Enantiomeric Metabolic Interactions and Stereoselective Human Methadone Metabolism

Totah, Rheem A.; Allen, Kyle E.; Sheffels, Pamela; Whittington, Dale; Kharasch, Evan D.

doi:10.1124/jpet.106.117580

Cited by 100 publications

(141 citation statements)

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“…Assessed over broader methadone concentrations, in vitro intrinsic clearances for CYP2B6.6 and CYP2B6.9 were significantly lower than for CYP2B6.1. Stereoselectivity of methadone metabolism was maintained in all CYP2B6 variants, with S-methadone N-demethylation 2-fold greater than that of R-methadone, similar to that with CYP2B6.1 (Gerber et al, 2004;Totah et al, 2007Totah et al, , 2008Chang et al, 2011;Gadel et al, 2013). Lower rates of CYP2B6.6-catalyzed methadone Ndemethylation in the present investigation, in which insect cells were transfected with individual virus constructs for CYP2B6, P450 reductase, and cytochrome b 5 , were also seen in an insect cell system transfected with a single virus containing all three proteins (Gadel et al, 2013).…”

Section: Discussionmentioning

confidence: 80%

“…EDDP formation by CYP2B6 variants was compared by analysis of variance. EDDP formation versus substrate concentration data were analyzed by nonlinear regression analysis (SigmaPlot 12.5; Systat, San Jose, CA) evaluating a single-enzyme Michaelis-Menten, AdairPauling, or substrate (or product inhibition) model as described previously (Totah et al, 2007(Totah et al, , 2008Gadel et al, 2013). The choice of model was based on whether the Eadie-Hofstee plots were linear or nonlinear and the goodness of fit regression diagnostics.…”

Section: Methodsmentioning

confidence: 99%

“…Both methadone clearance and N-demethylation are stereoselective. Methadone N-demethylation in vitro, by human liver microsomes and by expressed cytochrome P450s (P450s), is catalyzed most efficiently by CYP2B6 and CYP3A4, and only CYP2B6 N-demethylates methadone stereoselectively (S.R) (Gerber et al, 2004;Kharasch et al, 2004;Totah et al, 2007Totah et al, , 2008Chang et al, 2011;Gadel et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

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Differences in Methadone Metabolism by CYP2B6 Variants

2015

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Methadone is a long-acting opioid with considerable unexplained interindividual variability in clearance. Cytochrome P450 2B6 (CYP2B6) mediates clinical methadone clearance and metabolic inactivation via N-demethylation to 2-ethyl-1,5-dimethyl-3,3-diphenylpyrrolidine (EDDP). Retrospective studies suggest that individuals with the CYP2B6*6 allelic variant have higher methadone plasma concentrations. Catalytic activities of CYP2B6 variants are highly substrate-and expression-system dependent. This investigation evaluated methadone N-demethylation by expressed human CYP2B6 allelic variants in an insect cell coexpression system containing P450 reductase. Additionally, the influence of coexpressing cytochrome b 5 , whose role in metabolism can be inhibitory or stimulatory depending on the P450 isoform and substrate, on methadone metabolism, was evaluated. EDDP formation from therapeutic (0.25-1 mM) R-and S-methadone concentrations was CYP2B6.4 ‡ CYP2B6.1 ‡ CYP2B6.5 >> CYP2B6.9 CYP2B6.6, and undetectable from CYP2B6.18. Coexpression of b 5 had small and variant-specific effects at therapeutic methadone concentrations but at higher concentrations stimulated EDDP formation by CYP2B6.1, CYP2B6.4, CYP2B6.5, and CYP2B6.9 but not CYP2B6.6. In vitro intrinsic clearances were generally CYP2B6.4 ‡ CYP2B6.1 > CYP2B6.5 > CYP2B6.9 ‡ CYP2B6.6. Stereoselective methadone metabolism (S>R) was maintained with all CYP2B6 variants. These results show that methadone N-demethylation by CYP2B6.4 is greater compared with CYP2B6.1, whereas CYP2B6.9 and CYP2B6.6 (which both contain the 516G>T, Q172H polymorphism), are catalytically deficient. The presence or absence of b 5 in expression systems may explain previously reported disparate catalytic activities of CYP2B6 variants for specific substrates. Differences in methadone metabolism by CYP2B6 allelic variants provide a mechanistic understanding of pharmacogenetic variability in clinical methadone metabolism and clearance.

