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The gas-liquid chromatograph and the electron capture detection in equine drug testing.

机译:气相色谱仪和马药测试中的电子捕获检测。

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摘要

Three gas-liquid chromatographic (G.L.C.) procedures discussed have been designed around the four "esses" of detection tests--speed, sensitivity, simplicity, and specificity. These techniques are admirably applicable to the very low plasma drug levels encountered in blood testing under pre-race conditions. The methods are equally applicable to post-race testing procedures, where both blood and urine samples are tested. Drugs can only rarely be detected by the electron capture detector (E.C.D.) without a prior derivatization step, which conveys to the drug(s) high electron affinity. Because of broad applicability, two derivatizing agents, heptafluorobutyric (HFBA) and pentafluorpropionic (PFPA) anhydrides are employed. The three techniques, allowing broad coverage of various drug classes are: 1) direct derivatization of drugs to form strongly electron capturing amides and esters. 2) reductive fragmentation of drugs with lithium aluminum hydride to form alcohols, with conversion to ester derivatives. 3) oxidative fragmentation of drugs with potassium dichromate to form derivatizable groups, followed by direct derivatization.
机译:已经围绕检测测试的四个“精要”(速度,灵敏度,简便性和特异性)设计了三种讨论的气液色谱(G.L.C.)程序。这些技术非常适用于赛前条件下血液测试中遇到的非常低的血浆药物水平。该方法同样适用于赛后测试程序,在该程序中测试血液和尿液样本。没有预先衍生化步骤的电子捕获检测器(E.C.D.)很少能检测到药物,而衍生化步骤将高电子亲和力传递给药物。由于广泛的适用性,使用了两种衍生剂,七氟丁酸(HFBA)和五氟丙酸(PFPA)酸酐。允许广泛涵盖各种药物类别的三种技术是:1)药物直接衍生化以形成具有强电子捕获能力的酰胺和酯。 2)药物与氢化铝锂还原裂解形成醇,并转化为酯衍生物。 3)用重铬酸钾将药物氧化裂解形成可衍生基团,然后直接衍生化。

著录项

  • 作者

    Blake, J. W.; Tobin, T.;

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  • 年度 1976
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  • 原文格式 PDF
  • 正文语种 en
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