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首页> 外文期刊>Journal of chromatography, A: Including electrophoresis and other separation methods >Bis-pentafluorobenzyl derivatives of N-acetyl-l-methionine and N-acetyl-l-selenomethionine for the quantitative determination in human plasma by gas chromatography-negative ion chemical ionisation mass spectrometry
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Bis-pentafluorobenzyl derivatives of N-acetyl-l-methionine and N-acetyl-l-selenomethionine for the quantitative determination in human plasma by gas chromatography-negative ion chemical ionisation mass spectrometry

机译:N-乙酰基-1-甲硫氨酸和N-乙酰基-1-硒代甲硫氨酸的双五氟苄基衍生物用于气相色谱-负离子化学电离质谱法定量测定人血浆

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摘要

Targeted anti-cancer combination therapy with infusion of N-acetyl- l-methionine (NALM) and N-acetyl-l-selenomethionine (NASeLM) shows promising results in cancer treatment. Selenium has been recognised as a valuable additive in cancer therapeutics due to its ability to minimise side effects of chemotherapy and its role in cancer prevention and therapy. Due to the promising results of this new therapeutic approach evaluation of pharmacokinetic data for NALM and NASeLM is of ultimate importance. We have therefore elaborated a method for the quantitative measurement of these compounds in human plasma based on GC-negative ion chemical ionisation-MS. The derivatisation sequence elaborated can be regarded as a novel strategy for the chemical modification of delicate sulphur- and selenium-containing compounds, and underlines the enhanced reactivity of selenium-analogues of sulphur-containing amino acids. The target compounds were extracted from plasma with ethyl acetate and converted to the S/Se-pentafluorobenzyl-homocysteine pentafluorobenzyl ester derivative. Reaction conditions were optimised for derivative yield. Calibration graphs were established in the range of 2.938-481.105. ng/0.5. mL plasma (NALM) and 0.233-59.543. ng/0.5. mL plasma (NASeLM). Accuracy, precision and stability data were elaborated. The method was applied to pharmacokinetic profiling of the compounds after infusion into human volunteers.
机译:靶向输注N-乙酰基-1-蛋氨酸(NALM)和N-乙酰基-1-硒代蛋氨酸(NASeLM)的抗癌联合疗法在癌症治疗中显示出令人鼓舞的结果。硒由于其最大程度地降低化学疗法的副作用以及在癌症预防和治疗中的作用而被公认为是癌症治疗中的重要添加剂。由于这种新的治疗方法的有希望的结果,对于NALM和NASeLM的药代动力学数据的评估至关重要。因此,我们开发了一种基于GC负离子化学电离-MS定量测定人血浆中这些化合物的方法。阐述的衍生化序列可以被视为化学修饰精细的含硫和硒化合物的新策略,并强调了含硫氨基酸硒类似物的增强的反应性。用乙酸乙酯从血浆中提取目标化合物,并将其转化为S / Se-五氟苄基-高半胱氨酸五氟苄基酯衍生物。优化反应条件以获得衍生物产率。在2.938-481.105范围内建立校准图。 ng / 0.5。 mL血浆(NALM)和0.233-59.543。 ng / 0.5。 mL血浆(NASeLM)。详细阐述了准确性,精确性和稳定性数据。该方法应用于输注人类志愿者后化合物的药代动力学分析。

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