首页> 外文期刊>Xenobiotica: the fate of foreign compounds in biological systems >In vitro metabolism of alpha7 neuronal nicotinic receptor agonist AZD0328 and enzyme identification for its N-oxide metabolite.
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In vitro metabolism of alpha7 neuronal nicotinic receptor agonist AZD0328 and enzyme identification for its N-oxide metabolite.

机译:α7神经元烟碱受体激动剂AZD0328的体外代谢及其N-氧化物代谢物的酶鉴定。

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1. AZD0328 was pharmacologically characterized as a alpha7 neuronal nicotinic receptor agonist intended for treatment of Alzheimer's disease. In vitro AZD0328 cross species metabolite profile and enzyme identification for its N-oxide metabolite were evaluated in this study. 2. AZD0328 was very stable in the human hepatocyte incubation, whereas extensively metabolized in rat, dog and guinea pig hepatocyte incubations. The N-oxidation metabolite (M6) was the only metabolite detected in human hepatocyte incubations, and it also appeared to be the major in vitro metabolic pathway in a number of preclinical species. In addition, N-glucuronide metabolite of AZD0328 was observed in human liver microsomes. 3. Other metabolic pathways in the preclinical species include hydroxylation in azabicyclo octane or furopyridine part of the molecule. Pyridine N-methylation of AZD0328 (M2) was identified as a dog specific metabolite, not observed in human or other preclinical species. 4. Multiple enzymes including CYP2D6, CYP3A4/5, FMO1 and FMO3 catalyzed AZD0328 metabolism. The potential for AZD0328 to be inhibited clinically by co-administered drugs or genetic polymorphism is relative low.
机译:1. AZD0328是药理学表征,作为用于治疗阿尔茨海默病的α7神经元烟碱受体激动剂。在本研究中评估了体外AZD0328交叉物种代谢物分布和其N-氧化物代谢物的酶鉴定。 2. AZD0328在人类肝细胞孵育中非常稳定,而在大鼠,狗和豚鼠肝细胞孵育中广泛代谢。 N-氧化代谢物(M6)是在人肝细胞孵育中检测到的唯一代谢物,并且还似乎是许多临床前物种中的主要体外代谢途径。此外,在人肝微粒体中观察到AZD0328的N-葡糖醛酸代谢物。 3.临床前物种中的其他代谢途径包括在氮杂双环辛烷中的羟基化或分子的呋吡啶部分。将AZD0328(M2)的吡啶N-甲基化被鉴定为狗特异性代谢物,未观察到人或其他临床前物种。 4.多种酶,包括CYP2D6,CYP3A4 / 5,FMO1和FMO3催化AZD0328代谢。通过共同施用的药物或遗传多态性临床抑制AZD0328的可能性相对较低。

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