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首页> 外文期刊>SAR and QSAR in Environmental Research >The physicochemical basis of QSARs for baseline toxicity.
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The physicochemical basis of QSARs for baseline toxicity.

机译:QSARs基线毒性的理化基础。

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摘要

The physico-chemical properties relevant to the equilibrium partitioning (bioconcentration) of chemicals between organisms and their respired media of water and air are reviewed and illustrated for chemicals that range in hydrophobicity. Relationships are then explored between freely dissolved external concentrations such as LC50s and chemical properties for one important toxicity mechanism, namely baseline toxicity or narcosis. The 'activity hypothesis' proposed by Ferguson in 1939 provides a coherent and compelling explanation for baseline toxicity of chemicals in both water- and air-respiring organisms, as well as a reference point for identifying more specific toxicity pathways. From inhalation studies with fish and rodents, narcosis is shown to occur at a chemical activity exceeding approximately 0.01 and there is no evidence of narcosis at activities less than 0.001. The activity hypothesis provides a framework for directly comparing the toxic potency of chemicals in both air- and water-breathing animals. The activity hypothesis is shown to be consistent with the critical body residue concept, but it has the advantage of avoiding the confounding effect of lipid content of the test organism. It also provides a theoretically sound basis for assessing the baseline toxicity of mixtures. It is suggested that since activity is readily calculated from fugacity, observed or predicted environmental abiotic and biotic fugacities can be used to evaluate the potential for baseline toxicity. Further, models employing fugacity or activity can be used to improve the experimental design of bioassays, thus possibly reducing unnecessary animal testing.
机译:对于在疏水性范围内的化学物质,对与生物体及其呼吸的水和空气介质之间的化学物质的平衡分配(生物浓度)相关的理化性质进行了说明。然后研究了一种重要的毒性机制(即基线毒性或麻醉)的自由溶解的外部浓度(例如LC50)与化学性质之间的关系。弗格森(Ferguson)在1939年提出的“活性假说”为水和空气呼吸生物中化学物质的基线毒性提供了连贯且令人信服的解释,同时也是确定更具体的毒性途径的参考点。从鱼类和啮齿动物的吸入研究中,可以发现,化学活性超过约0.01时会发生麻醉,而活性低于0.001时则没有麻醉的迹象。活性假说提供了一个框架,可以直接比较空气呼吸动物和水呼吸动物中化学物质的毒性。活性假说被证明与关键的身体残留概念相一致,但是它具有避免测试生物的脂质含量混杂影响的优点。它还为评估混合物的基线毒性提供了理论上可靠的基础。有人建议,由于可以很容易地从逸度计算出活性,因此可以将观察到或预测的环境非生物和生物逸度用于评估基线毒性的可能性。此外,采用逸度或活性的模型可用于改进生物测定的实验设计,从而可能减少不必要的动物测试。

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