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肝脏微粒体细胞色素P-450两个催化不同结合位点的证据:对利多卡因氧化模式中物种和性别差异的重要性。

Evidence for two catalytically different binding sites of liver microsomal cytochrome P-450: importance for species and sex differences in oxidation pattern of lidocaine.

作者信息

von Bahr C, Hedlund I, Karlén B, Bäckström D, Grasdalen H

出版信息

Acta Pharmacol Toxicol (Copenh). 1977 Jul;41(1):39-48. doi: 10.1111/j.1600-0773.1977.tb02121.x.

Abstract

When the local anaesthetic drug lidocaine is added to liver microsomes biphasic type I spectral change titration curves can be observed. A high-affinity and a low-affinity phase is observed. In the present study we have found that microsomes from female rats have a dominant high-affinity phase, which can hardly be observed within microsomes from female guinea pigs. Male rats showed an intermediate phase. On incubation of lidocaine at concentrations of 1 micron or less with female rat liver microsomes a larger fraction of the drug was aromatically hydroxylated than deethylated. The opposite was true for guinea pig liver microsomes, and microsomes from male rats were intermediate. The ratio between the formation of deethylated and hydroxylated metabolites increased with the lidocaine concentration and at a lidocaine concentration of 10(-4)M deethylation was the dominant oxidation type in all microsomes. The data suggest that the two spectral phases represent two binding sites of cytochrome P-450 each having a certain "catalytic specificity" - the high affinity catalyzing aromatic hydroxylation and the "low-affinity site" deethylation. This hypothesis is further supported by the observed differential effects of pH and MgCl2 concentration on the two types of oxidation.

摘要

当将局部麻醉药利多卡因添加到肝微粒体中时,可以观察到双相I型光谱变化滴定曲线。观察到一个高亲和力阶段和一个低亲和力阶段。在本研究中,我们发现雌性大鼠的微粒体具有占主导地位的高亲和力阶段,而在雌性豚鼠的微粒体中几乎观察不到。雄性大鼠表现出中间阶段。当利多卡因以1微摩尔或更低的浓度与雌性大鼠肝微粒体一起孵育时,药物中芳香族羟基化的部分比脱乙基化的部分更大。豚鼠肝微粒体则相反,雄性大鼠的微粒体处于中间状态。脱乙基化和羟基化代谢产物形成的比例随利多卡因浓度增加而增加,在利多卡因浓度为10⁻⁴M时,脱乙基化是所有微粒体中的主要氧化类型。数据表明,这两个光谱阶段代表细胞色素P-450的两个结合位点,每个位点都具有一定的“催化特异性”——高亲和力催化芳香族羟基化,“低亲和力位点”催化脱乙基化。pH和MgCl₂浓度对两种氧化类型的不同影响进一步支持了这一假设。

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