1972
DOI: 10.1002/cpt1972132258
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Limited capacity for salicyl phenolic glucuronide formation and its effect on the kinetics of salicylate elimination in man

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Cited by 201 publications
(72 citation statements)
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“…The limited capacity for both salicyluric acid and salicyl phenolic glucuronide formation and excretion has been adequately demonstrated (Bedford, Cummings & Martin, 1965;Levy et al, 1972) and a total concept of the kinetics of salicylate metabolism claimed (Levy & Tsuchiya, 1972). It has been suggested that when the dose of aspirin exceeds 0.3 g the rate of formation of salicyluric acid becomes maximal and constant and that synthesis of salicyluric acid will not increase beyond this fixed ceiling despite increasing doses of aspirin, i.e.…”
Section: Resultsmentioning
confidence: 99%
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“…The limited capacity for both salicyluric acid and salicyl phenolic glucuronide formation and excretion has been adequately demonstrated (Bedford, Cummings & Martin, 1965;Levy et al, 1972) and a total concept of the kinetics of salicylate metabolism claimed (Levy & Tsuchiya, 1972). It has been suggested that when the dose of aspirin exceeds 0.3 g the rate of formation of salicyluric acid becomes maximal and constant and that synthesis of salicyluric acid will not increase beyond this fixed ceiling despite increasing doses of aspirin, i.e.…”
Section: Resultsmentioning
confidence: 99%
“…Both salicyluric acid and salicyl phenolic glucuronide are said to be rate limited in their formation and excretion (Levy & Tsuchiya, 1972). This implies that with increasing dosage their synthesis does not increase proportionally.…”
Section: Introductionmentioning
confidence: 99%
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“…These cited observations support our interpretation for the present findings which indicate that elimination of diflunisal for plasma is capacitylimited. In addition, pharmacokinetic studies with sodium salicylate, a compound possessing a chemical structure very close to that of diflunisal, have clearly demonstrated that man has a lmited capacity for salicyl phenolic glucuronide formation even within the therapeutic dose range (Levy & Procknal, 1968;Levy, Tsuchiya & Amsel, 1972), whereas salicyl acyl glucuronide formation is known to involve an apparent first-order process (Levy et al, 1972). Based on the above considerations, it is thus very likely that formation of 5-(2', 4'-difluorophenyl) salicyl phenolic glucuronide (=ether glucuronide), which is quantitatively the most important metabolic pathway for diflunisal, is capacity-limited.…”
Section: Discussionmentioning
confidence: 99%
“…Rates of urinary excretion of 4-hydroxydebrisoquine were tested for deviation from first-order kinetics by a statistical analysis based on the approach of Levy et al (1972). The observed urinary excretion rate of 4-hydroxydebrisoquine (V) and the calculated 'body load' of debrisoquine available for metabolism (DB;Cummings et al, 1967) The kinetic model employed assumes that metabolite elimination is very rapid in relation to the rate of metabolite formation, and the method of estimating ultimate recoveries of metabolites assumes that elimination is terminal and linear in the final period of the study; the use of ultimate recoveries of drug related material does, however, preclude the necessity of assuming quantitative absorption of the oral dose.…”
Section: Analysis Of Datamentioning
confidence: 99%