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使用“内源性”和“外源性”标记物的药物代谢研究。以咪达唑仑中15N与氯的对比为例进行说明。

Drug metabolism studies using "intrinsic" and "extrinsic" labels. A demonstration using 15N vs. Cl in midazolam.

作者信息

Song H, Abramson F

机构信息

Department of Pharmacology, George Washington University Medical Center, Washington, DC 20037.

出版信息

Drug Metab Dispos. 1993 Sep-Oct;21(5):868-73.

PMID:7902250
Abstract

The chemical reaction interface for mass spectrometry (CRIMS) has been used to evaluate the ability of an "intrinsic" label (chlorine) to replace an "extrinsic" label (15N) in a study of the metabolite profile of a drug, in this case the benzodiazepine anesthetic agent midazolam. We find equally high selectivity and comparable signal/noise characteristics for chlorine as for isotopic nitrogen demonstrating that the chlorine in midazolam is itself an effective label and that special synthesis to incorporate isotopic labels is not necessary. The power of either detection mode of CRIMS is shown by detecting 14 metabolites, whereas only four had been previously determined. The ratios of 15N/Cl for each metabolite peak along with conventional mass spectra provide clues to the structures of these new metabolites.

摘要

在一项关于药物(此次研究的是苯二氮䓬类麻醉剂咪达唑仑)代谢物谱的研究中,质谱化学反应界面(CRIMS)已被用于评估“内源性”标记物(氯)替代“外源性”标记物(15N)的能力。我们发现,氯的选择性与同位素氮相当,信号/噪声特性也类似,这表明咪达唑仑中的氯本身就是一种有效的标记物,无需进行特殊合成来引入同位素标记物。通过检测到14种代谢物,显示了CRIMS两种检测模式的能力,而之前仅确定了4种。每个代谢物峰的15N/Cl比率以及传统质谱为这些新代谢物的结构提供了线索。

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