Editorial
 
Risk of hemorrhagic stroke from aspirin use: Does risk outweigh the benefit?
Fatai Kunle Salawu1, Zira Gyhi Vandi2
1Division of Neurology, Department of Medicine, Federal Medical Centre Yola, Nigeria
2Division of Cardiology, Department of Medince, Aminu Kano Teaching Hospital, Kano, Nigeria

Article ID: 100012N06FS2018
doi:10.5348/N06-2018-12-ED-1

Corresponding Author:
Fatai Kunle Salawu
Division of Neurology, Department of Medicine,
Federal Meical Centre Yola 640001,
Adamawa State,
Nigeria

Access full text article on other devices

  Access PDF of article on other devices

[HTML Abstract]   [PDF Full Text] [Print This Article]
[Similar article in Pumed] [Similar article in Google Scholar]

How to cite this article
Salawu FK, Vandi ZG. Risk of hemorrhagic stroke from aspirin use: Does risk outweigh the benefit? Edorium J Neurol 2018;5:1–3

Aspirin has been widely used to prevent myocardial infarction and ischemic stroke but some authors have suggested that it increases the risk of hemorrhagic stroke. The first randomized controlled trial of aspirin in the prevention of vascular events was conducted in South Wales in 1974 [1]. Since then overviews of numerous trials [2][3] have established aspirin in cardiovascular disease, as the most thoroughly and the most highly cost-effective drug available in clinical practice. Aspirin is now a standard part of both the early and the long-term management of coronary thrombosis. Aspirin was introduced as an analgesic and antipyretic agent in the late 1890s. However, it is only during the past two decades that attention has been focused on the therapeutic effect of aspirin on cardiovascular disease [4]. A number of large randomized controlled clinical trials have demonstrated that aspirin treatment reduces the risk of subsequent myocardial infarction and ischemic stroke among patients with a wide range of pre-existing cardiovascular diseases [5][6] [7][8][9][10]. A study suggested that aspirin treatment reduces the risk of non-fatal myocardial infarction in healthy individuals [11][12]. Aspirin is now being used for primary and secondary prevention of cardiovascular disease in the general population [13][14][15]. Several studies have suggested that aspirin increases the risk of hemorrhagic stroke [5][6] [7][8][9][10][11][12]. It should be used with caution in individuals, who are at high risk of hemorrhagic stroke, e.g., hypertensive patients with a low level of serum cholesterol [16][17]. Although aspirin therapy has been well documented to reduce the incidence of myocardial infarction in those who are at relatively high risk, its benefits have not been well documented in healthy persons who are younger than 50 years [11][12]. Thus, aspirin treatment may not be recommended to such persons for the purpose of primary prevention of cardiovascular disease. There is overwhelming evidence that aspirin reduces cardiovascular disease morbidity and mortality in patients with ischemic heart disease or stroke. A meta-analysis of randomized controlled trials involving 16 trials with 55,462 participants and 108 hemorrhagic stroke cases revealed aspirin use was associated with an absolute reduction of 97 cardiovascular deaths per 10,000 persons, 137 myocardial infarction events per 10,000 persons and 39 ischemic stroke events per 10,000 persons. Even in healthy populations older than 50 years in western countries, the absolute risk reduction of myocardial infarction and ischemic stroke is much higher than that of hemorrhagic stroke [18]. Therefore, the overall benefit of aspirin use on myocardial infarction and ischemic stroke almost certainly overcomes the potential risk of hemorrhagic stroke in such groups.

There are several possible mechanisms by which aspirin could increase the risk of hemorrhagic stroke. Aspirin selectively acetylates the hydroxyl group of a single serine residue at position 529 within the polypeptide chain of platelet prostaglandin G/H synthase 1, causing irreversible loss of its cyclooxygenase activity [4][19]. This results in decreased conversion of arachidonate to prostaglandin G2 and ultimately of prostaglandin H2 and thromboxane A2, which are important mediators in platelet aggregation and thrombi formation. Platelets are exquisitely sensitive to aspirin. A dosage of only 30 mg/day effectively eliminates the synthesis of thromboxane A2. The minimum dosage of aspirin in the trials that were included in the meta-analysis by He et al. was 75 mg/day which is higher than this threshold [20]. Several trials failed to include data on stroke subtypes, while some of the trials were conducted in the late 1970s or early 1980s, when computed tomography might have been routinely used for the diagnosis of stroke.

There is little doubt wheter the use of aspirin in the primary and secondary prevention of cardiovascular events and stroke slightly increases the risk of serious bleeding, or not but this risk is outweighed by its beneficial effect.

