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Toxicokinetics of Polar Chemicals in Zebrafish Embryo (Danio rerio): Influence of Physicochemical Properties and of Biological Processes

机译:斑马鱼胚胎中的极性化学物质的毒代动力学(达尼奥·里约):理化性质和生物过程的影响。

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摘要

The time-resolved uptake of 17 nonionic and ionic polar compounds (logD ≤ 2) with a diversity of functional groups into zebrafish embryos (ZFE) was studied over 96 h of exposure. Among them were pharmaceuticals, pesticides and plant active ingredients. Uptake rates for the diffusion controlled passive uptake through the ZFE membrane ranged from 0.02 to 24 h~(-1) for the nonionic compounds and were slower for ionic compounds (<0.008-0.08 h~(-1)). The study compounds did not enrich much in the ZFE (median bioconcentration factor of 1, max. 7). Biotransformation significantly influenced the internal concentration of some of the test compounds over time (benzocaine, phenacetin, metribuzin, phenytoin, thiadoprid, valproic acid). For benzocaine, valproic acid and phenacetin several transformation products (TPs) were observed by LC-MS already at early life-stages (before 28 hpf); for benzocaine the TPs comprised >90% of the initial amount taken up into the ZFE. For six compounds internal concentrations remained very low (rel. int. conc. < 0.2). Besides biotransformation (sulfamethoxazole), poor membrane permeability (cimetidine, colchicine) and also affinity to efflux transporters (atropine and chloramphenicol) are the likely reasons for these low internal concentrations. This study outlines that the uptake of polar compounds into ZFE is influenced by their physicochemical properties. However, biological processes, biotransformation and, likely, efflux can strongly affect the internal concentrations already in early developmental stages of the ZFE. This should be considered in future toxicokinetic modeling. The evaluation of the toxicity of chemicals by ZFE requires toxicokinetic studies of the test compounds and their TPs to increase comparability to effects in fish.
机译:研究了在暴露96小时后,斑马鱼胚胎(ZFE)中17种具有多种官能团的非离子和离子极性化合物(logD≤2)的时间分辨摄取。其中包括药品,农药和植物活性成分。对于非离子化合物,通过ZFE膜进行扩散控制的被动吸收的吸收速率为0.02至24 h〜(-1),而对于离子化合物,则较慢(<0.008-0.08 h〜(-1))。所研究的化合物在ZFE中的富集并不多(中位生物浓缩系数为1,最大7)。随着时间的推移,生物转化会显着影响某些受试化合物(苯佐卡因,非那西丁,甲丁嗪,苯妥英钠,噻虫啉,丙戊酸)的内部浓度。对于苯佐卡因,丙戊酸和非那西丁,在生命的早期(28 hpf之前)已经通过LC-MS观察到了几种转化产物(TP)。对于苯佐卡因,TP占ZFE中初始量的> 90%。对于六种化合物,内部浓度仍然很低(相对内部浓度<0.2)。除了生物转化(磺胺甲恶唑)外,膜通透性差(西咪替丁,秋水仙碱)以及对外排转运蛋白(阿托品和氯霉素)的亲和力也是造成这些内部浓度低的可能原因。这项研究概述了极性化合物进入ZFE的吸收受到其理化性质的影响。但是,生物过程,生物转化以及可能的外排可强烈影响ZFE早期发育阶段的内部浓度。在以后的毒物动力学模型中应考虑到这一点。通过ZFE评估化学品的毒性需要对测试化合物及其TP进行毒代动力学研究,以提高对鱼类的可比性。

著录项

  • 来源
    《Environmental Science & Technology》 |2016年第18期|10264-10272|共9页
  • 作者单位

    Department of Analytical Chemistry, Helmholtz Centre for Environmental Research - UFZ, Permoserstrasse 15, 04318 Leipzig, Germany;

    Department of Analytical Chemistry, Helmholtz Centre for Environmental Research - UFZ, Permoserstrasse 15, 04318 Leipzig, Germany;

    Department Bioanalytical Ecotoxicoiogy, Helmholtz Centre for Environmental Research - UFZ, Permoserstrasse 15, 04318 Leipzig, Germany;

    Department of Analytical Chemistry, Helmholtz Centre for Environmental Research - UFZ, Permoserstrasse 15, 04318 Leipzig, Germany;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
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