Simultaneous modelling of the michaelis-menten kinetics of paracetamol sulphation and glucuronidation

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Abstract

1. The aim of the present study was to perform an in vivo estimation of the Michaelis-Menten constants of the major metabolic pathways of paracetamol (APAP). 2. A two-occasion, single-dose cross-over trial was performed using 60 and 90 mg/kg doses of APAP in healthy patients undergoing third molar dental extraction. Plasma samples were collected over 24 h and urine was collected for 8 h after dosing. Twenty patients were enrolled in the study and complete data for plasma and urine were available for both doses for 13 volunteers who were included in the analysis; seven of the volunteers were men, the median age (range) was 22 years (19-31) and the median weight (range) was 68 kg (50-86). 3. The mean (95% CI) km for APAP glucuronidation was 6.89 mmol/L (3.57-10.22) and the Vmax was 0.97 mmol/h per kg (0.65-1.28). The km for APAP sulphation was 0.097 mmol/L (0.041-0.152) and the V max was 0.011 mmol/h per kg (0.009-0.013). For the combined excretion of APAP-cysteine and APAP-mercapturate, the km was 0.303 mmol/L (0.131-0.475) and the Vmax was 0.004 mmol/h per kg (0.002-0.005). 4. The estimates for in vivo Michaelis-Menten constants for APAP glucuronidation and sulphation were in the order of those reported previously using in vitro methods. © 2008 The Authors.

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Reith, D., Medlicott, N. J., Kumara De Silva, R., Yang, L., Hickling, J., & Zacharias, M. (2009). Simultaneous modelling of the michaelis-menten kinetics of paracetamol sulphation and glucuronidation. Clinical and Experimental Pharmacology and Physiology, 36(1), 35–42. https://doi.org/10.1111/j.1440-1681.2008.05029.x

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