Discrepancies Between Pharmacokinetic Studies of Amitriptyline

Schulz, Pierre; Dick, P; Blaschke, Terrence F.; Hollister, Leo E.

doi:10.2165/00003088-198510030-00005

Cited by 64 publications

(25 citation statements)

References 32 publications

(20 reference statements)

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“…Fraction bound values obtained using the 96-well dialysis block and the Spectrum apparatus were very similar to each other and consistent with literature values [21][22][23][24][25][26][27][28][29][30] (Table 1). There were minor shifts in fraction bound values between successive experiments that were attributed to intersubject variations in plasma protein concentrations.…”

Section: Validation Of the 96-well Dialysis Apparatussupporting

confidence: 89%

Development and validation of a 96-well equilibrium dialysis apparatus for measuring plasma protein binding

Banker

Clark

Williams

2003

Journal of Pharmaceutical Sciences

266

197

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Section: Validation Of the 96-well Dialysis Apparatussupporting

confidence: 89%

Development and validation of a 96-well equilibrium dialysis apparatus for measuring plasma protein binding

Banker

Clark

Williams

2003

Journal of Pharmaceutical Sciences

266

197

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“…Thus, these in vitro fi ndings suggest that the metabolism of amitriptyline is lower under steady-state conditions as compared with the single-dose situation. This is supported by the fact that the apparent oral clearance is higher in the single-dose case than that under the steady-state situation [32]. Mellstrom and von Bahr [25] also reported that metabolites of amitriptyline reduced the metabolic rate at therapeutic concentrations.…”

Section: Discussionmentioning

confidence: 95%

Roles of polymorphic enzymes CYP2D6 and CYP2C19 for in vitro metabolism of amitriptyline at therapeutic and toxic levels

Jornil

Línnet

2009

Forensic Toxicol

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and likewise the importance of CYP2C19 decreased when the concentration of substrate was increased. The above results indicate that CYP2D6 or CYP2C19 are generally not likely to be critical enzymes related to accidental intoxication under treatment with amitriptyline, but other contributing factors would be important; for example, low levels of various CYP enzymes and/or drug-drug interactions resulting in inhibition of several CYP enzymes may cause amitriptyline poisoning.

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“…However, at therapeutic total plasma AMI concenrespectively, were appreciable but did not reach statistical significance. NT formation by a fourth, unidentified enzyme trations (0.15-1 mm) [21], CYPs 2C9, 2D6 and the unidentified enzyme were more important. The contribution was suggested by the finding of residual N-demethylase activity in liver microsomes in the combined presence of of the latter isoforms to net NT formation at 'therapeutic levels' varied significantly from liver to liver.…”

Section: Resultsmentioning

confidence: 90%

Cytochromes P450 mediating the N‐demethylation of amitriptyline

Ghahramani

Ellis

Lennard

et al. 1997

Brit J Clinical Pharma

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Aims Using human liver microsomes and heterologously expressed human enzymes, we have investigated the involvement of CYPs 1A2, 2C9, 2C19, 2D6 and 3A4 in the N-demethylation of amitriptyline (AMI), with a view to defining likely influences on its clinical pharmacokinetics. Methods The kinetics of formation of nortriptyline (NT) from AMI were measured over the substrate concentration range 1-500 mm, using liver microsomes from four extensive metabolisers (EM) and one poor metaboliser (PM) with respect to CYP2D6 activity. Results The data were best described by a two-site model comprising a MichaelisMenten function for a high affinity site and a Hill function for a low affinity site. The activity at the low affinity site was eliminated by triacetyloleandomycin and ketoconazole, selective inhibitors of CYP3A4, such that the kinetics were then described by a two-site model comprising two Michaelis-Menten functions. A further decrease in activity was associated with the addition of the CYP2C9 inhibitor sulphaphenazole such that the residual kinetics were best described by a single Michaelis-Menten function. The addition of quinidine, a selective inhibitor of CYP2D6, along with triacetyloleandomycin and sulphaphenazole produced an additional decrease in the rate of NT formation in all but the PM liver, but did not completely eliminate the reaction. The remaining activity was best described by a single Michaelis-Menten function. Inhibitors of CYP1A2 (furafylline) and CYP2C19 (mephenytoin) did not impair NT formation. Microsomes from yeast cells expressing CYP2D6 and from human lymphoblastoid cells expressing CYP3A4 or CYP2C9-Arg N-demethylated AMI, but those from cells expressing CYPs 1A2 and 2C19 did not. Conclusions We conclude that CYPs 3A4, 2C9 and 2D6 together with an unidentified enzyme, but not CYPs 1A2 and 2C19, mediate the N-demethylation of AMI. Thus, the clinical pharmacokinetics of AMI would be expected to depend upon the net activities of all of these enzymes. However, the quantitative importance of each isoform is difficult to predict without knowledge of the exposure of the enzymes in vivo to AMI.

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Discrepancies Between Pharmacokinetic Studies of Amitriptyline

Cited by 64 publications

References 32 publications

Development and validation of a 96-well equilibrium dialysis apparatus for measuring plasma protein binding

Development and validation of a 96-well equilibrium dialysis apparatus for measuring plasma protein binding

Roles of polymorphic enzymes CYP2D6 and CYP2C19 for in vitro metabolism of amitriptyline at therapeutic and toxic levels

Cytochromes P450 mediating the N‐demethylation of amitriptyline

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