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优化大型动物 MI 模型;对临床前研究对照组的系统分析。

Optimization of large animal MI models; a systematic analysis of control groups from preclinical studies.

机构信息

Department of Cardiology, University Medical Center Utrecht, Utrecht, The Netherlands.

Center for Clinical Brain Sciences, University of Edinburgh, Edinburgh, United Kingdom.

出版信息

Sci Rep. 2017 Oct 27;7(1):14218. doi: 10.1038/s41598-017-14294-z.

Abstract

Large animal models are essential for the development of novel therapeutics for myocardial infarction. To optimize translation, we need to assess the effect of experimental design on disease outcome and model experimental design to resemble the clinical course of MI. The aim of this study is therefore to systematically investigate how experimental decisions affect outcome measurements in large animal MI models. We used control animal-data from two independent meta-analyses of large animal MI models. All variables of interest were pre-defined. We performed univariable and multivariable meta-regression to analyze whether these variables influenced infarct size and ejection fraction. Our analyses incorporated 246 relevant studies. Multivariable meta-regression revealed that infarct size and cardiac function were influenced independently by choice of species, sex, co-medication, occlusion type, occluded vessel, quantification method, ischemia duration and follow-up duration. We provide strong systematic evidence that commonly used endpoints significantly depend on study design and biological variation. This makes direct comparison of different study-results difficult and calls for standardized models. Researchers should take this into account when designing large animal studies to most closely mimic the clinical course of MI and enable translational success.

摘要

大型动物模型对于开发心肌梗死的新型治疗方法至关重要。为了优化转化,我们需要评估实验设计对疾病结果的影响,并将模型实验设计与 MI 的临床过程相似。因此,本研究旨在系统地研究实验决策如何影响大型动物 MI 模型中的结果测量。我们使用了两个大型动物 MI 模型的独立荟萃分析的对照动物数据。所有感兴趣的变量均预先定义。我们进行了单变量和多变量荟萃回归分析,以分析这些变量是否影响梗死面积和射血分数。我们的分析纳入了 246 项相关研究。多变量荟萃回归显示,梗死面积和心功能独立受到物种选择、性别、合并用药、闭塞类型、闭塞血管、定量方法、缺血持续时间和随访持续时间的影响。我们提供了强有力的系统证据,表明常用终点显著取决于研究设计和生物学变异性。这使得不同研究结果的直接比较变得困难,并呼吁采用标准化模型。研究人员在设计大型动物研究时应考虑到这一点,以最接近地模拟 MI 的临床过程并实现转化成功。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4ffc/5660150/47a191af5a29/41598_2017_14294_Fig1_HTML.jpg

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