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Adverse Outcome Pathways during Early Fish Development: A Conceptual Framework for Identification of Chemical Screening and Prioritization Strategies

机译:鱼类早期发育过程中的不利结果途径:化学筛选和优先策略识别的概念框架

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摘要

The fish early life-stage (FELS) test guideline (OECD 210 or OCSPP 850.1400) is the most frequently used bioassay for predicting chronic fish toxicity and supporting aquatic ecological risk assessments around the world. For each chemical, the FELS test requires a minimum of 360 fish and 1 to 3 months from test initiation to termination. Although valuable for predicting fish full life-cycle toxicity, FELS tests are labor and resource intensive and, due to an emphasis on apical endpoints, provide little to no information about chemical mode of action. Therefore, the development and implementation of alternative testing strategies for screening and prioritizing chemicals has the potential to reduce the cost and number of animals required for estimating FELS toxicity and, at the same time, provides insights into mechanisms of toxicity. Using three reference chemicals with well-established yet distinct adverse outcome pathways (AOPs) in early life stages of fish, we proposed FELS-specific AOPs as conceptual frameworks for identifying useful chemical screening and prioritization strategies. The reference chemicals selected as case studies were a cardiotoxic aryl hydrocarbon receptor agonist (2,3,7,8-tetrachlorodibenzo-p-dioxin), neurotoxic acetylcholinesterase inhibitor (chlorpyrifos), and narcotic surfactant (linear alkylbenzene sulfonate). Using qualitative descriptions for each chemical during early fish development, we developed generalized AOPs and, based on these examples, proposed a three-tiered testing strategy for screening and prioritizing chemicals for FELS testing. Linked with biologically based concentration-response models, a tiered testing strategy may help reduce the reliance on long-term and costly FELS tests required for assessing the hazard of thousands of chemicals currently in commerce
机译:鱼类早期生命阶段(FELS)测试指南(OECD 210或OCSPP 850.1400)是用于预测鱼类慢性毒性和支持全球水生生态风险评估的最常用生物测定法。对于每种化学品,FELS测试至少需要360条鱼,并且从测试开始到终止至少需要1-3个月。尽管FELS测试对于预测鱼类整个生命周期的毒性很有价值,但它是劳动和资源密集型测试,并且由于强调根尖,因此几乎没有提供关于化学作用方式的信息。因此,开发和实施用于筛选和区分化学品优先级的替代测试策略,有可能降低估计FELS毒性所需的成本和动物数量,同时,还可以提供毒性机理的见解。我们在鱼类的生命早期阶段使用了三种具有完善但独特的不良结果途径(AOP)的参考化学品,我们提出了FELS特有的AOP作为概念框架,用于识别有用的化学品筛选和优先排序策略。作为案例研究选择的参考化学品是心脏毒性的芳烃受体激动剂(2,3,7,8-四氯二苯并-对-二恶英),神经毒性的乙酰胆碱酯酶抑制剂(毒死rif)和麻醉性表面活性剂(线性烷基苯磺酸盐)。通过在鱼类早期发育过程中使用每种化学物质的定性描述,我们开发了通用的AOP,并基于这些示例,提出了一种三层测试策略,用于筛选和优先考虑用于FELS测试的化学物质。与基于生物学的浓度响应模型相结合,分层测试策略可以帮助减少对评估目前市场上成千上万种化学品的危害所需的长期且昂贵的FELS测试的依赖

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