Investigation into UDP-Glucuronosyltransferase (UGT) Enzyme Kinetics of Imidazole- and Triazole-Containing Antifungal Drugs in Human Liver Microsomes and Recombinant UGT Enzymes

Bourcier, Karine; Hyland, Ruth; Kempshall, Sarah; Jones, Russell G.; Maximilien, Jacqueline; Irvine, Nicola; Jones, Barry

doi:10.1124/dmd.109.030676

Cited by 50 publications

(39 citation statements)

References 28 publications

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“…Expected CL R is the renal plasma clearance expected due to GFR if there was no reabsorption or tubular secretion (expected CL R = fraction unbound × GFR = f u × 110 mL/minute). Metabolism was attributed to glucuronidation via UGT2B7, and unbound intrinsic clearance (

{CL}_{normalI}^{'}

) was calculated using hepatic clearance (CL H ) 24. The CL H was assumed to be 15% of total empiric clearance 23.…”

Section: Methodsmentioning

confidence: 99%

Physiologically Based Pharmacokinetic Approach to Determine Dosing on Extracorporeal Life Support: Fluconazole in Children on ECMO

Watt

Cohen‐Wolkowiez

Barrett

et al. 2018

CPT Pharmacom & Syst Pharma

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Extracorporeal life support (e.g., dialysis, extracorporeal membrane oxygenation (ECMO)) can affect drug disposition, placing patients at risk for therapeutic failure. In this population, dose selection to achieve safe and effective drug exposure is difficult. We developed a novel and flexible approach that uses physiologically based pharmacokinetic (PBPK) modeling to translate results from ECMO ex vivo experiments into bedside dosing recommendations. To determine fluconazole dosing in children on ECMO, we developed a PBPK model, which was validated using fluconazole pharmacokinetic (PK) data in adults and critically ill infants. Next, an ECMO compartment was added to the PBPK model and parameterized using data from a previously published ex vivo study. Simulations using the final ECMO PBPK model reasonably characterized observed PK data in infants on ECMO, and the model was used to derive dosing in children on ECMO across the pediatric age spectrum. This approach can be generalized to other forms of extracorporeal life support (ECLS), such as dialysis.

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{CL}_{normalI}^{'}

) was calculated using hepatic clearance (CL H ) 24. The CL H was assumed to be 15% of total empiric clearance 23.…”

Section: Methodsmentioning

confidence: 99%

Physiologically Based Pharmacokinetic Approach to Determine Dosing on Extracorporeal Life Support: Fluconazole in Children on ECMO

Watt

Cohen‐Wolkowiez

Barrett

et al. 2018

CPT Pharmacom & Syst Pharma

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“…76 Voriconazole is also a low-affinity substrate for UGT1A4 in vitro. 49 An understanding of how genetic polymorphism affects voriconazole metabolism has been pivotal in explaining the pharmacokinetic variability observed in patients. The occurrence of genetic variants in the CYP alleles (Table 4) has a significant impact on the levels of drug achieved in those patients and probably upon the therapeutic efficacy of voriconazole.…”

Section: Anidulafunginmentioning

confidence: 99%

“…59 Recently, itraconazole was shown to be a substrate for the phase II enzyme UGT1A4, with an affinity similar to that of the imidazole antifungal agents, and it may also be an inhibitor of UGT1A4. 49 Itraconazole interacts with several genetically variable drug transporters and CYP enzymes, thus implicating them in the observed variability of itraconazole levels. Moreover, because CYP3A4 and P-glycoprotein also play a crucial role in the metabolism of many other drugs used in HSCT patients, this effect is likely to be compounded.…”

Section: Triazole Antifungalsmentioning

confidence: 99%

“…Its ability to inhibit 2C9 and 2C19 causes potential drug interactions particularly relevant to HSCT recipients; for example, the interaction with CY may result in increased formation of toxic metabolites, 47 although others have noted a protective effect of co-administration. 48 Fluconazole is both a substrate 49 and an inhibitor 50 of the UGT isoform, UGT2B7, the enzyme involved in its metabolism to the urinary metabolite fluconazole glucuronide. 43 It also inhibits UGT2B4, hence inhibiting, for example, the glucuronidation of codeine that may potentiate codeine-induced analgesia.…”

