Universität zu Köln

Li, Xia, Junge, Lisa, Taubert, Max ORCID: 0000-0001-8925-7782, von Georg, Anabelle, Dahlinger, Dominik, Starke, Chris, Frechen, Sebastian, Stelzer, Christoph, Kinzig, Martina, Soergel, Fritz, Jaehde, Ulrich, Toex, Ulrich, Goeser, Tobias and Fuhr, Uwe (2020). A Novel Study Design Using Continuous Intravenous and Intraduodenal Infusions of Midazolam and Voriconazole for Mechanistic Quantitative Assessment of Hepatic and Intestinal CYP3A Inhibition. J. Clin. Pharmacol., 60 (9). S. 1237 - 1254. HOBOKEN: WILEY. ISSN 1552-4604

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Abstract

The extent of a drug-drug interaction (DDI) mediated by cytochrome P450 (CYP) 3A inhibitors is highly variable during a dosing interval, as it depends on the temporal course of victim and perpetrator drug concentrations at intestinal and hepatic CYP3A expression sites. Capturing the time course of inhibition is therefore difficult using standard DDI studies assessing changes in area under the curve; thus, a novel design was developed. In a 4-period changeover pilot study, 6 healthy men received intraduodenal or intravenous infusions of the CYP3A substrate midazolam (MDZ) at a rate of 0.26 mg/h for 24 hours. This was combined with intraduodenal or intravenous infusion of the CYP3A inhibitor voriconazole (VRZ), administered at rates of 7.5 mg/h from 8 to 16 hours and of 15 mg/h from 16 to 24 hours, after starting midazolam administration. Plasma and urine concentrations of VRZ, MDZ, and its major metabolites were quantified by liquid chromatography-tandem mass spectrometry and analyzed by semiphysiological population pharmacokinetic nonlinear mixed-effects modeling. A model including mechanism-based inactivation of the metabolizing enzymes (maximum inactivation rate constant k(inact), 2.83 h(-1); dissociation rate constant KI, 9.33 mu M) described the pharmacokinetics of VRZ well. By introducing competitive inhibition by VRZ on primary and secondary MDZ metabolism, concentration-time profiles, MDZ and its metabolites were captured appropriately. The model provides estimates of local concentrations of substrate and inhibitor at the major CYP3A expression sites and thus of the respective dynamic extent of inhibition. A combination of intravenous and intraduodenal infusions of inhibitors and substrates has the potential to provide a more accurate assessment of DDIs occurring in both gut wall and liver.

Item Type:	Journal Article
Creators:	Creators Email ORCID ORCID Put Code Li, Xia UNSPECIFIED UNSPECIFIED UNSPECIFIED Junge, Lisa UNSPECIFIED UNSPECIFIED UNSPECIFIED Taubert, Max UNSPECIFIED orcid.org/0000-0001-8925-7782 UNSPECIFIED von Georg, Anabelle UNSPECIFIED UNSPECIFIED UNSPECIFIED Dahlinger, Dominik UNSPECIFIED UNSPECIFIED UNSPECIFIED Starke, Chris UNSPECIFIED UNSPECIFIED UNSPECIFIED Frechen, Sebastian UNSPECIFIED UNSPECIFIED UNSPECIFIED Stelzer, Christoph UNSPECIFIED UNSPECIFIED UNSPECIFIED Kinzig, Martina UNSPECIFIED UNSPECIFIED UNSPECIFIED Soergel, Fritz UNSPECIFIED UNSPECIFIED UNSPECIFIED Jaehde, Ulrich UNSPECIFIED UNSPECIFIED UNSPECIFIED Toex, Ulrich UNSPECIFIED UNSPECIFIED UNSPECIFIED Goeser, Tobias UNSPECIFIED UNSPECIFIED UNSPECIFIED Fuhr, Uwe UNSPECIFIED UNSPECIFIED UNSPECIFIED
URN:	urn:nbn:de:hbz:38-333497
DOI:	10.1002/jcph.1619
Journal or Publication Title:	J. Clin. Pharmacol.
Volume:	60
Number:	9
Page Range:	S. 1237 - 1254
Date:	2020
Publisher:	WILEY
Place of Publication:	HOBOKEN
ISSN:	1552-4604
Language:	English
Faculty:	Unspecified
Divisions:	Unspecified
Subjects:	no entry
Uncontrolled Keywords:	Keywords Language IN-VIVO PROBE; PHARMACOKINETIC MODEL; CYTOCHROME-P450 3A; 1ST-PASS METABOLISM; HUMAN LIVER; VITRO; BIOAVAILABILITY; PERFORMANCE; PREDICTION; IMPACT Multiple languages Pharmacology & Pharmacy Multiple languages
URI:	http://kups.ub.uni-koeln.de/id/eprint/33349