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Generalized efficacy of t-PA for acute stroke - Subgroup analysis of the NINDS t-PA stroke trial

T Brott,J Broderick,R Kothari,M ODonoghue,W Barsan,T Tomsick,J Spilker,R Miller,L Sauerbeck,J Farrell, J Kelly,T Perkins,R Miller, T McDonald,M Rorick,C Hickey,J Armitage,C Perry,K Thalinger, R Rhude, J Schill,PS Becker,RS Heath,D Adams,R Reed, M Klei, A Hughes,J Anthony, D Baudendistel, C Zadicoff,M Rymer, I Bettinger, P Laubinger,M Schmerler, G Meiros,P Lyden,J Dunford,J Zivin,K Rapp,T Babcock, P Daum, D Persona,M Brody,C Jackson,S Lewis,J Liss,Z Mahdavi,J Rothrock,T Tom,R Zweifler,R Kobayashi, J Kunin,J Licht,R Rowen,D Stein,J Grisolia, F Martin,E Chaplin,N Kaplitz,J Nelson, A Neuren,D Silver,T Chippendale,E Diamond, M Lobatz,D Murphy,D Rosenberg, T Ruel, M Sadoff,J Schim,J Schleimer,R Atkinson,D Wentworth,R Cummings,R Frink, P Heublein,JC Grotta,T DeGraba, M Fisher, A Ramirez,S Hanson,L Morgenstern,C Sills,W Pasteur,F Yatsu,K Andrews,C VillarCordova,P Pepe,P Bratina,L Greenberg,S Rozek,K Simmons,TG Kwiatkowski,SH Horowitz,R Libman,R Kanner,R Silverman, J LaMantia, C Mealie,R Duarte,R Donnarumma, M Okola, V Cullin,E Mitchell,SR Levine,CA Lewandowski,G Tokarski,NM Ramadan,P Mitsias,M Gorman, B Zarowitz,J Kokkinos, J Dayno,P Verro,C Gymnopoulos,R Dafer,L DOlhaberriague,K Sawaya,S Daley, M Mitchell,M Frankel,B Mackay,J Weissman,J Washington,B Nguyen,A Cook,H Karp, M Williams,T Williamson,C Barch,J Braimah, B Faherty,J MacDonald,S Sailor, M Kozinn, L Hellwick,EC Haley,TP Bleck,WS Cail,GH Lindbeck,MA Granner,SS Wolf,MW Gwynn, RW Mettetal,CWJ Chang,NJ Solenski,DG Brock, GF Ford,GL Kongable,KN Parks,SS Wilkinson,MK Davis,GL Sheppard,DW Zontine,KH Gustin,NM Crowe,SL Massey,M Meyer,K Gaines,A Payne, C Bales,J Malcolm,R Barlow, M Wilson, C Cape,T Bertorini, K Misulis, W Paulsen, D Shepard,BC Tilley,KMA Welch,SC Fagan,M Lu, S Patel, E Masha,J Verter, J Boura,J Main,L Gordon,N Maddy, T Chociemski, J Windham, SZ Zadeh,W Alves, MF Keller,JR Wenzel,N Raman,L Cantwell,A Warren,K Smith,E Bailey,JR Marler,JD Easton,JF Hallenbeck,G Lan,JD Marsh,MD Walker,J Froelich,J Breed, WC Fong

STROKE(1997)

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Abstract
Background and Purpose We sought to identify subgroups of stroke patients in w Methods We conducted a post hoc subgroup analysis of a randomized, double-blind, placebo-controlled clinical trial of intravenous tissue plasminogen activator (t-PA) for stroke patients presenting within 3 hours after symptom onset. Before treatment, historical, physical, and laboratory findings were summarized. We identified variables that might predict outcome and/or differential response to t-PA therapy. Outcome was measured with four stroke rating scales administered 3 months after treatment. Statistical significance was assessed with a global outcome procedure that considers the results of all four scales simultaneously. Using regression analysis, we compared the information collected before treatment with the global outcome. Multivariable procedures were used to find information that could guide selection of patients for t-PA. Results No pretreatment information significantly affected patients' response to t-PA. The power of the model to detect a treatment interaction was greater than 90%, and therefore the probability of a type II error is very low. Apart from t-PA therapy, outcome was related to age-by-deficit severity interaction, diabetes, age-by-blood pressure interaction, and early CT findings. These variables and interactions altered long-term patient outcome irrespective of t-PA treatment but did not alter the likelihood of responding favorably to t-PA therapy. Conclusions Patients should be selected for t-PA thrombolysis according to the guidelines published in the report of the NINDS t-PA Stroke Trial. Further subselection of patients, such as by age or stroke severity, is not supported by our post hoc analysis.
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Key words
thrombolytic therapy,cerebral ischemia,clinical trials,plasminogen activators
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