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Section: Discussionmentioning

confidence: 80%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Differences in Methadone Metabolism by CYP2B6 Variants

2015

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“…Methadone clearance was doubled by efavirenz and rifampin, which induce CYP2B6, as well as CYP3A4, and by ritonavir, which induces CYP2B6 while inhibiting CYP3A (Kharasch et al, 2004a(Kharasch et al, , 2008a. Increasing the activity of CYP2B6, which metabolizes methadone stereoselectively (Gerber et al, 2004;Kharasch et al, 2004a;Totah et al, 2007Totah et al, , 2008Chang et al, 2011), increased plasma R/S methadone ratios (Kharasch et al, 2004a(Kharasch et al, , 2008a(Kharasch et al, ,c, 2012bTotah et al, 2008), whereas inhibiting CYP3A, which metabolizes methadone nonstereoselectively, did not (Kharasch et al, 2009a(Kharasch et al, ,b, 2012a. CYP2B6 inhibition by ticlopidine increased methadone enantiomers AUC and reduced methadone N-demethylation and clearance (Kharasch and Stubbert, 2013).…”

Section: Controlmentioning

confidence: 96%

“…CYP2B6 catalyzes methadone N-demethylation in vitro as avidly as CYP3A4 and CYP2B6 but not CYP3A4 is stereoselective (Gerber et al, 2004;Kharasch et al, 2004a;Totah et al, 2007Totah et al, , 2008Chang et al, 2011). Methadone clearance was doubled by efavirenz and rifampin, which induce CYP2B6, as well as CYP3A4, and by ritonavir, which induces CYP2B6 while inhibiting CYP3A (Kharasch et al, 2004a(Kharasch et al, , 2008a.…”

Section: Controlmentioning

confidence: 99%

Cytochrome P4503A Does Not Mediate the Interaction between Methadone and Ritonavir-Lopinavir

Kharasch

Stubbert

2013

Drug Metab Dispos

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Plasma concentrations of orally administered methadone are reduced by the human immunodeficiency virus protease inhibitor combination ritonavir and lopinavir, but the mechanism is unknown. Methadone metabolism, clearance, and drug interactions have been attributed to CYP3A4, but this remains controversial. This investigation assessed the effects of acute (2 days) and steady-state (2 weeks) ritonavirlopinavir on intravenous and oral methadone metabolism and clearance, hepatic and intestinal CYP3A4/5 activity (using the probe substrate intravenous and oral alfentanil), and intestinal transporter activity (using oral fexofenadine) in healthy volunteers. Plasma and urine concentrations of methadone and metabolite enantiomers, and other analytes, were determined by mass spectrometry. Acute and chronic ritonavir-lopinavir reduced plasma methadone enantiomer concentrations in half, with an average 2.6-and 1.5-fold induction of systemic and apparent oral methadone clearances. Induction was attributable to stereoselectively increased hepatic methadone N-demethylation, hepatic extraction, and hepatic clearance, and there was a strong correlation between methadone N-demethylation and clearance. Methadone renal clearance was unchanged. Alfentanil's systemic clearance and hepatic extraction, apparent oral clearance, and intestinal extraction were reduced to 25%, 16%, and 35% of control, indicating strong inhibition of hepatic and intestinal CYP3A activities. Ritonavir-lopinavir (acute > chronic) increased fexofenadine exposure, suggesting intestinal P-glycoprotein inhibition. No correlation was found between methadone clearance and CYP3A activity. Acute and steady-state ritonavir-lopinavir stereoselectively induced methadone N-demethylation and clearance, despite significant inhibition of hepatic and intestinal CYP3A activity. Ritonavir-lopinavir inhibited intestinal transporters activity but had no effect on methadone bioavailability. These results do not support a significant role for CYP3A or ritonavir-lopinavir-inhibitable intestinal transporters in single-dose methadone disposition.

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Oxidative Drug Metabolism by Mammalian CytochromeP450Enzymes Using Their Monooxygenase and Peroxygenase Functions

Hrycay

Bandiera

2017

Encyclopedia of Drug Metabolism and Interactions

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The cytochrome P450 (CYP) enzyme system represents the predominant biotransformation pathway in the human body for lipophilic exogenous and endogenous compounds. The monooxygenase reaction catalyzed by CYP enzymes involves the addition of one oxygen atom from molecular oxygen to a lipophilic substrate, while incorporating the other oxygen atom into a molecule of water, thereby leading to the production of more polar and easily excreted metabolites. Thus, CYP enzymes are major determinants of duration of action and clearance of drugs. In some cases, CYP enzymes are involved in the formation of chemically reactive and potentially toxic metabolites, as well as in clinically significant drug–drug interactions, which are a widely recognized cause of adverse drug reactions in humans. This chapter focuses on the oxidative biotransformation of therapeutic drugs catalyzed by human CYP enzymes. The topics covered include the identification of human hepatic and extrahepatic CYP enzymes involved in drug biotransformation, CYP bioactivation of prodrugs to pharmacologically active compounds, human CYP drug–drug interactions, CYP monooxygenase and peroxygenase reactions involving drug substrates, and mechanisms involved in CYP oxidative drug reactions.

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Enantiomeric Metabolic Interactions and Stereoselective Human Methadone Metabolism

Cited by 100 publications

References 31 publications

Differences in Methadone Metabolism by CYP2B6 Variants

Differences in Methadone Metabolism by CYP2B6 Variants

Cytochrome P4503A Does Not Mediate the Interaction between Methadone and Ritonavir-Lopinavir

Oxidative Drug Metabolism by Mammalian CytochromeP450Enzymes Using Their Monooxygenase and Peroxygenase Functions

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