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Title: Effects of age and other drugs on benzodiazepine kinetics. Author: Greenblatt DJ, Shader RI. Journal: Arzneimittelforschung; 1980; 30(5a):886-90. PubMed ID: 6106490. Abstract: Because benzodiazepine derivatives are biotransformed by a variety of metabolic pathways, it is not surprising that age has varying effects on their kinetic properties. Both chlordiazepoxide and diazepam are biotransformed by hepatic N-demethylation. The aging process is associated with prolonged half-life and reduced clearance of both of these drugs. Sex may also influence their kinetics. In the case of diazepam, aging effects may be masked by alterations in protein binding. Desmethyldiazepam and desalkylflurazepam are biotransformed by hydroxylation. Old age tends to be associated with reduced clearance of these two compounds, particularly among elderly males, but age explains a relatively small portion of individual variation in their kinetics. Oxazepam, lorazepam, and temazepam undergo glucuronidation. Age has a relatively minor effect on the kinetics of these compounds. In general, altered hepatic clearance in the elderly does not necessarily predict changes in drug sensitivity, since many factors complicate the relation between blood concentrations and clinical response. Drug interactions with benzodiazepine derivatives are relatively uncommon and generally are not of clinical significance. Antacid coadministration reduces the rate but not the completeness of benzodiazepine absorption. Concurrent therapy with disulfiram impairs the clearance of chlordiazepoxide and diazepam, but not of oxazepam or lorazepam. Kinetic interactions with alcohol have been inconsistently reported, but probably are less important than the predictable additive central depressant effects.[Abstract] [Full Text] [Related] [New Search]