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烷基-克来烯和烷基-苯并[a]蒽对日本青鳉鱼胚胎慢性毒性的定量构效关系。

Quantitative structure-activity relationships for chronic toxicity of alkyl-chrysenes and alkyl-benz[a]anthracenes to Japanese medaka embryos (Oryzias latipes).

机构信息

Department of Biology, Queen's University, Kingston, Ontario K7L3N6, Canada.

School of Environmental Studies, Queen's University, Kingston, Ontario K7L3N6, Canada.

出版信息

Aquat Toxicol. 2015 Feb;159:109-18. doi: 10.1016/j.aquatox.2014.11.027. Epub 2014 Dec 5.

Abstract

Alkylated polycyclic aromatic hydrocarbons (alkyl-PAHs) are a class of compounds found at significant concentrations in crude oils, and likely the main constituents responsible for the chronic toxicity of oil to fish. Alkyl substituents at different locations on the aromatic rings change the size and shape of PAH molecules, which results in different interactions with tissue receptors and different severities of toxicity. The present study is the first to report the toxicity of several alkylated derivatives of chrysene and benz[a]anthracene to the embryos of Japanese medaka (Oryzias latipes) using the partition controlled delivery (PCD) method of exposure. The PCD method maintained the desired exposure concentrations by equilibrium partitioning of hydrophobic test compounds from polydimethylsiloxane (PDMS) films. Test concentrations declined by only 13% over a period of 17 days. Based on the prevalence of signs of blue sac disease (BSD), as expressed by median effective concentrations (EC50s), benz[a]anthracene (B[a]A) was more toxic than chrysene. Alkylation generally increased toxicity, except at position 2 of B[a]A. Alkyl-PAHs substituted in the middle region had a lower EC50 than those substituted at the distal region. Except for B[a]A and 7-methylbenz[a]anthracene (7-MB), estimated EC50 values were higher than their solubility limits, which resulted in limited toxicity within the range of test concentrations. The regression between log EC50s and logKow values provided a rough estimation of structure-activity relationships for alkyl-PAHs, but Kow alone did not provide a complete explanation of the chronic toxicity of alkyl PAHs.

摘要

烷基多环芳烃(alkyl-PAHs)是一类在原油中浓度较高的化合物,可能是导致鱼类慢性毒性的主要成分。芳香环上不同位置的烷基取代基改变了 PAH 分子的大小和形状,导致与组织受体的不同相互作用和不同程度的毒性。本研究首次报道了几种苊和苯并[a]蒽的烷基衍生物对日本青鳉(Oryzias latipes)胚胎的毒性,使用的是分区控制释放(PCD)暴露方法。PCD 方法通过从聚二甲基硅氧烷(PDMS)薄膜中平衡分配疏水性测试化合物来维持所需的暴露浓度。在 17 天的时间内,测试浓度仅下降了 13%。基于蓝囊病(BSD)症状的普遍出现率(以中位有效浓度(EC50)表示),苯并[a]蒽(B[a]A)比苊更具毒性。烷基化通常会增加毒性,但 B[a]A 的 2 位除外。位于中间区域的烷基取代的多环芳烃的 EC50 低于位于远端区域的烷基取代的多环芳烃。除了 B[a]A 和 7-甲基苯并[a]蒽(7-MB)之外,估计的 EC50 值高于其溶解度极限,这导致在测试浓度范围内毒性有限。log EC50 值与 logKow 值之间的回归提供了对烷基多环芳烃结构-活性关系的粗略估计,但 Kow 本身并不能完全解释烷基多环芳烃的慢性毒性。

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