Donnan G A, Davis S M, Chambers B R, Gates P C, Hankey G J, McNeil J J, Rosen D, Stewart-Wynne E G, Tuck R R
Austin and Repatriation Medical Centre, Heidelberg, Victoria, Australia.
JAMA. 1996 Sep 25;276(12):961-6.
To determine whether the administration of 1.5 million units of streptokinase intravenously within 4 hours of the onset of acute ischemic stroke would reduce morbidity and mortality at 3 months and whether outcomes may be better for those receiving therapy within 3 hours of stroke onset compared with those receiving it after 3 hours.
Randomized, double-blind, placebo-controlled trial with 3-month follow-up.
A total of 340 patients, aged 18 to 85 years, with moderate to severe strokes were randomized from 40 centers throughout Australia from June 1992 to November 1994.
Administration of 1.5 million units of streptokinase or placebo intravenously in 100 mL of normal saline over 1 hour.
Combined death and disability score (Barthel index <60) 3 months after the stroke.
Using an intention-to-treat analysis with a combined death and disability score at 3 months after stroke as the primary end point, we found a nonsignificant overall trend toward unfavorable outcomes for streptokinase vs placebo (relative risk [RR] of unfavorable outcome, 1.08; 95% confidence interval [CI], 0.74-1.58) and an excess of hematomas (13.2%[12.6% symptomatic] in the treated group, 3% [2.4% symptomatic] for placebo [P<.01]). However, poor outcomes were confined to patients receiving therapy more than 3 hours after stroke onset (RR of unfavorable outcome, 1.22; 95% CI, 0.80-1.86). In contrast, among the 70 patients who were entered into the trial within 3 hours of stroke onset, there was a trend toward improved outcomes for those who received streptokinase (RR of unfavorable outcome, 0.66; 95% CI, 0.28-1.58), and this outcome pattern was significantly better than for those receiving therapy after 3 hours (P=.04). Streptokinase administration resulted in excess deaths in the group treated after 3 hours (RR, 1.98; 95% CI, 1.18-3.35), but not among those treated within 3 hours (RR, 1.11; 95% CI, 0.38-3.21).
The administration of streptokinase within 4 hours of acute ischemic stroke increased morbidity and mortality at 3 months. While treatment within 3 hours of stroke was safer and associated with significantly better outcomes than later treatment, it showed no significant benefit over placebo. The timing of thrombolytic therapy for acute stroke is critical.
确定在急性缺血性卒中发病4小时内静脉注射150万单位链激酶是否会降低3个月时的发病率和死亡率,以及与卒中发病3小时后接受治疗的患者相比,卒中发病3小时内接受治疗的患者预后是否更好。
随机、双盲、安慰剂对照试验,随访3个月。
1992年6月至1994年11月期间,来自澳大利亚各地40个中心的340例年龄在18至85岁之间的中重度卒中患者被随机分组。
在1小时内将150万单位链激酶或安慰剂加入100 mL生理盐水中静脉注射。
卒中后3个月时的死亡和残疾综合评分(Barthel指数<60)。
以卒中后3个月时的死亡和残疾综合评分为主要终点进行意向性分析,我们发现链激酶组与安慰剂组相比,总体上有不良结局的趋势但无统计学意义(不良结局的相对风险[RR]为1.08;95%置信区间[CI]为0.74 - 1.58),且血肿发生率更高(治疗组为13.2%[有症状的为12.6%],安慰剂组为3%[有症状的为2.4%][P<0.01])。然而,不良结局仅限于卒中发病3小时后接受治疗的患者(不良结局的RR为1.22;95%CI为0.80 - 1.86)。相比之下,在卒中发病3小时内纳入试验的70例患者中,接受链激酶治疗的患者有预后改善的趋势(不良结局的RR为0.66;95%CI为0.28 - 1.58),且这种结局模式明显优于3小时后接受治疗的患者(P = 0.04)。链激酶治疗导致3小时后治疗组死亡人数增加(RR为1.98;95%CI为1.18 - 3.35),但3小时内治疗的患者中未出现这种情况(RR为1.11;95%CI为0.38 - 3.21)。
急性缺血性卒中发病4小时内使用链激酶会增加3个月时的发病率和死亡率。虽然卒中发病3小时内治疗比更晚治疗更安全且结局明显更好,但与安慰剂相比无显著益处。急性卒中溶栓治疗的时机至关重要。
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