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Generation of statin drug metabolites through electrochemical and enzymatic oxidations

机译:通过电化学和酶促氧化生成他汀类药物代谢产物

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The generation of key drug metabolites for the purpose of their complete structural characterization, toxicity testing, as well as to serve as standards for quantitative studies, is a critical step in the pharmaceutical discovery and development cycle. Here, we utilized electrochemistry/mass spectrometry for the detection and subsequent generation of six phase I metabolites of simvastatin and lovastatin. Both simvastatin and lovastatin are widely used for the treatment of hypercholesterolemia. There are known drug–drug interaction issues of statin therapy, and it has been suggested that the oxidative metabolites may contribute to the cholesterol-lowering effect of both statins. Of the known phase I metabolites of simvastatin and lovastatin, none are commercially available, and chemical means for the synthesis of a very few of them have been previously reported. Here, we report that electrochemical oxidation of less than 1 mg each of simvastatin and lovastatin led to the generation of three oxidative metabolites of each parent to allow complete nuclear magnetic resonance characterization of all six metabolites. The yields obtained by the electrochemical approach were also compared with incubation of parent drug with commercially available bacterial mutant CYP102A1 enzymes, and it was found that the electrochemical approach gave higher yields than the enzymatic oxidations for the generation of most of the observed oxidative metabolites in this study.
机译:为了完整的结构表征,毒性测试以及用作定量研究的标准,关键药物代谢物的产生是药物发现和开发周期中的关键步骤。在这里,我们利用电化学/质谱分析法检测并随后生成了辛伐他汀和洛伐他汀的六种I相代谢产物。辛伐他汀和洛伐他汀均广泛用于治疗高胆固醇血症。他汀类药物疗法存在药物相互作用的已知问题,并且有人提出氧化代谢产物可能有助于两种他汀类药物的降胆固醇作用。在辛伐他汀和洛伐他汀的已知的I期代谢物中,没有一种是可商购的,并且先前已经报道了合成其中极少数的化学方法。在这里,我们报道辛伐他汀和洛伐他汀各自的电化学氧化小于1 mg,导致每个亲本的三种氧化代谢产物的产生,以允许对所有六种代谢产物进行完整的核磁共振表征。还将通过电化学方法获得的产率与母体药物与可商购的细菌突变体CYP102A1酶的温育进行比较,并且发现在该方法中,大多数观察到的氧化代谢物的产生,电化学方法比酶促氧化的产率更高。研究。

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