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应用秀丽隐杆线虫(线虫)和斑马鱼胚胎(斑马鱼)作为模型系统筛选哌嗪类化合物的发育毒性和生殖毒性。

Application of Caenorhabditis elegans (nematode) and Danio rerio embryo (zebrafish) as model systems to screen for developmental and reproductive toxicity of Piperazine compounds.

机构信息

ZF-screens BV, J.H. Oortweg 19, 2333 CH Leiden, The Netherlands.

University of Applied Sciences Utrecht, Heidelberglaan 7, 3584 CS Utrecht, The Netherlands.

出版信息

Toxicol In Vitro. 2017 Oct;44:11-16. doi: 10.1016/j.tiv.2017.06.002. Epub 2017 Jun 26.

Abstract

To enable selection of novel chemicals for new processes, there is a recognized need for alternative toxicity screening assays to assess potential risks to man and the environment. For human health hazard assessment these screening assays need to be translational to humans, have high throughput capability, and from an animal welfare perspective be harmonized with the principles of the 3Rs (Reduction, Refinement, Replacement). In the area of toxicology a number of cell culture systems are available but while these have some predictive value, they are not ideally suited for the prediction of developmental and reproductive toxicology (DART). This is because they often lack biotransformation capacity, multicellular or multi- organ complexity, for example, the hypothalamus pituitary gonad (HPG) axis and the complete life cycle of whole organisms. To try to overcome some of these limitations in this study, we have used Caenorhabditis elegans (nematode) and Danio rerio embryos (zebrafish) as alternative assays for DART hazard assessment of some candidate chemicals being considered for a new commercial application. Nematodes exposed to Piperazine and one of the analogs tested showed a slight delay in development compared to untreated animals but only at high concentrations and with Piperazine as the most sensitive compound. Total brood size of the nematodes was also reduced primarily by Piperazine and one of the analogs. In zebrafish Piperazine and analogs showed developmental delays. Malformations and mortality in individual fish were also scored. Significant malformations were most sensitively identified with Piperazine, significant mortality was only observed in Piperazine and only at the higest dose. Thus, Piperazine seemed the most toxic compound for both nematodes and zebrafish. The results of the nematode and zebrafish studies were in alignment with data obtained from conventional mammalian toxicity studies indicating that these have potential as developmental toxicity screening systems. The results of these studies also provided reassurance that none of the Piperazines tested are likely to have any significant developmental and/or reproductive toxicity issues to humans when used in their commercial applications.

摘要

为了能够选择新型化学物质用于新工艺,人们认识到需要替代毒性筛选检测方法来评估对人类和环境的潜在风险。对于人类健康危害评估,这些筛选检测方法需要具有向人类转化的能力、高通量能力,并且从动物福利的角度来看,需要与 3R(减少、优化、替代)原则相协调。在毒理学领域,有许多可用的细胞培养系统,但尽管这些系统具有一定的预测价值,但它们并不完全适合发育和生殖毒理学(DART)的预测。这是因为它们通常缺乏生物转化能力、多细胞或多器官的复杂性,例如下丘脑-垂体-性腺(HPG)轴和整个生物体的完整生命周期。为了尝试克服这些局限性,我们使用秀丽隐杆线虫(线虫)和斑马鱼胚胎(斑马鱼)作为一些候选化学物质的 DART 危害评估的替代检测方法,这些候选化学物质正在考虑用于新的商业应用。与未处理的动物相比,暴露于哌嗪和测试的一种类似物的线虫的发育稍有延迟,但仅在高浓度下,哌嗪是最敏感的化合物。线虫的总产卵量也主要受到哌嗪和一种类似物的影响。在斑马鱼中,哌嗪和类似物显示出发育延迟。还对个体鱼的畸形和死亡率进行了评分。哌嗪最能敏感地识别出明显的畸形,仅在哌嗪和最高剂量下观察到明显的死亡率。因此,哌嗪似乎对线虫和斑马鱼都是最有毒的化合物。线虫和斑马鱼研究的结果与从常规哺乳动物毒性研究中获得的数据一致,表明这些方法具有作为发育毒性筛选系统的潜力。这些研究的结果还保证了在其商业应用中,测试的哌嗪类化合物都不太可能对人类产生任何重大的发育和/或生殖毒性问题。

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