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急性缺血性卒中伴极早期临床改善:美国国立神经疾病和卒中研究所重组组织型纤溶酶原激活剂卒中试验的探索性分析。

Acute Ischemic Stroke with Very Early Clinical Improvement: A National Institute of Neurological Disorders and Stroke Recombinant Tissue Plasminogen Activator Stroke Trials Exploratory Analysis.

作者信息

Balucani Clotilde, Levine Steven R, Khoury Jane C, Khatri Pooja, Saver Jeffrey L, Broderick Joseph P

机构信息

Downstate Medical Center, The State University of New York, Brooklyn, New York.

Downstate Medical Center, The State University of New York, Brooklyn, New York; Departments of Neurology and Emergency Medicine, Kings County Medical Center, Brooklyn, New York.

出版信息

J Stroke Cerebrovasc Dis. 2016 Apr;25(4):894-901. doi: 10.1016/j.jstrokecerebrovasdis.2015.10.028. Epub 2016 Jan 26.

Abstract

BACKGROUND

A high proportion of patients excluded from recombinant tissue plasminogen activator (rt-PA) treatment because of rapid improvement occurring before treatment decision had incomplete recovery. The National Institute of Neurological Disorders and Stroke (NINDS) rt-PA Stroke Trials dataset allows for systematic analyses of very early postrandomization improvement (VEPRIM) in stroke severity as a National Institutes of Health Stroke Scale (NIHSS) score was available for all subjects enrolled in the study at baseline (NIHSSB) and at 2 hours after randomization (NIHSS2H). We explored various definitions of VEPRIM to characterize predictive values for clinical outcomes.

METHODS

Post hoc analyses of the NINDS rt-PA Stroke Trials were conducted. VEPRIM was defined as the difference between the NIHSSB and the NIHSS2H scores using 3 approaches: raw, percent, and normalized change. We assessed the association between VEPRIM and 3-month favorable outcome (mRS score of 0-1), symptomatic intracerebral hemorrhage (sICH), and death.

RESULTS

In the 624 subjects, every VEPRIM definition was independently associated with an increased probability of favorable outcome: for each unit of change within the VEPRIM definitions, there were 2%-24% (all P < .05) relative increased probability of favorable outcome, 2%-15% (all P < .05) decreased likelihood of death, and 2%-13% (all P < .05) decreased likelihood of sICH. Adjusting for NIHSSB and prestroke mRS scores, there was a significant rt-PA treatment effect for improvement seen for all 3 VEPRIM definitions.

CONCLUSIONS

VEPRIM predicted favorable outcomes independent of definition and treatment arm. Patients with VEPRIM by any definition, while doing better than patients without VEPRIM, also derived increased clinical benefit when treated with rt-PA compared to placebo. Even with VEPRIM, a substantial percentage of patients had unfavorable outcomes.

摘要

背景

由于在做出治疗决策之前病情迅速改善,有很大一部分患者被排除在重组组织型纤溶酶原激活剂(rt-PA)治疗之外,且恢复不完全。美国国立神经疾病与中风研究所(NINDS)rt-PA 中风试验数据集允许对中风严重程度的极早期随机化后改善情况(VEPRIM)进行系统分析,因为在基线时(NIHSSB)和随机化后 2 小时(NIHSS2H),该研究纳入的所有受试者均有美国国立卫生研究院中风量表(NIHSS)评分。我们探讨了 VEPRIM 的各种定义,以确定其对临床结局的预测价值。

方法

对 NINDS rt-PA 中风试验进行事后分析。使用 3 种方法将 VEPRIM 定义为 NIHSSB 与 NIHSS2H 评分之间的差值:原始变化、百分比变化和标准化变化。我们评估了 VEPRIM 与 3 个月时良好结局(改良 Rankin 量表[mRS]评分为 0 - 1)、症状性脑出血(sICH)和死亡之间的关联。

结果

在 624 名受试者中,每种 VEPRIM 定义均与良好结局的概率增加独立相关:在 VEPRIM 定义范围内,每变化一个单位,良好结局的相对概率增加 2% - 24%(所有 P < 0.05);死亡可能性降低 2% - 15%(所有 P < 0.05);sICH 可能性降低 2% - 13%(所有 P < 0.05)。在调整了 NIHSSB 和中风前 mRS 评分后,对于所有 3 种 VEPRIM 定义,均观察到 rt-PA 治疗对改善有显著效果。

结论

VEPRIM 可预测良好结局,且与定义和治疗组无关。无论采用何种定义,有 VEPRIM 的患者不仅比没有 VEPRIM 的患者情况更好;与安慰剂相比,接受 rt-PA 治疗时,他们还能获得更大的临床益处。即使有 VEPRIM,仍有相当比例的患者结局不佳。

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