Selective Mechanism-Based Inactivation of CYP3A4 by CYP3cide (PF-04981517) and Its Utility as an In Vitro Tool for Delineating the Relative Roles of CYP3A4 versus CYP3A5 in the Metabolism of Drugs

Walsky, Robert L.; Obach, R. Scott; Hyland, Ruth; Kang, Ping; Zhou, Sue; West, Michael; Geoghegan, Kieran F.; Helal, Christopher J.; Walker, Gregory S.; Goosen, Theunis C.; Zientek, Michael

doi:10.1124/dmd.112.045302

Cited by 77 publications

(81 citation statements)

References 43 publications

(42 reference statements)

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“…Among the selective inhibitors tested, ketoconazole (CYP3A inhibitor) strongly inhibited the catalytic activity of HLM, further implying the prominent role of CYP3A in RB hydroxylation. Furthermore, CYP3cide, a potent and specific time-dependent inhibitor of CYP3A4 (Walsky et al, 2012), exhibited similar inhibitory effects on RB 5b-hydroxlation in HLM and rhCYP3A4 (Supplemental Fig. 1).…”

Section: Resultsmentioning

confidence: 83%

“…The selective inhibitors and their concentrations were as follows (Bjornsson et al, 2003): montelukast (2 mM) for CYP2C8 (Walsky et al, 2005), sulfaphenazole (10 mM) for CYP2C9, omeprazole (20 mM) for CYP2C19, quinidine (10 mM) for CYP2D6, clomethiazole (50 mM) for CYP2E1, ketoconazole (1 mM) for CYP3A. Inhibition by furafylline (10 mM) for CYP1A2, 8-methoxypsoralen (2.5 mM) for CYP2A6, TEPA (50 mM) for CYP2B6 (Rae et al, 2002), CYP3cide (2 mM) for CYP3A4 (Walsky et al, 2012) and ABT (500 mM) for broad P450s (Emoto et al, 2003) were examined by adding RB after preincubation with NADPH-generating system at 37°C for 40 minutes.…”

Section: In Vitro Metabolism Of Resibufogeninmentioning

confidence: 99%

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Characterization of Phase I Metabolism of Resibufogenin and Evaluation of the Metabolic Effects on Its Antitumor Activity and Toxicity

Ning

et al. 2014

Drug Metab Dispos

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Resibufogenin (RB), one of the major active compounds of the traditional Chinese medicine Chansu, has displayed great potential as a chemotherapeutic agent in oncology. However, it is a digoxinlike compound that also exhibits extremely cardiotoxic effects. The present study aimed to characterize the metabolic behaviors of RB in humans as well as to evaluate the metabolic effects on its bioactivity and toxicity. The phase I metabolic profile in human liver microsomes was characterized systemically, and the major metabolite was identified as marinobufagenin (5b-hydroxylresibufogenin, 5-HRB) by liquid chromatography-mass spectrometry and nuclear magnetic imaging techniques. Both cytochrome P450 (P450) reaction phenotyping and inhibition assays using P450-selective chemical inhibitors demonstrated that CYP3A4 was mainly involved in RB 5b-hydroxylation with much higher selectivity than CYP3A5. Kinetic characterization demonstrated that RB 5b-hydroxylation in both human liver microsomes and human recombinant CYP3A4 obeyed biphasic kinetics and displayed similar apparent kinetic parameters. Furthermore, 5-HRB could significantly induce cell growth inhibition and apoptosis in A549 and H1299 by facilitating apoptosome assembly and caspase activation. Meanwhile, 5-HRB displayed very weak cytotoxicity of human embryonic lung fibroblasts, and in mice there was a greater tolerance to acute toxicity. In summary, CYP3A4 dominantly mediated 5b-hydroxylation and was found to be a major metabolic pathway of RB in the human liver, whereas its major metabolite (5-HRB) displayed better druglikeness than its parent compound RB. Our findings lay a solid foundation for RB metabolism studies in humans and encourage further research on the bioactive metabolite of RB.

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Section: Resultsmentioning

confidence: 83%

Section: In Vitro Metabolism Of Resibufogeninmentioning

confidence: 99%

Characterization of Phase I Metabolism of Resibufogenin and Evaluation of the Metabolic Effects on Its Antitumor Activity and Toxicity

Ning

et al. 2014

Drug Metab Dispos

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“…Clinical results indicated no clear correlation of CYP3A5 polymorphisms with variability in axitinib pharmacokinetics (Brennan et al, 2012), indicating CYP3A5 may have a rather small clinical contribution to overall oral clearance. Recently, in vitro tools to confirm or refute the contribution of CYP3A5 have been made available via the use of CYP3cide, a specific CYP3A4 inhibitor (Walsky et al, 2012b). When axitinib was assessed using CYP3cide, in tandem with CYP3A5-genotyped donor pools of microsomes (CYP3A5 *1/*1 and *3/*3) and axitinib substrate loss was followed over time.…”

Section: Discussionmentioning

confidence: 99%

“…These CYP3cide substrate depletion studies were not conducted with a dilution step, which if diluted would minimize any time-dependent effects of CYP3cide on CYP3A5 activity. The absence of the dilution step method has been shown to be an effective method for delineating CYP3A5 contribution from CYP3A4 (Walsky et al, 2012b), especially when combined with quantifying the metabolite formation in the presence and absence of inhibitors at a time point where relatively little loss of the parent compound is observed. When comparing the data from the formation of the sulfoxide metabolite, a similar contribution of CYP3A5 (18%) was noted to that of the parent loss method.…”

