Risks of intracranial hemorrhage among patients with acute ischemic stroke receiving warfarin and treated with intravenous tissue plasminogen activator.

dc.contributor.author

Xian, Y

dc.contributor.author

Liang, L

dc.contributor.author

Smith, EE

dc.contributor.author

Schwamm, LH

dc.contributor.author

Reeves, MJ

dc.contributor.author

Olson, DM

dc.contributor.author

Hernandez, AF

dc.contributor.author

Fonarow, GC

dc.contributor.author

Peterson, ED

dc.date.accessioned

2020-11-03T18:54:07Z

dc.date.available

2020-11-03T18:54:07Z

dc.date.issued

2012-06

dc.date.updated

2020-11-03T18:54:07Z

dc.description.abstract

Intravenous tissue plasminogen activator (tPA) is known to improve outcomes in ischemic stroke; however, patients receiving long-term chronic warfarin therapy may face an increased risk for intracranial hemorrhage when treated with tPA. Although current guidelines endorse administering intravenous tPA to warfarin-treated patients if their international normalized ratio (INR) is 1.7 or lower, there are few data on safety of intravenous tPA in warfarin-treated patients in clinical practice.To determine the risk of symptomatic intracranial hemorrhage (sICH) among patients with ischemic stroke treated with intravenous tPA who were receiving warfarin vs those who were not and to determine this risk as a function of INR.Observational study, using data from the American Heart Association Get With The Guidelines-Stroke Registry, of 23,437 patients with ischemic stroke and with INR of 1.7 or lower, treated with intravenous tPA in 1203 registry hospitals from April 2009 through June 2011.Symptomatic intracranial hemorrhage. Secondary end points include life-threatening/serious systemic hemorrhage, any tPA complications, and in-hospital mortality.Overall, 1802 (7.7%) patients with stroke treated with tPA were receiving warfarin (median INR, 1.20; interquartile range [IQR], 1.07-1.40). Warfarin-treated patients were older, had more comorbid conditions, and had more severe strokes. The unadjusted sICH rate in warfarin-treated patients was higher than in non-warfarin-treated patients (5.7% vs 4.6%, P < .001), but these differences were not significantly different after adjustment for baseline clinical factors (adjusted odds ratio [OR], 1.01 [95% CI, 0.82-1.25]). Similarly, there were no significant differences between warfarin-treated and non-warfarin-treated patients for serious systemic hemorrhage (0.9% vs 0.9%; adjusted OR, 0.78 [95% CI, 0.49-1.24]), any tPA complications (10.6% vs 8.4%; adjusted OR, 1.09 [95% CI, 0.93-1.29]), or in-hospital mortality (11.4% vs 7.9%; adjusted OR, 0.94 [95% CI, 0.79-1.13]). Among warfarin-treated patients with INRs of 1.7 or lower, the degree of anticoagulation was not statistically significantly associated with sICH risk (adjusted OR, 1.10 per 0.1-unit increase in INR [95% CI, 1.00-1.20]; P = .06).Among patients with ischemic stroke, the use of intravenous tPA among warfarin-treated patients (INR ≤1.7) was not associated with increased sICH risk compared with non-warfarin-treated patients.

dc.identifier

1199153

dc.identifier.issn

0098-7484

dc.identifier.issn

1538-3598

dc.identifier.uri

https://hdl.handle.net/10161/21676

dc.language

eng

dc.publisher

American Medical Association (AMA)

dc.relation.ispartof

JAMA

dc.relation.isversionof

10.1001/jama.2012.6756

dc.subject

Humans

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Brain Ischemia

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Intracranial Hemorrhages

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Acute Disease

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Warfarin

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Tissue Plasminogen Activator

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Fibrinolytic Agents

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Anticoagulants

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International Normalized Ratio

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Infusions, Intravenous

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Registries

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Hospital Mortality

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Risk

dc.subject

Case-Control Studies

dc.subject

Aged

dc.subject

Aged, 80 and over

dc.subject

Female

dc.subject

Male

dc.subject

Stroke

dc.title

Risks of intracranial hemorrhage among patients with acute ischemic stroke receiving warfarin and treated with intravenous tissue plasminogen activator.

dc.type

Journal article

duke.contributor.orcid

Xian, Y|0000-0002-1237-1162

duke.contributor.orcid

Hernandez, AF|0000-0003-3387-9616

duke.contributor.orcid

Peterson, ED|0000-0002-5415-4721

pubs.begin-page

2600

pubs.end-page

2608

pubs.issue

24

pubs.organisational-group

Faculty

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Duke

pubs.organisational-group

School of Medicine

pubs.organisational-group

Duke Clinical Research Institute

pubs.organisational-group

Medicine, Cardiology

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Institutes and Centers

pubs.organisational-group

Medicine

pubs.organisational-group

Clinical Science Departments

pubs.organisational-group

Neurology, Neurocritical Care

pubs.organisational-group

Medicine, Clinical Pharmacology

pubs.organisational-group

Neurology

pubs.publication-status

Published

pubs.volume

307

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