Polymorphic drug oxidation: pharmacokinetic basis and comparison of experimental indices.

Self Cite

1. The shape of histograms used to illustrate density distributions of indices of polymorphic drug metabolism was shown to be sensitive to the position of the cell divisions. 2. Non‐linearity of the probit plot was shown not to indicate bimodality of the original density distribution. Computer simulation was used to generate examples of unimodal density distributions with curvilinear probit plots. 3. Using the same technique probit plots for bimodal density distributions were constructed. Some were shown to differ less from the probit plots of certain unimodal distributions than did the original density distributions. 4. The position of the antimode was shown not to coincide with inflections seen in the probit plots. 5. A new method for determining the linearity of probit plots is suggested.

Section: Introductionmentioning

confidence: 99%

Testing for bimodality in frequency distributions of data suggesting polymorphisms of drug metabolism‐histograms and probit plots.

Jackson

Tucker

Woods

1989

Self Cite

“…1-MU is the only metabolic product of 1-MX and this reaction is catalysed by xanthine oxidase (Birkett et al, 1983). The use of the ratio of product to substrate in urine collections, as an indication of the metabolic clearance of substrate, has been described previously (Jackson et al, 1986;Birkett et al, 1987). A further assumption, made when using this approach, was that allopurinol does not affect the renal clearance of 1-MU or 1-MX.…”

Section: Resultsmentioning

confidence: 99%

Relationship between plasma oxipurinol concentrations and xanthine oxidase activity in volunteers dosed with allopurinol.

Day

Miners

Birkett

et al. 1988

1 1-methyl xanthine (1-MX) is metabolized exclusively to 1-methyl uric acid (1-MU) by the enzyme xanthine oxidase. 2 The ratio of 1-MU to 1-MX in the urine, following a dose of 50 mg of 1-MX infused intravenously over 20 min, was used to measure the inhibition of xanthine oxidase induced by different doses of allopurinol. 3 Normal volunteers (n=8) were given allopurinol 50, 100, 300 and 600 mg daily for 1 week each, in random order and 1 week separated each treatment. Inhibition of xanthine oxidase was assessed twice, on the last 2 days of each treatment week. 4 Steady-state oxipurinol concentrations increased linearly with increasing dose of allopurinol. 5 There was a hyperbolic relationship between the 1-MU/1-MX ratio and plasma oxipurinol concentrations, with an initial steep decline in the ratio which plateaued when plasma oxipurinol was around 4-6 mg 1-1. This reduction in the ratio was quickly reversible upon cessation of allopurinol. 6 The 50% and 90% effective inhibitory oxipurinol concentrations, in relation to the 1-MU-/1-MX ratio were 1.4 ± 0.46 and 4.08 ± 2.03 mg 1-1 respectively. 7 The concentration of oxipurinol required for almost complete inhibition of the enzyme was substantially less than those often observed in clinical practice.

“…Peart et al (1986) have demonstrated an excellent correlation between DMR obtained by 4 h and 8 h urine collection. Jackson et al (1986) explored the pharmacokinetic basis of the urinary drug/metabolite ratio in a model drug with kinetic properties similar to that of D. They concluded that the time of urine collection would make little difference to the frequency distribution of the metabolic ratio. Table 1 shows that hourly sampling of urine was unable to provide adequate data for the calculation of the DMR in PM subjects.…”

Section: Discussionmentioning

confidence: 99%

“…With the small number of subjects studied it is not possible to infer from the present work whether phenotyping by a short urine collection, as suggested above, will result in a shift of the antimode. Jackson et al (1986) suggested that a change in the antimode would occur only when urine collection time was a small fraction of the elimination half-life of the parent drug. P.A.P.…”

Section: Discussionmentioning

confidence: 99%

Determination of debrisoquine metabolic ratio from hourly urine collections in healthy volunteers.

Philip

James

Rogers

1987

The possibility of simplifying the regimen for the collection of urine samples in the determination of the debrisoquine metabolic ratio (DMR) was explored in 15 normal subjects. In the extensive metaboliser subgroup (EM; n = 11), there was a close correlation between the DMR as determined by an 8 h urine collection and the debrisoquine/4-hydroxydebrisoquine ratio (D/4-OHD) in the hourly samples (excluding the first hour). In the poor metabolisers (PM; n = 4) the phenotype could be identified, but it was not possible to estimate the DMR reliably.