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Diving into drug-screening: zebrafish embryos as an in vivo platform for antimicrobial drug discovery and assessment

机译:深入研究药物筛选:斑马鱼胚胎作为抗菌药物发现和评估的体内平台

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摘要

The rise of multidrug-resistant bacteria underlines the need for innovative treatments, yet the introduction of new drugs has stagnated despite numerous antimicrobial discoveries. A major hurdle is a poor correlation between promising in vitro data and in vivo efficacy in animal models, which is essential for clinical development. Early in vivo testing is hindered by the expense and complexity of existing animal models. Therefore, there is a pressing need for cost-effective, rapid preclinical models with high translational value. To overcome these challenges, zebrafish embryos have emerged as an attractive model for infectious disease studies, offering advantages such as ethical alignment, rapid development, ease of maintenance, and genetic manipulability. The zebrafish embryo infection model, involving microinjection or immersion of pathogens and potential antibiotic hit compounds, provides a promising solution for early-stage drug screening. It offers a cost-effective and rapid means of assessing the efficacy, toxicity and mechanism of action of compounds in a whole-organism context. This review discusses the experimental design of this model, but also its benefits and challenges. Additionally, it highlights recently identified compounds in the zebrafish embryo infection model and discusses the relevance of the model in predicting the compound’s clinical potential.
机译:多重耐药细菌的兴起凸显了对创新疗法的需求,但尽管有许多抗菌发现,但新药的引入却停滞不前。一个主要障碍是有前景的体外数据与动物模型中的体内疗效之间的相关性差,这对于临床开发至关重要。早期体内测试受到现有动物模型的费用和复杂性的阻碍。因此,迫切需要具有高转化价值的成本效益、快速的临床前模型。为了克服这些挑战,斑马鱼胚胎已成为传染病研究的一种有吸引力的模型,具有伦理一致性、快速发育、易于维护和遗传可操作性等优势。斑马鱼胚胎感染模型涉及病原体和潜在抗生素苗头化合物的显微注射或浸泡,为早期药物筛选提供了一个有前途的解决方案。它提供了一种经济高效且快速的方法,用于评估化合物在整个生物体环境中的功效、毒性和作用机制。本文讨论了该模型的实验设计,以及其优点和挑战。此外,它还强调了斑马鱼胚胎感染模型中最近发现的化合物,并讨论了该模型在预测化合物临床潜力方面的相关性。

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