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Clinical Pharmacokinetics

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01.11.2001 | Original Research Article

Quantitative Pharmacogenetics of Nortriptyline

A Novel Approach

verfasst von: Elin E. Kvist, Ayman Al-Shurbaji, Marja-Liisa Dahl, Conny Nordin, Gunnar Alván, Dr Lars Ståhle

Erschienen in: Clinical Pharmacokinetics | Ausgabe 11/2001

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Abstract

Objective

To quantitatively model nortriptyline clearance as a function of the cytochrome P450 (CYP) 2D6 genotype and to estimate the contribution of genotype to the interindividual variability in steady-state plasma concentration and metabolic clearance.

Design

Modelling study using data from two previously published studies.

Participants

20 healthy volunteers receiving single oral doses of nortriptyline and 20 patients with depression on steady-state oral treatment.

Methods

A total of 275 nortriptyline plasma concentrations were analysed by standard nonlinear regression and nonlinear mixed effect models. The pharmacokinetic model was a 1-compartment model with first order absorption and elimination. All participants had previously been genotyped with respect to the CYP2D6 polymorphism.

Results

A model in which the intrinsic clearance is a linear function of the number of functional CYP2D6 genes and hepatic blood flow is fixed to 60 L/h gave the closest fit of the pharmacokinetic model to the data. Stable estimates were obtained for population pharmacokinetic parameters and interindividual variances. Assuming 100% absorption, the model allows systemic clearance and bioavailability to be estimated. Bioavailability was found to vary between 0.17 and 0.71, depending on the genotype. Using the frequency distribution of CYP2D6 genotype with the above results we estimate that, in compliant Swedish individuals on nortriptyline monotherapy, the number of functional CYP2D6 genes could explain 21 % of the total interindividual variance in oral clearance of nortriptyline and 34% of that in steady-state plasma concentrations.

Conclusion

Nonlinear mixed-effects modelling can be used to quantify the influence of the number of functional CYP2D6 genes on the metabolic clearance and plasma concentration of drugs metabolised by this enzyme. Gene dose has a significant impact on drug pharmacokinetics and prior knowledge of it may aid in predicting plasma concentration of the drug and thus tailoring patient-specific dosage regimens.

Sjöqvist F, Hammer W. Plasma levels of monomethylated anti-depressants during treatment with imipramine compounds. Life Sci 1967; 6(17): 1895–903PubMedCrossRef

Asberg M, Evans DA, Sjöqvist F. Genetic control of nortriptyline kinetics in man: a study of relatives of propositi with high plasma concentration. J Med Gen 1971; 8(2): 129–35CrossRef

Alexanderson B, Evans DA, Sjöqvist F. Steady-state plasma levels of nortriptyline in twins: influence of genetic factors and drug therapy. BMJ 1969; 4(686): 764–8PubMedCrossRef

Mellström B, Bertilsson L, Säwe J, et al. E- and Z-10 hydroxylation of nortriptyline: relationship to polymorphic debrisoquine hydroxylation. Clin Pharmacol Ther 1981; 30(2): 189–93PubMedCrossRef

Steiner E, Bertilsson L, Säwe J, et al. Polymorphic debrisoquine hydroxylation in 757 Swedish subjects. Clin Pharmacol Ther 1988; 44(4): 431–5PubMedCrossRef

Alván G, Bechtel P, Iselius L, et al. Hydroxylation polymorphisms of debrisoquine and mephenytoin in European populations. Eur J Clin Pharmacol 1990; 39(6): 533–7PubMedCrossRef

Marez D, Legrand M, Sabbagh N, et al. Polymorphism of the cytochrome P450 CYP2D6 gene in a European population: characterization of 48 mutations and 53 alleles, their frequency and evolution. Pharmacogenetics 1997; 7(3): 193–202PubMedCrossRef

Johansson I, Lundquist E, Bertilsson L, et al. Inherited amplification of an active gene in the cytochrome P450 CYP2D locus as a cause of ultrarapid metabolism of debrisoquine. Prod Natl Acad Sci USA 1993; 90(24): 11825–9CrossRef

Dahl ML, Johansson I, Bertilsson L, et al. Ultrarapid hydroxylation of debrisoquine in a Swedish population. Analysis of the molecular genetic basis. J Pharmacol Exp Ther 1995; 274(1): 516–20PubMed

10.

Agúndez JAG, Ledesma MC, Ladero JM, et al. Prevalence of CYP2D6 gene duplication and its repercussion on the oxidative phenotype in a white population. Clin Pharmacol Ther 1995; 57(3): 265–9PubMedCrossRef

11.

Bernai ML, Sinues B, Johansson I, et al. Ten percent of north Spanish individuals carry duplicated or triplicated CYP2D6 genes associated with ultrarapid metabolism of debrisoquine. Pharmacogenetics 1999; 9(5): 657–60CrossRef

12.

Scordo MG, Spina E, Facciolà, et al. Cytochrome P450 2D6 genotype and steady state plasma levels of risperidone and 9-hydroxyrisperidone. Psychopharmacology 1999; 147(3): 300–5PubMedCrossRef

13.

Dahl ML, Bertilsson L, Nordin C. Steady-state plasma levels of nortriptyline and its 10-hydroxy metabolite: relationship to the CYP2D6 genotype. Psychopharmacology 1996; 123(4): 315–9PubMedCrossRef

14.

Dalén P, Dahl ML, Bernal-Ruiz ML. 10-hydroxylation of nortriptyline in white persons with 0, 1,2, 3, and 13 functional CYP2D6 genes. Clin Pharmacol Ther 1998; 63(4): 444–52PubMedCrossRef

15.

