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肝脏微粒体细胞色素P-450中自旋平衡移动、还原速率和N-去甲基化活性与一系列作为底物的苄非他明类似物之间的相关性。

Correlations between spin equilibrium shift, reduction rate, and N-demethylation activity in liver microsomal cytochrome P-450 and a series of benzphetamine analogues as substrates.

作者信息

Blanck J, Rein H, Sommer M, Ristau O, Smettan G, Ruckpaul K

出版信息

Biochem Pharmacol. 1983 Jun 1;32(11):1683-8. doi: 10.1016/0006-2952(83)90109-0.

Abstract

Cytochrome P-450 forms a thermal ferric spin equilibrium which is significantly shifted by substrate binding. Within a series of benzphetamine analogues the liver microsomal enzyme system exhibits a close correlation of the substrate induced spin equilibrium shift towards the high spin state and both the rate of P-450 reduction, and of substrate turnover, as well. The spin equilibrium regulates the first electron transfer by favoured high spin state reduction and rapid pre-equilibration with respect to the low spin fraction.

摘要

细胞色素P - 450形成一种热铁自旋平衡,该平衡会因底物结合而发生显著变化。在一系列苄非他明类似物中,肝脏微粒体酶系统显示出底物诱导的自旋平衡向高自旋状态的转变与P - 450还原速率以及底物周转速率之间存在密切相关性。自旋平衡通过有利于高自旋状态的还原以及相对于低自旋部分的快速预平衡来调节首次电子转移。

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