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Testing the Translational Power of the Zebrafish: An Interspecies Analysis of Responses to Cardiovascular Drugs

机译:测试斑马鱼的翻译能力:对心血管药物反应的种间分析。

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摘要

The zebrafish is rapidly emerging as a promising alternative in vivo model for the detection of drug-induced cardiovascular effects. Despite its increasing popularity, the ability of this model to inform the drug development process is often limited by the uncertainties around the quantitative relevance of zebrafish responses compared with nonclinical mammalian species and ultimately humans. In this test of concept study, we provide a comparative quantitative analysis of the in vivo cardiovascular responses of zebrafish, rat, dog, and human to three model compounds (propranolol, losartan, and captopril), which act as modulators of two key systems (beta-adrenergic and renin–angiotensin systems) involved in the regulation of cardiovascular functions. We used in vivo imaging techniques to generate novel experimental data of drug-mediated cardiovascular effects in zebrafish larvae. These data were combined with a database of interspecies mammalian responses (i.e., heart rate, blood flow, vessel diameter, and stroke volume) extracted from the literature to perform a meta-analysis of effect size and direction across multiple species. In spite of the high heterogeneity of study design parameters, our analysis highlighted that zebrafish and human responses were largely comparable in >80% of drug/endpoint combinations. However, it also revealed a high intraspecies variability, which, in some cases, prevented a conclusive interpretation of the drug-induced effect. Despite the shortcomings of our study, the meta-analysis approach, combined with a suitable data visualization strategy, enabled us to observe patterns of response that would likely remain undetected with more traditional methods of qualitative comparative analysis. We propose that expanding this approach to larger datasets encompassing multiple drugs and modes of action would enable a rigorous and systematic assessment of the applicability domain of the zebrafish from both a mechanistic and phenotypic standpoint. This will increase the confidence in its application for the early detection of adverse drug reactions in any major organ system.
机译:斑马鱼正迅速成为一种有前途的替代体内模型,用于检测药物诱发的心血管效应。尽管该模型越来越受欢迎,但与非临床哺乳动物物种以及最终人类相比,该模型在药物开发过程中提供信息的能力通常受到斑马鱼反应定量相关性不确定性的限制。在这项概念研究测试中,我们提供了斑马鱼,大鼠,狗和人对三种模型化合物(普萘洛尔,氯沙坦和卡托普利)的体内心血管反应的比较定量分析,这三种化合物是两个关键系统的调节剂( β-肾上腺素和肾素-血管紧张素系统)参与心血管功能的调节。我们使用体内成像技术来产生药物介导的斑马鱼幼虫心血管效应的新实验数据。这些数据与从文献中提取的种间哺乳动物反应(即心率,血流量,血管直径和中风量)的数据库相结合,以对多种物种的效应大小和方向进行荟萃分析。尽管研究设计参数存在高度异质性,但我们的分析强调,斑马鱼和人类的反应在80%以上的药物/终点组合中可比。但是,它也显示出种内的高度变异性,在某些情况下,这无法最终解释药物诱导的作用。尽管我们的研究存在缺陷,但荟萃分析方法与合适的数据可视化策略相结合,使我们能够观察到响应模式,而用传统的定性比较分析方法可能无法发现这些响应模式。我们建议将这种方法扩展到包含多种药物和作用方式的更大数据集,将能够从机理和表型的角度对斑马鱼的适用范围进行严格而系统的评估。这将增加其在任何主要器官系统中早期发现药物不良反应的应用的信心。

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