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Quantitative analysis of the spin equilibrium of cytochrome P-450 LM2 fraction from rabbit liver microsomes.

作者信息

Ristau O, Rein H, Greschner S, Jänig G R, Ruckpaul K

出版信息

Acta Biol Med Ger. 1979;38(2-3):177-85.

PMID:229674
Abstract

The LM2 fraction of cytochrome P-450 from phenobarbital induced rabbit liver microsomes in the presence and in the absence of substrate (benzphetamine) is shown to be a thermal equilibrium of a high spin (S = 5/2) and a low spin (S = 1/2) state each of which exhibiting its individual optical basic spectrum with the Soret maxima at 387 nm and 417 nm for the high spin form and the low spin form, respectively. The equilibrium constants and thermodynamic parameters describing the spin transition and the substrate binding have been evaluated from the temperature and substrate difference spectra. These two interacting equilibria are presented in terms of a thermodynamic model, which provides a quantitative description of the relationship between the substrate binding and the spin equilibrium. From kinetic experiments it is concluded that the spin equilibrium is an electronic one and is not caused by iron ligand dissociation.

摘要

相似文献

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Quantitative analysis of the spin equilibrium of cytochrome P-450 LM2 fraction from rabbit liver microsomes.
Acta Biol Med Ger. 1979;38(2-3):177-85.
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Interaction of constitutive and phenobarbital-induced cytochrome P-450 isozymes during the sequential oxidation of benzphetamine. Explanation for the difference in benzphetamine-induced hydrogen peroxide production and 455-nm complex formation in microsomes from untreated and phenobarbital-treated rats.苯丙胺连续氧化过程中组成型和苯巴比妥诱导的细胞色素P-450同工酶的相互作用。对未处理和苯巴比妥处理大鼠微粒体中苯丙胺诱导的过氧化氢产生和455纳米复合物形成差异的解释。
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