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Comparative metabolism and covalent binding of procainamide by human leukocytes.

作者信息

Uetrecht J, Sokoluk B

机构信息

Faculty of Pharmacy, University of Toronto, Ontario, Canada.

出版信息

Drug Metab Dispos. 1992 Jan-Feb;20(1):120-3.

PMID:1346986
Abstract

Activated neutrophils and monocytes were found to metabolize procainamide to a reactive hydroxylamine. In contrast, there was little or no metabolism by lymphocytes or platelets. Therefore, it appears that only leukocytes that contain myeloperoxidase can metabolize procainamide to a significant degree. There was no difference in the degree to which neutrophils from males or females metabolized procainamide; however, monocytes from males formed significantly more hydroxylamine than did monocytes from females. By use of radiolabeled procainamide, covalent binding of procainamide to leukocytes was detected, and the degree of binding correlated with the cells' ability to oxidize procainamide. These findings suggest that myeloperoxidase is the major enzyme involved in the formation of reactive metabolites by leukocytes, a pathway that we propose may be responsible for procainamide-induced lupus and agranulocytosis.

摘要

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The use of a three compartment in vitro model to investigate the role of hepatic drug metabolism in drug-induced blood dyscrasias.
使用三室体外模型研究肝脏药物代谢在药物性血细胞减少症中的作用。
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