Section: Discussionmentioning

confidence: 99%

“…Axitinib (1.0 mM) was incubated, in triplicate, with pooled lots of HLM CYP3A5 *1/*1 (from five donors, see the Materials section) and HLM CYP3A5 *3/*3 (from six donors, see the Materials section) at a protein concentration of 1 mg/ml for measurement of intrinsic clearance (Cl int ) in the presence and absence of chemical inhibitors, essentially as previously described (Walsky et al, 2012b;Tseng et al, 2014). Incubations were carried out in triplicate in 100 mM KH 2 PO 4 (pH 7.4) containing MgCl 2 (3.3 mM), ketoconazole (2 mM), or CYP3cide (1 mM) and NADPH (1.3 mM) in a total volume of 0.3 ml.…”

Section: Delineation Of the Fraction Metabolized Via Cyp3a4 Versus Cymentioning

confidence: 99%

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In Vitro Kinetic Characterization of Axitinib Metabolism

Zientek

Goosen

Tseng

et al. 2015

Drug Metabolism and Disposition

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, respectively. Using a CYP3A4-specific inhibitor (Cyp3cide) in liver microsomes expressing CYP3A5, 66% of the axitinib intrinsic clearance was attributable to CYP3A4 and 15% to CYP3A5. Axitinib N-glucuronidation was primarily catalyzed by UDPglucuronosyltransferase (UGT) UGT1A1, which was verified by chemical inhibitors and UGT1A1 null expressers, with lesser contributions from UGTs 1A3, 1A9, and 1A4. The K m and V max values describing the formation of the N-glucuronide in HLM or rUGT1A1 were 2.7 mM or 0.75 mM and 8.9 or 8.3 pmol·min 21 ·mg 21 , respectively. In summary, CYP3A4 is the major enzyme involved in axitinib clearance with lesser contributions from CYP3A5, CYP2C19, CYP1A2, and UGT1A1.

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Target Enzyme‐Activated Two‐Photon Fluorescent Probes: A Case Study of CYP3A4 Using a Two‐Dimensional Design Strategy

Ning

Wang

et al. 2019

Angewandte Chemie

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The rapid development of fluorescent probes for monitoring target enzymes is still agreat challenge owingtothe lacko fe fficient ways to optimizeaspecific fluorophore. Herein, ap ractical two-dimensional strategy was designed for the development of an isoform-specific probe for CYP3A4, ak ey cytochrome P450 isoform responsible for the oxidation of most clinical drugs.Infirst dimension of the design strategy, ap otential two-photon fluorescent substrate (NN)f or CYP3A4 was effectively selected using ensemble-based virtual screening.Inthe second dimension, various substituent groups were introduced into NN to optimize the isoform-selectivity and reactivity.F inally,w ith ideal selectivity and sensitivity, NEN was successfully applied to the real-time detection of CYP3A4 in living cells and zebrafish. These findings suggested that our strategy is practical for developing an isoform-specific probe for atarget enzyme.Cytochrome P450 monooxygenase (CYP) is as uperfamily of oxidative enzymes that metabolizes thousands of endogenous and exogenous substances through alkyl carbon and aromatic ring hydroxylation, O-a nd N-dealkylation, and epoxidation. [1] CYP3A4 is regarded as the most important CYP isoform in humans owing to its high abundance in liver and broad substrate spectrum, which contributes to the metabolism of more than 50 %o fclinical drugs. [2,3] Unfortunately,C YP3A4 activity can be modulated by many clinical drugs,t hereby frequently causing unfavorable drug-drug interactions (DDI), further leading to altered clinical outcomes or even life-threatening adverse reactions. [4] Additionally,asignificant inter-individual variability of CYP3A4 activity is frequently reported, arising from an umber of sources including genetic polymorphism and the response to environmental influences. [5] These factors have greatly limited the understanding of the precise role of CYP3A4 in drug metabolism and DDI, as aresult, negatively impacted clinical medication safety and effectiveness.To accurately characterize CYP3A4 activity,s ensitive technologies capable of the real-time monitoring of CYP3A4 activity are urgently needed. Tr aditional detection methods mainly rely upon mass spectrometry or high-performance liquid chromatography, [6,7] which are not compatible with living cell or in vivo applications.T wo-photon (TP) fluorescence microscopy,byvirtue of its higher sensitivity,real-time high spatial resolution imaging,a nd amenability to deeptissue bioimaging,h as shed new light on the monitoring of target enzyme activity in complex systems. [8, 9] However,n o TP fluorescent probe has been developed for the real-time and selective imaging of endogenous CYP3A4 activity in living systems.Previous attempts to develop af luorescent probe for CYP3A4 were based on adealkylation mechanism to release ad etectable moiety.T he O-alkyl derivatives of coumarin, resorufin, and fluorescein were designed and synthesized but met with limited success in isoform selectivity. [10] Theleading cause for the poor specificity of these probes is th...

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Selective Mechanism-Based Inactivation of CYP3A4 by CYP3cide (PF-04981517) and Its Utility as an In Vitro Tool for Delineating the Relative Roles of CYP3A4 versus CYP3A5 in the Metabolism of Drugs

Cited by 77 publications

References 43 publications

Characterization of Phase I Metabolism of Resibufogenin and Evaluation of the Metabolic Effects on Its Antitumor Activity and Toxicity

Characterization of Phase I Metabolism of Resibufogenin and Evaluation of the Metabolic Effects on Its Antitumor Activity and Toxicity

In Vitro Kinetic Characterization of Axitinib Metabolism

Target Enzyme‐Activated Two‐Photon Fluorescent Probes: A Case Study of CYP3A4 Using a Two‐Dimensional Design Strategy

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