GT Tucker scite author profile

inhibited CYP2D6 activity. The major circulating metabolites of paroxetine in man produced negligible inhibition. In contrast, norfluoxetine the active metabolite of fluoxetine, was a potent CYP2D6 inhibitor (0.43 piM). CYP2D6 activity was also diminished by the tricyclic antidepressant drugs clomipramine (2.2 pM), desipramine (2.3 pRM) and amitriptyline (4.0 IIM). These findings suggest that compounds with SSRI activity are likely to interact with human CYP2D6 in vivo with the potential of causing drug interactions.

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‘In silico’ simulations to assess the ‘in vivo’ consequences of ‘in vitro’ metabolic drug–drug interactions

Rostami‐Hodjegan

Tucker

2004

Drug Discovery Today: Technologies

211

167

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Metoprolol metabolism and debrisoquine oxidation polymorphism‐ population and family studies.

McGourty¹,

Silas²,

Lennard³

et al. 1985

Brit J Clinical Pharma

150

112

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1 The metabolism of metoprolol was studied in 143 unselected hypertensive patients and in 10 families. 2 The loglo metoprolol to a-hydroxymetoprolol urinary ratio was bimodally distributed and was correlated with the debrisoquine oxidation phenotype (rs = 0.81, P < 0.001).3 The results of the pedigree study were compatible with poor hydroxylation of metoprolol being inherited as an autosomal recessive trait. 4 The major urinary metabolite of metoprolol metabolism was H117-04, the endproduct of O-dealkylation. The distribution of the log1o metoprolol to H117-04 (M/H117-04) urinary ratio was unimodal. However, there was a significant correlation between this ratio and the debrisoquine oxidation phenotype (rs = 0.68, P < 0.001) and poor metabolisers of debrisoquine (PMs) were concentrated at the upper end of the range of M/H117-04 values. 5 These results indicate that both the a-hydroxylation and O-dealkylation of metoprolol are under polymorphic control of the debrisoquine type. 6 Plasma concentrations of metoprolol were about three times higher in PMs than in extensive metabolisers of debrisoquine (EMs) at 3 h after dosing. 7 In a sub-group of 24 subjects, all seven PMs but only two EMs showed more than a 10% reduction in post-exercise heart rate at 24 h after dosing.

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Enantiomer specific pharmacokinetics

Tucker

Lennard

1990

Pharmacology & Therapeutics

189

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GT Tucker

Metformin kinetics in healthy subjects and in patients with diabetes mellitus.

The effect of selective serotonin re‐uptake inhibitors on cytochrome P4502D6 (CYP2D6) activity in human liver microsomes.

‘In silico’ simulations to assess the ‘in vivo’ consequences of ‘in vitro’ metabolic drug–drug interactions

Metoprolol metabolism and debrisoquine oxidation polymorphism‐ population and family studies.

Enantiomer specific pharmacokinetics

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