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斑马鱼的行为神经科学:揭示大脑与行为关系的复杂性。

Behavioral neuroscience in zebrafish: unravelling the complexity of brain-behavior relationships.

机构信息

Department of Pharmacology, Calcutta Institute of Pharmaceutical Technology & AHS, Uluberia, Howrah, 711316, West Bengal, India.

P.G. Institute of Medical Sciences, Dhurabila, Dhamkuria, Paschim Medinipur: 72:1201, Chandrakona Town, West Bengal, India.

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 2024 Dec;397(12):9295-9313. doi: 10.1007/s00210-024-03275-5. Epub 2024 Jul 6.

Abstract

This paper reviews the utility of zebrafish (Danio rerio) as a model system for exploring neurobehavioral phenomena in preclinical research, focusing on physiological processes, disorders, and neurotoxicity biomarkers. A comprehensive review of the current literature was conducted to summarize the various behavioral characteristics of zebrafish. The study examined the etiological agents used to induce neurotoxicity and the biomarkers involved, including Aβ42, tau, MMP-13, MAO, NF-Кβ, and GFAP. Additionally, the different zebrafish study models and their responses to neurobehavioral analysis were discussed. The review identified several key biomarkers of neurotoxicity in zebrafish, each impacting different aspects of neurogenesis, inflammation, and neurodegeneration. Aβ42 was found to alter neuronal growth and stem cell function. Tau's interaction with tubulin affected microtubule stability and led to tauopathies under pathological conditions. MMP-13 was linked to oxidative assault and sensory neuron degeneration. MAO plays a role in neurotransmitter metabolism and neurotoxicity conversion. NF-Кβ was involved in pro-inflammatory pathways, and GFAP was indicative of neuroinflammation and astroglial activation. Zebrafish provide a valuable model for neurobehavioral research, adhering to the "3Rs" philosophy. Their neurotoxicity biomarkers offer insights into the mechanisms of neurogenesis, inflammation, and neurodegeneration. This model system aids in evaluating physiological and pathological conditions, enhancing our understanding of neurobehavioral phenomena and potential therapeutic interventions.

摘要

本文综述了斑马鱼(Danio rerio)作为一种模型系统在探索临床前研究中的神经行为现象的应用,重点介绍了生理过程、疾病和神经毒性生物标志物。对当前文献进行了全面综述,以总结斑马鱼的各种行为特征。该研究检查了用于诱导神经毒性的病因剂和涉及的生物标志物,包括 Aβ42、tau、MMP-13、MAO、NF-Кβ和 GFAP。此外,还讨论了不同的斑马鱼研究模型及其对神经行为分析的反应。该综述确定了斑马鱼神经毒性的几个关键生物标志物,每个标志物都影响神经发生、炎症和神经退行性变的不同方面。Aβ42 被发现改变神经元生长和干细胞功能。Tau 与微管蛋白的相互作用影响微管稳定性,并在病理条件下导致 tau 病。MMP-13 与氧化攻击有关,导致感觉神经元退化。MAO 参与神经递质代谢和神经毒性转化。NF-Кβ 参与促炎途径,GFAP 是神经炎症和星状胶质细胞激活的指标。斑马鱼为神经行为研究提供了有价值的模型,符合“3R”原则。它们的神经毒性生物标志物为神经发生、炎症和神经退行性变的机制提供了深入了解。该模型系统有助于评估生理和病理条件,增强我们对神经行为现象和潜在治疗干预措施的理解。

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