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Human neurospheres as three-dimensional cellular systems for developmental neurotoxicity testing.

机译:人类神经球作为用于发展性神经毒性测试的三维细胞系统。

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摘要

BACKGROUND: Developmental neurotoxicity (DNT) of environmental chemicals is a serious threat to human health. Current DNT testing guidelines propose investigations in rodents, which require large numbers of animals. With regard to the "3 Rs" (reduction, replacement, and refinement) of animal testing and the European regulation of chemicals [Registration, Evaluation, and Authorisation of Chemicals (REACH)], alternative testing strategies are needed in order to refine and reduce animal experiments and allow faster and less expensive screening. OBJECTIVES: The goal of this study was to establish a three-dimensional test system for DNT screening based on human fetal brain cells. METHODS: We established assays suitable for detecting disturbances in basic processes of brain development by employing human neural progenitor cells (hNPCs), which grow as neurospheres. Furthermore, we assessed effects of mercury and oxidative stress on these cells. RESULTS: We found that human neurospheres imitate proliferation, differentiation, and migration in vitro. Exposure to the proapoptotic agent staurosporine further suggests that human neurospheres possess functioning apoptosis machinery. The developmental neurotoxicants methylmercury chloride and mercury chloride decreased migration distance and number of neuronal-like cells in differentiated hNPCs. Furthermore, hNPCs undergo caspase-independent apoptosis when exposed toward high amounts of oxidative stress. CONCLUSIONS: Human neurospheres are likely to imitate basic processes of brain development, and these processes can be modulated by developmental neurotoxicants. Thus, this three-dimensional cell system is a promising approach for DNT testing.
机译:背景:环境化学物质的发育性神经毒性(DNT)对人类健康构成严重威胁。当前的DNT测试指南建议对需要大量动物的啮齿动物进行调查。关于动物测试的“ 3 Rs”(减少,替换和完善)和欧洲化学品法规[化学品的注册,评估和授权(REACH)],需要其他测试策略以完善和减少动物实验,可以更快,更便宜地进行筛查。目的:本研究的目的是建立基于人类胎儿脑细胞的三维DNT筛查测试系统。方法:我们建立了适用于通过使用作为神经球生长的人类神经祖细胞(hNPC)来检测大脑发育基本过程中的障碍的检测方法。此外,我们评估了汞和氧化应激对这些细胞的影响。结果:我们发现人类神经球在体外模拟增殖,分化和迁移。暴露于促凋亡剂星形孢菌素进一步表明人神经球具有功能性凋亡机制。发育中的神经毒物氯化甲基汞和氯化汞减少了分化的hNPC中的迁移距离和神经元样细胞的数量。此外,hNPCs暴露于大量的氧化应激时会经历caspase独立的凋亡。结论:人的神经球很可能模仿大脑发育的基本过程,而这些过程可以被发育性神经毒性物质调节。因此,这种三维电池系统是用于DNT测试的有前途的方法。

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