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固相微萃取测定微量污染物-大分子分配系数。

Solid-phase microextraction to determine micropollutant-macromolecule partition coefficients.

机构信息

Institute of Biological Chemistry, Biophysics and Bioengineering, Heriot-Watt University, Edinburgh, UK.

The National Institute of Public Health and the Environment (RIVM), Bilthoven, the Netherlands.

出版信息

Nat Protoc. 2016 Aug;11(8):1328-44. doi: 10.1038/nprot.2016.068. Epub 2016 Jun 30.

Abstract

Aqueous micropollutants such as estradiol can have a large environmental impact-even at low concentrations. Part of understanding this impact involves determining the extent to which the micropollutants interact with macromolecules in water. In environmental samples, relevant macromolecules to which micropollutants bind are referred to as dissolved organic matter, and the most common examples of these in freshwater and coastal seawater are fulvic and humic acids. In living organisms, the most common macromolecules that affect bioavailability of a drug (or toxin) are proteins such as albumin. Using [2, 4, 6, 7 - (3)H]estradiol as an example compound, this protocol uses solid-phase microextraction and scintillation detection as analytical tools to quantify the amount of radiolabeled micropollutant available in solution. The measured free concentration after exposure to various concentrations of macromolecule (dissolved organic matter or protein) or micropollutant is used to determine the partition coefficient in the case of micropollutant-macromolecule interactions. The calibration and preparatory studies take at least 8 d, and the steps to determine the partition coefficient can be completed within 3 d. The protocol could be modified such that nonlabeled compounds are studied; instead of detection of activity by a liquid scintillation counter (LSC), the compounds can be quantified using gas chromatography-mass spectrometry (GC-MS) or liquid chromatography (LC)-MS(/MS).

摘要

水相中的微量污染物,如雌二醇,即使在低浓度下,也可能对环境产生重大影响。了解这种影响的一部分内容涉及确定微量污染物与水中大分子相互作用的程度。在环境样本中,与微量污染物结合的相关大分子被称为溶解的有机物质,而在淡水和沿海水体中最常见的例子是腐殖酸和富里酸。在生物体中,影响药物(或毒素)生物利用度的最常见的大分子是蛋白质,如白蛋白。本协议使用[2,4,6,7-(3)H]雌二醇作为示例化合物,使用固相微萃取和闪烁检测作为分析工具来量化溶液中放射性标记的微量污染物的可用量。暴露于不同浓度的大分子(溶解的有机物质或蛋白质)或微量污染物后测量的游离浓度用于确定微量污染物-大分子相互作用的分配系数。校准和预备研究至少需要 8 天,而确定分配系数的步骤可以在 3 天内完成。该协议可以进行修改,以研究非标记化合物;而不是通过液体闪烁计数器(LSC)检测活性,化合物可以使用气相色谱-质谱法(GC-MS)或液相色谱(LC)-质谱法(MS/MS)进行定量。

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