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Binding of nitrosamines to cytochrome P-450 of liver microsomes.
Authors:K E Appel  H H Ruf  B Mahr  M Schwarz  R Rickart  W Kunz
Affiliation:1. Abt. Molekulare Toxikologie, Institut für Biochemie, Deutsches Krebsforschungszentrum, Im Neuenheimer Feld 280, D-6900 Heidelberg F.R.G.;2. Institut für Physiologische Chemie, Universität des Saarlandes, Homburg/Saar F.R.G.
Abstract:The interactions of 5 carcinogenic and 1 non-carcinogenic nitrosamines with hepatic microsomal cytochrome (cyt.) P-450 were investigated, using both optical difference and electron paramagnetic resonance (EPR) spectroscopic methods. Liver microsomes from phenobarbital (PB)-pretreated mice and 3-methylcholanthrene (3-MC)-pretreated rats were used, in order to have an increased specific content of cyt. P-450 and cyt. P-448 respectively. The optical and EPR spectral data obtained in the oxidised state suggest that nitrosamines are able to bind both as substrates and as ligands to the hemoprotein cyt. P-450, depending on the concentration of nitrosamine, its chemical identity and the cytochrome species present. After reduction with dithionite or NADPH in the optical difference spectrum a Soret band developed between 444 and 453 nm to an extent, which is dependent on the particular nitrosamine present. This initial nitrosamine-induced spectrum might represent a ferrous nitric oxide (NO)-cyt. P-450 complex. It appears unstable and is converted kinetically into a spectrum lacking a Soret band, but with a predominant absorbance minimum at about 425 nm. A visible band is located at 585 nm. In the EPR spectrum a sharp 3-line signal around g = 2.01 appears concomitantly. Both spectral parameters are typical of a NO-cyt. P-420 complex. These results, in conjunction with metabolic studies, indicate that nitrosamines are denitrosated by a reductive process in which cyt. P-450 appears to be involved. The resulting NO-cyt. P-450 complex denatures to a NO-cyt. P-420 complex when the dioxygen level is not sufficiently high to complete successfully.
Keywords:cyt.  cytochrome  DBNA  DENA  diethylnitrosamine  DiphenNA  Diphenylnitrosamine  DMNA  dimethylnitrosamine  DMSO  dimethylsulphoxide  DPNA  EPR  electron paramagnetic resonance  3-MC  3-methylcholanthrene  MoNA  NO  nitric oxide  PB  phenobarbital
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