Relationship between covalent binding to microsomal protein and the destruction of adrenal cytochrome P-450 by spironolactone

Colby, H. D.; O'Donnell, J. P.; Flowers, N. L.; Kossor, D. C.; Johnson, P. B.; Levitt, M.

doi:10.1016/0300-483x(91)90138-q

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Relationship between covalent binding to microsomal protein and the destruction of adrenal cytochrome P-450 by spironolactone
Citation	Colby HD, O'Donnell JP, Flowers NL, Kossor DC, Johnson PB, Levitt M. Toxicology 1991; 67(2): 143-154.
Copyright	(Copyright © 1991, Elsevier Publishing)
DOI	10.1016/0300-483x(91)90138-q
PMID	2031249
Abstract	Previous investigations have demonstrated that guinea pig adrenal microsomes catalyze an NADPH-dependent activation of spironolactone (SL) resulting in the degradation of cytochrome(s) P-450 and decreases in steroidogenic enzyme activities. Studies were done to evaluate the relationship between the destruction of cytochrome P-450 and the covalent binding to microsomal protein by SL and by 7 alpha-thiospironolactone (7 alpha-thio-SL), an obligatory intermediate in the activation pathway. NADPH-dependent irreversible binding to guinea pig adrenal microsomal protein was demonstrable with 22-14C- and with 35S-labelled SL or 7 alpha-thio-SL as substrates. In the absence of NADPH, there was relatively little binding. NADPH-dependent covalent binding was not demonstrable with hepatic microsomal preparations. The amount of covalent binding to adrenal microsomes was far greater with 7 alpha-thio-SL than with SL and also greater with 35S-labelled than with 14C-labelled substrates. The latter results suggest the possibility of more than one reactive metabolite. Time-course experiments revealed a good correlation between covalent binding and P-450 destruction by SL and by 7 alpha-thio-SL. In addition, the 17 alpha-hydroxylase inhibitor, SU-10'603, and the 17 alpha-hydroxylase substrate, progesterone, prevented both the degradation of cytochrome P-450 and the NADPH-dependent covalent binding by 7 alpha-thio-SL. Reduced glutathione also decreased covalent binding but did not diminish P-450 destruction. The latter results indicate that some of the covalent binding is unrelated to the degradation of cytochrome P-450. However, all of the data are consistent with the hypothesis that 7 alpha-thio-SL is a suicide inhibitor of adrenal cytochrome P-450 and that covalent binding to protein is involved in the degradation of cytochrome P-450. Language: en
Keywords	Adrenal Glands; Animals; Cytochrome P-450 Enzyme System; Guinea Pigs; Male; Microsomes; Microsomes, Liver; NADP; Proteins; Spironolactone