Keywords : Aspirin, Coronary thrombosis, Hemorrhagic stroke


REFERENCES
  1. Elwood PC, Cochrane AL, Burr ML, et al. A randomized controlled trial of acetyl salicylic acid in the secondary prevention of mortality from myocardial infarction. Br Med J 1974 Mar 9;1(5905):436–40.   [Pubmed]    Back to citation no. 1
  2. Rapaport E, Gheorghiade M. Pharmacologic therapies after myocardial infarction. Am J Med 1996 Oct 8;101(4A):4A61S-69S; discussion 4A69S–70S.   [CrossRef]   [Pubmed]    Back to citation no. 2
  3. Prasad N, Srikanthan VS, Wright A, Dunn FG. Management of suspected myocardial infarction before admission: Updated audit. BMJ 1998 Jan 31;316(7128):353.   [CrossRef]   [Pubmed]    Back to citation no. 3
  4. Willard JE, Lange RA, Hillis LD. The use of aspirin in ischemic heart disease. N Engl J Med 1992 Jul 16;327(3):175–81.   [CrossRef]   [Pubmed]    Back to citation no. 4
  5. Elwood PC, Sweetnam PM. Aspirin and secondary mortality after myocardial infarction. Lancet 1979 Dec 22–29;2(8156–8157):1313–5.   [CrossRef]   [Pubmed]    Back to citation no. 5
  6. A randomized, controlled trial of aspirin in persons recovered from myocardial infarction. JAMA 1980 Feb 15;243(7):661–9.   [CrossRef]   [Pubmed]    Back to citation no. 6
  7. Randomised trial of intravenous streptokinase, oral aspirin, both, or neither among 17,187 cases of suspected acute myocardial infarction: ISIS-2: ISIS-2 (Second international study of infarct survival) collaborative group. Lancet 1988 Aug 13;2(8607):349–60.   [CrossRef]   [Pubmed]    Back to citation no. 7
  8. Swedish aspirin low-dose trial (SALT) of 75 mg aspirin as secondary prophylaxis after cerebrovascular ischaemic events: The SALT collaborative group. Lancet 1991 Nov 30;338(8779):1345–9.   [CrossRef]   [Pubmed]    Back to citation no. 8
  9. Farrell B, Godwin J, Richards S, Warlow C. The United Kingdom transient ischaemic attack (UK-TIA) aspirin trial: Final results. J Neurol Neurosurg Psychiatry 1991 Dec;54(12):1044–54.   [CrossRef]   [Pubmed]    Back to citation no. 9
  10. Juul-Möller S, Edvardsson N, Jahnmatz B, Rosén A, Sørensen S, Omblus R. Double-blind trial of aspirin in primary prevention of myocardial infarction in patients with stable chronic angina pectoris: The Swedish angina pectoris aspirin trial (SAPAT) group. Lancet 1992 Dec 12;340(8833):1421–5.   [CrossRef]   [Pubmed]    Back to citation no. 10
  11. Peto R, Gray R, Collins R, et al. Randomised trial of prophylactic daily aspirin in British male doctors. Br Med J (Clin Res Ed) 1988 Jan 30;296(6618):313–6.   [Pubmed]    Back to citation no. 11
  12. 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 Jul 20;321(3):129–35.   [CrossRef]   [Pubmed]    Back to citation no. 12
  13. Hume AL, Barbour MM, Lapane KL, Assaf AR, Carleton RA. Prevalence and descriptors of aspirin use as an antiplatelet agent in two New England communities. Ann Pharmacother 1993 Apr;27(4):442–4.   [CrossRef]   [Pubmed]    Back to citation no. 13
  14. Shahar E, Folsom AR, Romm FJ, et al. Patterns of aspirin use in middle-aged adults: The atherosclerosis risk in communities (ARIC) study. Am Heart J 1996 May;131(5):915–22.   [CrossRef]   [Pubmed]    Back to citation no. 14
  15. Reeves MJ, McGee H, Rafferty AP, Remington P, Cautley E. Prevalence of aspirin use to prevent heart disease: Wisconsin, 1991, and Michigan, 1994. MMWR Morb Mortal Wkly Rep 1997 Jun 6;46(22):498–502.    Back to citation no. 15
  16. Puddey IB. Low serum cholesterol and the risk of cerebral haemorrhage. Atherosclerosis 1996 Jan 5;119(1):1–6.   [Pubmed]    Back to citation no. 16
  17. He J, Klag MJ, Wu Z, Whelton PK. Stroke in the People's Republic of China. I. Geographic variations in incidence and risk factors. Stroke 1995 Dec;26(12):2222–7.   [CrossRef]   [Pubmed]    Back to citation no. 17
  18. American Heart Association. Heart and Stroke Facts: 1997 Statistical Supplement. Dallas, Tx: American Heart Association; 1997.    Back to citation no. 18
  19. Patrono C. Aspirin as an antiplatelet drug. N Engl J Med 1994 May 5;330(18):1287–94.   [CrossRef]   [Pubmed]    Back to citation no. 19
  20. He J, Whelton PK, Vu B, Klag MJ. Aspirin and risk of hemorrhagic stroke: A meta-analysis of randomized controlled trials. JAMA 1998 Dec 9;280(22):1930–5.   [CrossRef]   [Pubmed]    Back to citation no. 20

[HTML Abstract]   [PDF Full Text]
Author Contributions
Fatai Kunle Salawu – Substantial contributions to conception and design, Acquisition of data, Analysis and interpretation of data, Drafting the article, Revising it critically for important intellectual content, Final approval of the version to be published
Zira Gyhi Vandi – Substantial contributions to conception and design, Acquisition of data, Analysis and interpretation of data, Drafting the article, Revising it critically for important intellectual content, Final approval of the version to be published
Guarantor of Submission
The corresponding author is the guarantor of submission.
Source of Support
None
Conflict of Interest
Authors declare no conflict of interest.
Copyright
© 2018 Fatai Kunle Salawu et al. This article is distributed under the terms of Creative Commons Attribution License which permits unrestricted use, distribution and reproduction in any medium provided the original author(s) and original publisher are properly credited. Please see the copyright policy on the journal website for more information.