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In vitro acute and developmental neurotoxicity screening: an overview of cellular platforms and high-throughput technical possibilities

机译:体外急性和发育神经毒性筛选:蜂窝平台概述和高通量技术可能性

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Neurotoxicity and developmental neurotoxicity are important issues of chemical hazard assessment. Since the interpretation of animal data and their extrapolation to man is challenging, and the amount of substances with information gaps exceeds present animal testing capacities, there is a big demand for in vitro tests to provide initial information and to prioritize for further evaluation. During the last decade, many in vitro tests emerged. These are based on animal cells, human tumour cell lines, primary cells, immortalized cell lines, embryonic stem cells, or induced pluripotent stem cells. They differ in their read-outs and range from simple viability assays to complex functional endpoints such as neural crest cell migration. Monitoring of toxicological effects on differentiation often requires multiomics approaches, while the acute disturbance of neuronal functions may be analysed by assessing electrophysiological features. Extrapolation from in vitro data to humans requires a deep understanding of the test system biology, of the endpoints used, and of the applicability domains of the tests. Moreover, it is important that these be combined in the right way to assess toxicity. Therefore, knowledge on the advantages and disadvantages of all cellular platforms, endpoints, and analytical methods is essential when establishing in vitro test systems for different aspects of neurotoxicity. The elements of a test, and their evaluation, are discussed here in the context of comprehensive prediction of potential hazardous effects of a compound. We summarize the main cellular characteristics underlying neurotoxicity, present an overview of cellular platforms and read-out combinations assessing distinct parts of acute and developmental neurotoxicology, and highlight especially the use of stem cell-based test systems to close gaps in the available battery of tests.
机译:神经毒性和发育神经毒性是化学危害评估的重要问题。由于动物数据的解释及其对人的外推具有挑战性,并且具有信息差距的物质量超过现有的动物测试能力,因此对体外测试有很大的需求,以提供初始信息并优先考虑进一步评估。在过去十年中,许多体外测试出现了。这些基于动物细胞,人肿瘤细胞系,原代细胞,永生化细胞系,胚胎干细胞或诱导多能干细胞。它们的读出和范围与简单的活力测定的范围不同,以复杂的功能终点,例如神经嵴细胞迁移。监测对差异化的毒理学效应通常需要多组合器方法,而通过评估电生理学特征,可以分析神经元功能的急性扰动。从体外数据到人类的外推需要深入了解测试系统生物学,所使用的终点和测试的适用性结构域。此外,重要的是这些以正确的方式组合来评估毒性。因此,关于为神经毒性的不同方面建立体外测试系统时,所有细胞平台,终点和分析方法的优缺点知识是必不可少的。这里的测试元素及其评价在这里讨论了化合物潜在危险效果的综合预测。我们总结了神经毒性的主要细胞特征,概述了细胞平台和评估急性和发育神经毒理学的不同部分的读出组合,并突出了干细胞的测试系统在可用的测试电池中关闭间隙。 。

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