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Enhanced FTase activity achieved via piperazine interaction with catalytic zinc.

机译:通过哌嗪与催化锌的相互作用获得增强的FTase活性。

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摘要

Benzocycloheptapyridine tricyclic compounds with piperazine or substituted piperidine moieties extending either from the 5- or 6-position of the tricyclic bridgehead exhibited enhanced FTase activity: this resulted from favorable binding of the ligand nitrogen with the catalytic zinc found in the FTase. A single isomer at C-11 with piperazine adduct extending from the 6-position, compound 24, exhibited excellent FTase activity with IC50 = 0.007 microM, soft agar IC50 = 72 nM, and Rat AUC(PO, 10 mpk) = 4.0 microM x h. X-ray of (-)-[8-chloro-6-(1-piperazinyl)-1H-benzo[5,6]]cyclohepta[1,2-b]pyridine-11 -yl]-1-(methylsulfonyl)piperidine 24 bound to Ftase revealed favorable interaction between piperazine nitrogen and catalytic zinc atom.
机译:具有从三环桥头的5位或6位延伸的哌嗪或取代的哌啶部分的苯并七庚啶三环化合物具有增强的FTase活性:这是由于配体氮与FTase中的催化锌良好结合所致。 C-11处的一个单一异构体与哌嗪加合物从6位开始延伸,化合物24表现出出色的FTase活性,IC50 = 0.007 microM,软琼脂IC50 = 72 nM,大鼠AUC(PO,10 mpk)= 4.0 microM x H。 (-)-[8-氯-6-(1-哌嗪基)-1H-苯并[5,6]]环庚[1,2-b]吡啶-11-基] -1-(甲基磺酰基)的X射线与Ftase结合的哌啶24显示哌嗪氮与催化性锌原子之间具有良好的相互作用。

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