agents in the secondary and primary
prevention of cardiovascular disease.
Circulation. 1989;80:749-756.
10. Hebert P, Fuster V, Hennekens CH. Antiplatelet and anticoagulant therapy in evolving MI and primary prevention. In: Fuster V, Verstraete M, eds. Thrombosis and Cardiovascular Disease. Philadelphia, Pa: WB Saunders; 1992;14:261-273.
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Dyken ML, Barnett HJ, Easton JD, Fields WS, Fuster V,
Hachinski V, Norris JW, Sherman DG. Low dose aspirin and stroke: `It
ain't necessarily so.' Stroke. 1992;23:1395-1399.
12. UK-TIA Study Group. United Kingdom transient ischaemic attack (UK-TIA) aspirin trial interim results. Br Med J. 1988;296:316-320.
13. Antiplatelet Trialists Collaboration (Barnett H, Bousser M-G, Boysen G, Breddin K, Britton M, Cairns J, Canner P, Collins R, Cortellaro M, Daniels A, Deykin D, Elwood P, Elwin E-E, Eschwege E, Farrell B, Fields WS, Gent M, Gray R, Guiraud-Chaumeil B, Hennekens CH, Klimt C, Lewis HD, Loria Y, Lowenthal A, MacMahon C, Miller J, Peto R, Qizilbash N, Reuther R, Richards S, Rosen A, Sandercock P, Sorensen PS, Sweetnam D, Taylor W, Thibult N, van Gijn J, Vogel G, Warlow C, Yusuf S). Secondary prevention of vascular disease by prolonged antiplatelet therapy. Br Med J. 1988;296:320-331.
14. Hass WK, Easton JD, Adams HP Jr, Pryse-Phillips W, Molony BA, Anderson S, Kamm B. A randomized trial comparing ticlopidine hydrochloride with aspirin for the prevention of stroke in high-risk patients. N Engl J Med. 1989;321:501-507.[Abstract]
15. CAPRIE Steering Committee. A randomised, blinded trial of clopidogrel versus aspirin in patients at risk of ischaemic events (CAPRIE). Lancet. 1996;348:1329-1339.[Medline] [Order article via Infotrieve]
16. Aspirin for heart patients. FDA Drug Bull. 1985;15:34-36.[Medline] [Order article via Infotrieve]
17. Aspirin for TIAs. FDA Drug Bull. 1980;10:2.
18. Steering Committee of the Physicians' Health Study Research Group. Final report on the aspirin component of the ongoing Physicians' Health Study. N Engl J Med. 1989;321:129-135.[Abstract]
19. Buring JE, Hennekens CH, for the Women's Health Study Research Group. The Women's Health Study: summary of the study design. J Myocardial Ischemia. 1992;4:27-29.
20. US Preventive Services Task Force. Guide to Clinical Preventive Services. 2nd ed. Baltimore, Md: Williams & Wilkins; 1996.
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