Reactive metabolites are believed to be responsible for many types of toxicity, including idiosyncratic drug reactions. Bone marrow is a frequent target of idiosyncratic reactions, and, since these reactions have characteristics that suggest involvement of the immune system, the formation of reactive metabolites by leucocytes could also play a role in the aetiology of idiosyncratic drug reactions. The major oxidation system in neutrophils and monocytes is a combination of NADPH oxidase and myeloperoxidase. This system oxidizes primary arylamines, such as sulphonamides, to reactive metabolites and these drugs are also associated with a high incidence of agranulocytosis, generalized idiosyncratic reactions and/ or drug-induced lupus. Clozapine is oxidized by this system to a relatively stable nitrenium ion; clozapine is also associated with a high incidence of agranulocytosis. Arylamines that have an oxygen or nitrogen in the para position, such as amodiaquine, vesnarinone and 5-aminosalicylic acid, are oxidized to quinone-like reactive intermediates. Aminopyrine is oxidized to a very reactive dication. Such reactive metabolites could also inhibit neutrophil function and mediate some of the therapeutic effects of these drugs: for example, the use of dapsone for dermatitis herpetiformis and the use of 5-aminosalicylic acid for inflammatory bowel disease.
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November 1995
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Conference Article|
November 01 1995
Myeloperoxidase as a generator of drug free radicals
Jack P. Uetrecht
Jack P. Uetrecht
1
1Faculties of Pharmacy and Medicine, Drug Safety Research Group, University of Toronto and Sunnybrook Health Science Centre, Toronto, Canada
1Address for correspondence: Faculty of Pharmacy, University of Toronto, 19 Russell Street, Toronto, Canada M5S 2S2
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Publisher: Portland Press Ltd
Online ISSN: 1744-1439
Print ISSN: 0067-8694
© 1995 The Biochemical Society
1995
Biochem Soc Symp (1995) 61: 163–170.
Citation
C. Rice-Evans, B. Halliwell, G.G. Lunt, Jack P. Uetrecht; Myeloperoxidase as a generator of drug free radicals. Biochem Soc Symp 1 November 1995; 61 163–170. doi: https://doi.org/10.1042/bss0610163
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