1981
DOI: 10.1016/0163-7258(81)90075-9
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Substrate interaction with cytochrome P-450

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Cited by 195 publications
(97 citation statements)
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References 86 publications
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“…The results showed that after dialysis the treated enzyme had only 16% of the activity of the control, indicating that the timedependent inhibition is an irreversible inactivation. The spectral binding constant (K s ) of CYP3cide for CYP3A4 was not possible to calculate from the observed difference spectra in which no significant spin shift was observed (Schenkman et al, 1981). Examination of the CO binding difference spectrum in inactivated enzyme versus control showed a substantial decrease in the 450-nm CO binding spectrum (Fig.…”
Section: Resultsmentioning
confidence: 99%
“…The results showed that after dialysis the treated enzyme had only 16% of the activity of the control, indicating that the timedependent inhibition is an irreversible inactivation. The spectral binding constant (K s ) of CYP3cide for CYP3A4 was not possible to calculate from the observed difference spectra in which no significant spin shift was observed (Schenkman et al, 1981). Examination of the CO binding difference spectrum in inactivated enzyme versus control showed a substantial decrease in the 450-nm CO binding spectrum (Fig.…”
Section: Resultsmentioning
confidence: 99%
“…Binding of substrates and xenobiotics to P450s can result in two types of characteristic spectral changes in the UV/VIS heme Soret spectrum, referred to as Type I and Type II (Schenkman et al, 1981;Isin and Guengerich, 2008). A classical Type I spectrum results from the spin-state shift of the Soret band at about 418 nm that represents the ferric (Fe III ) low-spin substrate free form tõ 390 nm for the ferric (Fe III ) high-spin form originating from the displacement of H 2 O as the sixth ligand when a substrate is bound in close proximity to the heme.…”
Section: Determination Of Spectral Dissociation Constantsmentioning
confidence: 99%
“…More importantly, however, this finding indicates that ketoconazole inhibition is selective with some cytochrome P-450 enzymes being more affected than others. Presumably this reflects differences in affinities for binding to the cytochrome and formation of a sixth axial ferric coordinate complex between the imidazole nitrogen and the different haem proteins (Schenkman et al;Sheets & Mason, 1984. There has been previous speculation about this possibility (Sheets & Mason, 1984;Meredith et al, 1985), but this is the first direct evidence in humans of such specificity.…”
Section: Discussionmentioning
confidence: 99%