Effect of Alteplase on Ischemic Stroke Mortality Is Dependent on Stroke Severity

Author:

de Havenon Adam12,Abbasi Mehdi1ORCID,Yaghi Shadi3,Delic Alen4,Bangad Aaron1ORCID,Johnston Karen5,Tirschwell David6,Sheth Kevin N.12ORCID

Affiliation:

1. Department of Neurology Yale University New Haven CT USA

2. Yale Center for Brain & Mind Health Yale University New Haven CT USA

3. Department of Neurology The Warren Alpert Medical School of Brown University Providence RI USA

4. Department of Neurology University of Utah Salt Lake City Utah USA

5. Department of Neurology University of Virginia Charlottesville VA USA

6. Department of Neurology University of Washington Washington DC USA

Abstract

ObjectiveAlthough intravenous alteplase (IV‐tPA) has a beneficial effect on functional outcome after ischemic stroke (IS), prior studies of IV‐tPA's impact on post‐stroke mortality did not have sufficient representation of more severe stroke.MethodsWe determined if the interaction between the baseline National Institutes of Health (NIH) Stroke Scale (NIHSS) and IV‐tPA modified the risk of mortality after IS in two cohorts: (1) National Inpatient Sample 2016–2020, and (2) a harmonized cohort of IS patients from the NINDS IV‐tPA, ALIAS part 2, SHINE, FAST‐MAG, IMS‐III, POINT, and DEFUSE 3 trials. We fit logistic regression models to the outcome of in‐hospital mortality (National Inpatient Sample [NIS] cohort) or mortality within 90 days (harmonized cohort), adjusted for baseline variables.ResultsWe included 198,668 patients in the NIS cohort, of which 14.0% received IV‐tPA and 3.4% died in hospital. We included 7,138 patients in the harmonized cohort, of which 33.2% received IV‐tPA and 9.4% died by 90 days. Mortality in the NIS cohort was associated with older age, female sex, non‐Hispanic white race, atrial fibrillation, and higher NIHSS. In the harmonized cohort, mortality was associated with older age, diabetes, atrial fibrillation, and higher NIHSS. In both cohorts, the interaction between NIHSS and IV‐tPA was significant. In the NIS cohort, the separation became significant at NIHSS 15 and in the harmonized cohort at NIHSS 23, at which point, IV‐tPA began to have a significant benefit for both in‐hospital and 90‐day mortality, respectively.InterpretationIV‐tPA is associated with a reduction in both in‐hospital and 90‐day mortality for patients with more severe IS. ANN NEUROL 2023;93:1106–1116

Funder

American Heart Association

National Center for Advancing Translational Sciences

National Institute of Neurological Disorders and Stroke

Publisher

Wiley

Subject

Neurology (clinical),Neurology

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