Section: Triazole Antifungalsmentioning

confidence: 99%

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Has the era of individualised medicine arrived for antifungals? A review of antifungal pharmacogenomics

Ashbee

Gilleece

2011

Bone Marrow Transplant

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“…The disposition and clearance of drugs may be significantly changed when UGT are modulated by co-administrated drugs or herbal medicines. For example, fluconazole itself is not metabolized by UGT but alter pharmacokinetic parameters of co-administrated zidovudine in AIDS patients, because the glucuronidation of zidovudine by UGT2B7 is strongly inhibited by fluconazole [12]; indinavir Although much research has been carried on the in vitro and in vivo metabolism profiles of AST and CAG, only a few articles that deal with metabolism enzymes elucidate the potential toxicity and herb-drug interactions. Shan et al [10] reported that AST was a competitive inhibitor of CYP2C9 and a non-competitive inhibitor of CYP3A4 in an in vitro study.…”

Section: Introductionmentioning

confidence: 99%

Evaluation and Comparison of the Inhibition Effect of Astragaloside IV and Aglycone Cycloastragenol on Various UDP-Glucuronosyltransferase (UGT) Isoforms

Ran

Zhang

et al. 2016

Molecules

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As one of the main active ingredients from Radix Astragali (RA), orally dosed astragaloside IV (AST) is easily transformed to sapogenin-cycloastragenol (CAG) by deglycosylation in the gastrointestinal tract. Because the potential adverse effects of AST and CAG remain unclear, the present study in this article was carried out to investigate the inhibition effects of AST and CAG on UDP-glucuronosyltransferases (UGTs) to explore potential clinical toxicity. An in vitro UGTs incubation mixture was employed to study the inhibition of AST and CAG towards UGT isoforms. Concentrations of 100 µM for each compound were used to initially screen the inhibitory efficiency. Deglycosylation of AST to CAG could strongly increase the inhibitory effects towards almost all of the tested UGT isoforms, with an IC 50 of 0.84 µM and 11.28 µM for UGT1A8 and UGT2B7, respectively. Ulteriorly, the inhibition type and kinetics of CAG towards UGT1A8 and UGT2B7 were evaluated depending on the initial screening results. Data fitting using Dixon and Lineweaver-Burk plots demonstrated that CAG competitively inhibited UGT1A8 and noncompetitively inhibited UGT2B7. From the second plot drawn with the slopes from the Lineweaver-Burk plot versus the concentrations of CAG, the inhibition constant (Ki) was calculated to be 0.034 µM and 20.98 µM for the inhibition of UGT1A8 and UGT2B7, respectively. Based on the [I]/Ki standard ([I]/Ki < 0.1, low possibility; 1 > [I]/Ki > 0.1, medium possibility; [I]/Ki > 1, high possibility), it was successfully predicted here that an in vivo herb-drug interaction between AST/CAG and drugs mainly undergoing UGT1A8-or UGT2B7-catalyzed metabolism might occur when the plasma concentration of CAG is above 0.034 µM and 20.98 µM, respectively.

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Investigation into UDP-Glucuronosyltransferase (UGT) Enzyme Kinetics of Imidazole- and Triazole-Containing Antifungal Drugs in Human Liver Microsomes and Recombinant UGT Enzymes

Cited by 50 publications

References 28 publications

Physiologically Based Pharmacokinetic Approach to Determine Dosing on Extracorporeal Life Support: Fluconazole in Children on ECMO

Physiologically Based Pharmacokinetic Approach to Determine Dosing on Extracorporeal Life Support: Fluconazole in Children on ECMO

Has the era of individualised medicine arrived for antifungals? A review of antifungal pharmacogenomics

Evaluation and Comparison of the Inhibition Effect of Astragaloside IV and Aglycone Cycloastragenol on Various UDP-Glucuronosyltransferase (UGT) Isoforms

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