Morita S, Shimoda K, Someya T, et al. Steady state plasma levels of nortriptyline and its hydroxylated metabolites in Japanese patients: impact of CYP2D6 genotype on the hydroxylation of nortriptyline. J Clin Psychopharmacol 2000; 20(2): 141–9PubMedCrossRef

16.

Nordin C, Siwers B, Benitez J, et al. Plasma concentraion of nortriptyline and its 10-hydroxymetabolite in depressed patients — relationship to the debrisoquine hydroxylation ratio. Br J Clin Pharmacol 1985; 19: 832–5PubMedCrossRef

17.

Nordin C, Bertilsson L, Siwers B. Clinical and biochemical effects during treatment of depression with nortriptyline: the role of 10-hydroxynortriptyline. Clin Pharmacol Ther 1987; 42: 10–9PubMedCrossRef

18.

Meyer U-A, Heim M. Genotyping of poor metabolisers of debrisoquine by allele-specific PCR amplification. Lancet 1990; 336(8714): 529–32PubMedCrossRef

19.

Dahl ML, Johansson I, Porsmyr-Palmertz M, et al. Analysis of the CYP2D6 gene in relation to debrisoquin and desipramine hydroxylation in a Swedish population. Clin Pharmacol Ther 1992; 51(1): 12–7PubMedCrossRef

20.

Beal LS, Boeckmann JA, Sheiner LB. NONMEM users guide: part V. San Francisco (CA): University of California, 1994

21.

WinNonlin Reference guide-version 3.0. San Francisco (CA): Pharsight Corporation, 1998–1999

22.

Rowland M, Tozer TN. Clinical pharmacokinetics concepts and applications. 3rd ed. Baltimore (MD): Williams & Wilkins, 1995

23.

Rowland M, Pang SK. Hepatic clearance of drugs: I. Theoretical considerations of a ‘well-stirred’ model and a ‘parallel tube’ model. Influence of hepatic blood flow, plasma and blood cell binding, and the hepatocellular enzymatic activity on hepatic drug clearance. J Pharmacokinet Biopharm 1977; 5(6): 625–53PubMed

24.

Rowland M, Pang SK. Hepatic clearance of drugs: II. Experimental evidence for acceptance of the ‘well-stirred’ model over the ‘parallel tube’ model using lidocaine in the perfused rat liver in situ preparation. J Pharmacokinet Biopharm 1977; 5(6): 655–80PubMed

25.

Rowland M, Pang SK. Hepatic clearance of drugs: III. Additional experimental evidence supporting the ‘well-stirred’ model using metabolite (MEGX) generated from lidocaine under varying hepatic blood flow rates and linear conditions in the perfused rat liver in situ preparations. J Pharmacokinet Biopharm 1977; 5(6): 681–99PubMed

26.

Wagner JG. Modelling first-pass metabolism. Life Sci 1988; 145: 129–49

27.

Guyton CA, Hall JE. Textbook of medical physiology. 10th ed. Philadelphia (PA): WB. Saunders Company, 2000: 176

28.

Alexanderson B, Borgå O, Alvan G. The availability of orally administered nortriptyline. Eur J Clin Pharmacol 1973; 5: 181–5CrossRef

29.

Gram LF, Overø-Fredricson K. First-pass metabolism of nortriptyline in man. Clin Pharmacol Ther 1975; 18(3): 305–14PubMed

30.

Alvan G, Borgå M, Palmer L, et al. First pass hydroxylation of nortriptyline: concentration of parent drug and major metabolites in plasma. Eur J Clin Pharmacol 1977; 11: 219–24PubMedCrossRef

31.

Olesen OV, Linnet K. Hydroxylation and demethylation of the tricyclic antidepressant nortriptyline by cDNA-expressed human cytochrome P-450 isoenzymes. Drug Metab Dispos 1997; 25(6): 740–4PubMed

32.

Venkatakrishnan K, von Moltke LL, Greenblatt DJ. Nortriptyline E-10-hydroxylation in vitro is mediated by human CYP2D6 (high affinity) and CYP3A4 (low affinity): implications for interactions with enzyme-inducing drugs. J Clin Pharmacol 1999; 39(6): 567–77PubMedCrossRef

33.

Jerling M, Alván G. Nonlinear kinetics of nortriptyline in relation to nortriptyline clearance as observed during therapeutic drug monitoring. Eur J Clin Pharmacol 1994; 46(1): 67–70PubMedCrossRef

34.

Jerling M, Merlé Y, Mentré F, et al. Population pharmacokinetics of nortriptyline during monotherapy and during concomitant treatment with the nonparametric maximum likelihood method. Br J Clin Pharmacol 1994; 38(5): 453–62PubMedCrossRef

Titel: Quantitative Pharmacogenetics of Nortriptyline
A Novel Approach
verfasst von: Elin E. Kvist
Ayman Al-Shurbaji
Marja-Liisa Dahl
Conny Nordin
Gunnar Alván
Dr Lars Ståhle
Publikationsdatum: 01.11.2001
Verlag: Springer International Publishing
Erschienen in: Clinical Pharmacokinetics / Ausgabe 11/2001
Print ISSN: 0312-5963
Elektronische ISSN: 1179-1926
DOI: https://doi.org/10.2165/00003088-200140110-00005

Live-Webinar "Chronische Unterbauch- und Viszeralschmerzen in der Praxis managen"

Springer Medizin

Quantitative Pharmacogenetics of Nortriptyline

A Novel Approach

Abstract

Objective

Design

Participants

Methods

Results

Conclusion

Live-Webinar "Chronische Unterbauch- und Viszeralschmerzen in der Praxis managen"

Springer Medizin

Abstract

Objective

Design

Participants

Methods

Results

Conclusion

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