TY - JOUR KW - Female KW - Humans KW - Aged KW - Double-Blind Method KW - Male KW - Middle Aged KW - Prognosis KW - Placebos KW - Stroke KW - Age Factors KW - Treatment Failure KW - Comorbidity KW - Drug Administration Schedule KW - Meta-Analysis as Topic KW - Epidemiology KW - physiopathology KW - Administration and dosage KW - Adverse effects KW - Drug therapy KW - metabolism KW - Prevention and control KW - Antioxidants KW - Benzenesulfonates KW - Brain Ischemia KW - Brain KW - Cerebral Hemorrhage KW - Cerebral Infarction KW - Emergency Medical Services KW - Encephalitis KW - Hyperglycemia KW - Injections KW - Intravenous KW - Neuroprotective Agents AU - Davis S. AU - Diener H. AU - Lees K. AU - Grotta J. AU - Davalos A. AU - Shuaib A. AU - Ashwood T. AU - Wasiewski W. AU - Alderfer V. AU - Hardemark H. AU - Rodichok L. AU - SAINT I and II Investigators AU - Lyden P. AU - Anderson Craig AB -
BACKGROUND AND PURPOSE: In animal models of acute ischemic stroke (AIS), the free radical-trapping agent NXY-059 showed promise as a neuroprotectant. SAINT I and II were randomized, placebo-controlled, double-blind trials to investigate the efficacy of NXY-059 in patients with AIS. METHODS: Patients with AIS received an infusion of intravenous NXY-059 or placebo within 6 hours from the onset of stroke symptoms. A pooled individual patient analysis was prespecified to assess the overall efficacy and to examine subgroups. The primary end point was the distribution of disability scores measured on the modified Rankin scale (mRS) at 90 days. Neurologic and activities of daily living scores were investigated as secondary end points. We also evaluated whether treatment with NXY-059 would reduce alteplase-related intracranial hemorrhages. Finally, we evaluated possible predictors of good or poor outcome. RESULTS: An intent-to-treat efficacy analysis was based on 5028 patients. Baseline parameters and prognostic factors were well balanced between treatment groups. The distribution of scores on the mRS was not different in the group treated with NXY-059 (n=2438) compared with the placebo group (n=2456): odds ratio for limiting disability=1.02; 95% CI, 0.92 to 1.13 (P=0.682, Cochran-Mantel-Haenszel test). Comparisons at each level of the mRS confirmed an absence of benefit. There was no evidence of efficacy in prespecified subgroups or from the secondary outcome analyses. Mortality was equal in the 2 groups (16.7% vs 16.5%), and adverse event rates were similar. Among patients treated with alteplase, there was no decrease in rates of symptomatic or asymptomatic hemorrhage associated with NXY-059 treatment versus placebo. Subgroup analyses identified National Institutes of Health Stroke Scale score, age, markers of inflammation, blood glucose, and right-sided infarct as predictors of poor outcome. CONCLUSIONS: NXY-059 is ineffective for treatment of AIS within 6 hours of symptom onset. This is also true for subgroups and the prevention of alteplase-associated hemorrhage.
AD - Department of Neurology, University of Duisburg-Essen, Hufelandstrasse 55, 45122 Essen, Germany. hans.diener@uni-duisburg-essen.de AN - 18369171 BT - Stroke DP - NLM ET - 2008/03/29 LA - eng M1 - 6 N1 - Diener, Hans-ChristophLees, Kennedy RLyden, PatrickGrotta, JimDavalos, AntoniDavis, Stephen MShuaib, AshfaqAshwood, TimWasiewski, WarrenAlderfer, VivianHardemark, Hans-GoranRodichok, LarrySAINT I and II InvestigatorsRandomized Controlled TrialUnited StatesStroke. 2008 Jun;39(6):1751-8. Epub 2008 Mar 27. N2 -BACKGROUND AND PURPOSE: In animal models of acute ischemic stroke (AIS), the free radical-trapping agent NXY-059 showed promise as a neuroprotectant. SAINT I and II were randomized, placebo-controlled, double-blind trials to investigate the efficacy of NXY-059 in patients with AIS. METHODS: Patients with AIS received an infusion of intravenous NXY-059 or placebo within 6 hours from the onset of stroke symptoms. A pooled individual patient analysis was prespecified to assess the overall efficacy and to examine subgroups. The primary end point was the distribution of disability scores measured on the modified Rankin scale (mRS) at 90 days. Neurologic and activities of daily living scores were investigated as secondary end points. We also evaluated whether treatment with NXY-059 would reduce alteplase-related intracranial hemorrhages. Finally, we evaluated possible predictors of good or poor outcome. RESULTS: An intent-to-treat efficacy analysis was based on 5028 patients. Baseline parameters and prognostic factors were well balanced between treatment groups. The distribution of scores on the mRS was not different in the group treated with NXY-059 (n=2438) compared with the placebo group (n=2456): odds ratio for limiting disability=1.02; 95% CI, 0.92 to 1.13 (P=0.682, Cochran-Mantel-Haenszel test). Comparisons at each level of the mRS confirmed an absence of benefit. There was no evidence of efficacy in prespecified subgroups or from the secondary outcome analyses. Mortality was equal in the 2 groups (16.7% vs 16.5%), and adverse event rates were similar. Among patients treated with alteplase, there was no decrease in rates of symptomatic or asymptomatic hemorrhage associated with NXY-059 treatment versus placebo. Subgroup analyses identified National Institutes of Health Stroke Scale score, age, markers of inflammation, blood glucose, and right-sided infarct as predictors of poor outcome. CONCLUSIONS: NXY-059 is ineffective for treatment of AIS within 6 hours of symptom onset. This is also true for subgroups and the prevention of alteplase-associated hemorrhage.
PY - 2008 SN - 1524-4628 (Electronic)0039-2499 (Linking) SP - 1751 EP - 8 T2 - Stroke TI - NXY-059 for the treatment of acute stroke: pooled analysis of the SAINT I and II Trials VL - 39 ER -