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Stable Isotope- and Mass Spectrometry-based Metabolomics as Tools in Drug Metabolism: A Study Expanding Tempol Pharmacology

机译:稳定的同位素和质谱基代代谢组科作为药物代谢的工具:一种扩展Tempol Pharmacology的研究

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The application of mass spectrometry-based metabolomics in the field of drug metabolism has yielded important insights not only into the metabolic routes of drugs but has provided unbiased, global perspectives of the endogenous metabolome that can be useful for identifying biomarkers associated with mechanism of action, efficacy, and toxicity. In this report, a stable isotope- and mass spectrometry-based metabolomics approach that captures both drug metabolism and changes in the endogenous metabolome in a single experiment is described. Here the antioxidant drug tempol (4-hydroxy-2,2,6,6-tetramethylpiperidine-N-oxyl) was chosen because its mechanism of action is not completely understood and its metabolic fate has not been studied extensively. Furthermore, its small size (MW = 172.2) and chemical composition (C9H18NO2) makes it challenging to distinguish from endogenous metabolites. In this study, mice were dosed with tempol or deuterated tempol (C9D17HNO2) and their urine profiled using ultraperformance liquid chromatography coupled with quadrupole time-of-flight mass spectrometry. Principal component analysis of the urinary metabolomics data generated a Y-shaped scatter plot containing drug metabolites (protonated and deuterated) that were clearly distinct from the endogenous metabolites. Ten tempol drug metabolites, including eight novel metabolites, were identified. Phase II metabolism was the major metabolic pathway of tempol in vivo, including glucuronidation and glucosidation. Urinary endogenous metabolites significantly elevated by tempol treatment included 2,8-dihydroxyquinoline (8.0-fold, P<0.05) and 2,8-dihydroxyquinoline-β-D-glucuronide (6.8-fold, P<0.05). Urinary endogenous metabolites significantly attenuated by tempol treatment including pantothenic acid (1.3-fold, P<0.05) and isobutrylcarnitine (5.3-fold, P<0.01). This study underscores the power of a stable isotope- and mass spectrometry-based metabolomics in expanding the view of drug pharmacology.
机译:基于质谱的代谢组学在药物代谢领域的应用不仅对药物的代谢途径产生了重要见解,而且对内源性代谢组学提供了无偏见的全局视角,可用于识别与作用机制相关的生物标志物,功效和毒性。在本报告中,描述了一种基于同位素和质谱的稳定代谢组学方法,该方法可在单个实验中捕获药物代谢和内源性代谢组的变化。在这里选择抗氧化剂药物tempol(4-羟基-2,2,6,6-四甲基哌啶-N-氧基)是因为其作用机理尚未完全了解,并且其代谢命运尚未得到广泛研究。此外,它的体积小(MW = 172.2)和化学成分(C9H18NO2)使其很难与内源性代谢物区分开。在这项研究中,给小鼠注射了tempol或氘代的tempol(C9D17HNO2),并使用超高效液相色谱结合四极杆飞行时间质谱对小鼠的尿液进行了分析。尿液代谢组学数据的主成分分析生成了一个Y形散点图,其中包含与内源性代谢物明显不同的药物代谢物(质子化和氘代)。确定了十种tempol药物代谢物,其中包括八种新型代谢物。 II期代谢是tempol在体内的主要代谢途径,包括葡萄糖醛酸化和葡萄糖苷化。经tempol处理显着升高的尿内源性代谢物包括2,8-二羟基喹啉(8.0倍,P <0.05)和2,8-二羟基喹啉-β-D-葡萄糖醛酸(6.8倍,P <0.05)。 tempol处理后尿内源性代谢产物显着减弱,包括泛酸(1.3倍,P <0.05)和异丁卡尼汀(5.3倍,P <0.01)。这项研究强调了稳定的基于同位素和质谱的代谢组学在扩大药物药理学观点方面的作用。

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