University Department of Medicine and Therapeutics, Gardiner Institute, Western Infirmary and Faculty of Medicine, University of Glasgow, Glasgow G116NT, UK.
Stroke. 2010 Jan;41(1):e25-33. doi: 10.1161/STROKEAHA.109.566869. Epub 2009 Nov 19.
Clinical benefit from thrombolysis is reduced as stroke onset to treatment time increases. The use of "mismatch" imaging to identify patients for delayed treatment has face validity and has been used in case series and clinical trials. We undertook a meta-analysis of relevant trials to examine whether present evidence supports delayed thrombolysis among patients selected according to mismatch criteria.
We collated outcome data for patients who were enrolled after 3 hours of stroke onset in thrombolysis trials and had mismatch on pretreatment imaging. We selected the trials on the basis of a systematic search of the Web of Knowledge. We compared favorable outcome, reperfusion and/or recanalization, mortality, and symptomatic intracerebral hemorrhage between the thrombolyzed and nonthrombolyzed groups of patients and the probability of a favorable outcome among patients with successful reperfusion and clinical findings for 3 to 6 versus 6 to 9 hours from poststroke onset. Results are expressed as adjusted odds ratios (a-ORs) with 95% CIs. Heterogeneity was explored by test statistics for clinical heterogeneity, I(2) (inconsistency), and L'Abbé plot.
We identified articles describing the DIAS, DIAS II, DEDAS, DEFUSE, and EPITHET trials, giving a total of 502 mismatch patients thrombolyzed beyond 3 hours. The combined a-ORs for favorable outcomes were greater for patients who had successful reperfusion (a-OR=5.2; 95% CI, 3 to 9; I(2)=0%). Favorable clinical outcome was not significantly improved by thrombolysis (a-OR=1.3; 95% CI, 0.8 to 2.0; I(2)=20.9%). Odds for reperfusion/recanalization were increased among patients who received thrombolytic therapy (a-OR=3.0; 95% CI, 1.6 to 5.8; I(2)=25.7%). The combined data showed a significant increase in mortality after thrombolysis (a-OR=2.4; 95% CI, 1.2 to 4.9; I(2)=0%), but this was not confirmed when we excluded data from desmoteplase doses that were abandoned in clinical development (a-OR=1.6; 95% CI, 0.7 to 3.7; I(2)=0%). Symptomatic intracerebral hemorrhage was significantly increased after thrombolysis (a-OR=6.5; 95% CI, 1.2 to 35.4; I(2)=0%) but not significant after exclusion of abandoned doses of desmoteplase (a-OR=5.4; 95% CI, 0.9 to 31.8; I(2)=0%).
Delayed thrombolysis amongst patients selected according to mismatch imaging is associated with increased reperfusion/recanalization. Recanalization/reperfusion is associated with improved outcomes. However, delayed thrombolysis in mismatch patients was not confirmed to improve clinical outcome, although a useful clinical benefit remains possible. Thrombolysis carries a significant risk of symptomatic intracerebral hemorrhage and possibly increased mortality. Criteria to diagnose mismatch are still evolving. Validation of the mismatch selection paradigm is required with a phase III trial. Pending these results, delayed treatment, even according to mismatch selection, cannot be recommended as part of routine care.
随着脑卒中发病至治疗时间的延长,溶栓治疗的临床获益降低。利用“不匹配”影像来识别适合延迟治疗的患者具有表面有效性,已经在病例系列研究和临床试验中得到应用。我们对相关试验进行了荟萃分析,以评估根据不匹配标准选择的患者接受延迟溶栓治疗是否有现有证据支持。
我们汇总了在溶栓试验中发病 3 小时后入组且预处理影像存在不匹配的患者的结局数据。我们通过系统搜索 Web of Knowledge 来选择试验。我们比较了溶栓和未溶栓患者的良好结局、再灌注和/或再通、死亡率和症状性颅内出血,以及再灌注成功患者的良好结局概率和发病后 3 至 6 小时与 6 至 9 小时的临床发现。结果表示为调整后的优势比(a-OR)及其 95%置信区间(CI)。通过临床异质性检验统计量、I(2)(不一致性)和 L'Abbé 图来探索异质性。
我们确定了描述 DIAS、DIAS II、DEDAS、DEFUSE 和 EPITHET 试验的文章,共纳入 502 例发病超过 3 小时后接受溶栓治疗的不匹配患者。再灌注成功患者的联合 a-OR 更高(a-OR=5.2;95%CI,3 至 9;I(2)=0%)。溶栓治疗并未显著改善临床结局(a-OR=1.3;95%CI,0.8 至 2.0;I(2)=20.9%)。接受溶栓治疗的患者再灌注/再通的可能性更高(a-OR=3.0;95%CI,1.6 至 5.8;I(2)=25.7%)。合并数据显示溶栓治疗后死亡率显著增加(a-OR=2.4;95%CI,1.2 至 4.9;I(2)=0%),但当排除在临床开发中被放弃的地塞米松剂量数据时,这一结果并不成立(a-OR=1.6;95%CI,0.7 至 3.7;I(2)=0%)。溶栓治疗后症状性颅内出血显著增加(a-OR=6.5;95%CI,1.2 至 35.4;I(2)=0%),但排除地塞米松剂量数据后,这一结果并不显著(a-OR=5.4;95%CI,0.9 至 31.8;I(2)=0%)。
根据不匹配影像选择的延迟溶栓治疗与再灌注/再通增加相关。再灌注/再通与改善结局相关。然而,延迟溶栓治疗并不能改善不匹配患者的临床结局,尽管仍可能存在有益的临床获益。溶栓治疗存在明显的症状性颅内出血风险,可能增加死亡率。诊断不匹配的标准仍在不断发展。需要进行 III 期试验来验证不匹配选择的合理性。在这些结果公布之前,不能推荐根据不匹配选择进行延迟治疗,即使是延迟治疗也不能作为常规治疗的一部分。
