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The dermal absorption of selected agricultural and industrial chemicals through porcine skin with emphasis on chemical mixture effects.

机译:通过猪皮对某些农业和工业化学品的皮肤吸收,重点是化学混合物的作用。

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摘要

The stratum corneum is the primary barrier to dermal absorption and the processes of absorption include partitioning into, and diffusion through, the lipid matrix of the stratum corneum. These studies were aimed at furthering our understanding of these processes and modeling dermal absorption. We used 11 industrial and agricultural compounds, including 14C labeled phenol, 4-nitrophenol, pentachlorophenol, dimethyl parathion, parathion, chloropyrifos, fenthion, triazine, atrazine, simazine and propazine, and 24 solvent mixtures consisting of combinations of water, ethanol, propylene glycol, sodium lauryl sulphate and methyl nicotinate. Study methods included in vitro partitioning using isolated stratum corneum and permeability studies, Fourier transform infrared spectroscopy, multivariate clustering techniques, transmission electron microscopy and light microscopy. A model of dermal absorption was developed using a physiological-based (PBPK) approach. Ethanol and ethanol/water mixtures altered the stratum corneum through lipid extraction, rather than through disruption of lipid order. Partitioning was primarily determined by relative compound solubility between the stratum corneum lipids and the donor solvent. Permeability reflected the result of successive, complex processes and was not consistently correlated with stratum corneum partitioning. These results demonstrated the potential of using large datasets to identify consistent solvent and chemical mixture effects. Diffusion cell studies were conducted to validate the PBPK model under a variety of conditions including different dose ranges (6.3--106.9 mug/cm2 for parathion; 0.8--23.6 mug/cm 2 for fenthion; 1.6--39.3 mug/cm2 for methyl parathion), different solvents (ethanol, 2-propanol and acetone), different solvent volumes (5--120 mul for ethanol; 20--80 mul for 2-propanol and acetone), occlusion versus open to atmosphere dosing, and corneocyte removal by tape-stripping. The study demonstrated the utility of PBPK models for studying dermal absorption, which can be useful as explanatory and predictive tools; and may be used for in silico hypotheses generation and limited hypotheses testing. These data have direct relevance to topical chemical exposure risk assessments.
机译:角质层是真皮吸收的主要障碍,吸收过程包括分配进入角质层的脂质基质并通过其扩散。这些研究旨在加深我们对这些过程的理解并建立皮肤吸收模型。我们使用了11种工业和农业化合物,包括14C标记的苯酚,4-硝基苯酚,五氯苯酚,二甲基对硫磷,对硫磷,毒死rif,倍硫磷,三嗪,阿特拉津,辛嗪和丙嗪,以及24种由水,乙醇,丙二醇组成的溶剂混合物,月桂基硫酸钠和烟酸甲酯。研究方法包括使用分离的角质层进行体外分配和渗透性研究,傅立叶变换红外光谱,多元聚类技术,透射电子显微镜和光学显微镜。使用基于生理的(PBPK)方法开发了皮肤吸收模型。乙醇和乙醇/水的混合物通过脂质提取而不是通过破坏脂质顺序来改变角质层。分配主要由角质层脂质和供体溶剂之间的相对化合物溶解度决定。渗透率反映了连续,复杂过程的结果,并且与角质层分配没有始终如一的关联。这些结果证明了使用大型数据集识别一致的溶剂和化学混合物效应的潜力。进行扩散细胞研究以验证PBPK模型在各种条件下的有效性,包括不同的剂量范围(对硫磷为6.3--106.9杯/ cm2;二硫磷为0.8--23.6杯/ cm 2;甲基为1.6--39.3杯/ cm2对硫磷),不同的溶剂(乙醇,2-丙醇和丙酮),不同的溶剂体积(乙醇为5--120 mul; 2-丙醇和丙酮为20--80 mul),闭塞vs.通过胶带剥离。这项研究证明了PBPK模型在研究皮肤吸收方面的实用性,可以用作解释和预测工具。并可用于计算机模拟假设生成和有限假设测试。这些数据与局部化学品暴露风险评估直接相关。

著录项

  • 作者

    Van der Merwe, Deon.;

  • 作者单位

    North Carolina State University.;

  • 授予单位 North Carolina State University.;
  • 学科 Health Sciences Toxicology.
  • 学位 Ph.D.
  • 年度 2005
  • 页码 172 p.
  • 总页数 172
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 毒物学(毒理学);
  • 关键词

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