1,026 Experimental treatments in acute stroke

医学 临床试验 机制(生物学) 冲程(发动机) 范围(计算机科学) 重症监护医学 药品 急性中风 内科学 物理医学与康复 医学物理学 物理疗法 药理学 计算机科学 哲学 工程类 程序设计语言 认识论 组织纤溶酶原激活剂 机械工程
作者
Victoria O’Collins,Malcolm Macleod,Geoffrey A. Donnan,Laura L. Horky,Bart H. van der Worp,David W. Howells
出处
期刊:Annals of Neurology [Wiley]
卷期号:59 (3): 467-477 被引量:1406
标识
DOI:10.1002/ana.20741
摘要

Preclinical evaluation of neuroprotectants fostered high expectations of clinical efficacy. When not matched, the question arises whether experiments are poor indicators of clinical outcome or whether the best drugs were not taken forward to clinical trial. Therefore, we endeavored to contrast experimental efficacy and scope of testing of drugs used clinically and those tested only experimentally.We identified neuroprotectants and reports of experimental efficacy via a systematic search. Controlled in vivo and in vitro experiments using functional or histological end points were selected for analysis. Relationships between outcome, drug mechanism, scope of testing, and clinical trial status were assessed statistically.There was no evidence that drugs used clinically (114 drugs) were more effective experimentally than those tested only in animal models (912 drugs), for example, improvement in focal models averaged 31.3 +/- 16.7% versus 24.4 +/- 32.9%, p > 0.05, respectively. Scope of testing using Stroke Therapy Academic Industry Roundtable (STAIR) criteria was highly variable, and no relationship was found between mechanism and efficacy.The results question whether the most efficacious drugs are being selected for stroke clinical trials. This may partially explain the slow progress in developing treatments. Greater rigor in the conduct, reporting, and analysis of animal data will improve the transition of scientific advances from bench to bedside.
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