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肝脏微粒体对他克林生物活化的种属差异。

Species variation in the bioactivation of tacrine by hepatic microsomes.

作者信息

Madden S, Spaldin V, Hayes R N, Woolf T F, Pool W F, Park B K

机构信息

Department of Pharmacology and Therapeutics, University of Liverpool, UK.

出版信息

Xenobiotica. 1995 Jan;25(1):103-16. doi: 10.3109/00498259509061837.

Abstract
  1. The metabolite profile of tacrine (1,2,3,4-tetrahydro-9-amino acridine) was similar in hepatic microsomes from man, rat, dog, rabbit, mouse and hamster. Major metabolites were 1-, 2-, 4- and 7-OH tacrine. Only quantitative differences in metabolite profile were evident between species. 2. Bioactivation to protein-reactive metabolite(s) was seen in microsomes from all species. 3. 7-Methyl tacrine was found to undergo significantly less bioactivation than either 7-OH tacrine or tacrine itself. 4. In the presence of hepatic microsomes and thiol-containing agents protein-reactive metabolite formation was significantly reduced. With mercaptoethanol present a stable thioether adduct was generated from both tacrine and 7-OH tacrine. 5. Analysis of the thioether adduct by mass spectrometry yielded a molecular ion of m/z 290 consistent with the presence of a covalent adduct of 7-OH tacrine complexed in a 1:1 molar ratio with mercaptoethanol. 6. We have therefore provided further evidence for a two-step mechanism in the bioactivation of tacrine involving an initial 7-hydroxylation followed by a postulated 2-electron oxidation to yield a reactive quinone methide. This mechanism of bioactivation appears to be identical in human and animal hepatic microsomes.
摘要
  1. 他克林(1,2,3,4-四氢-9-氨基吖啶)在人、大鼠、狗、兔、小鼠和仓鼠的肝微粒体中的代谢物谱相似。主要代谢物为1-、2-、4-和7-羟基他克林。不同物种之间仅在代谢物谱上存在定量差异。2. 在所有物种的微粒体中均观察到生物活化生成蛋白质反应性代谢物。3. 发现7-甲基他克林的生物活化程度明显低于7-羟基他克林或他克林本身。4. 在肝微粒体和含硫醇试剂存在的情况下,蛋白质反应性代谢物的形成显著减少。存在巯基乙醇时,他克林和7-羟基他克林均生成稳定的硫醚加合物。5. 通过质谱分析硫醚加合物得到的分子离子峰m/z为290,这与7-羟基他克林与巯基乙醇以1:1摩尔比络合形成的共价加合物一致。6. 因此,我们为他克林的生物活化两步机制提供了进一步证据,该机制包括最初的7-羟基化,随后推测发生双电子氧化生成反应性醌甲基化物。这种生物活化机制在人和动物肝微粒体中似乎是相同的。

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