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Verfasst von:Geist, Marcus Julian Peter [VerfasserIn]   i
 Ziesenitz, Victoria C. [VerfasserIn]   i
 Bardenheuer, Hubert J. [VerfasserIn]   i
 Burhenne, Jürgen [VerfasserIn]   i
 Skopp, Gisela [VerfasserIn]   i
 Mikus, Gerd [VerfasserIn]   i
Titel:Minor contribution of cytochrome P450 3A activity on fentanyl exposure in palliative care cancer patients
Verf.angabe:Marcus J.P. Geist, Victoria C. Ziesenitz, Hubert J. Bardenheuer, Juergen Burhenne, Gisela Skopp & Gerd Mikus
E-Jahr:2019
Jahr:10 October 2019
Umfang:6 S.
Teil:volume:9
 year:2019
 extent:6
Fussnoten:Gesehen am 10.12.2019
Titel Quelle:Enthalten in: Scientific reports
Ort Quelle:[London] : Macmillan Publishers Limited, part of Springer Nature, 2011
Jahr Quelle:2019
Band/Heft Quelle:9(2019) Artikel-Nummer 14635, 6 Seiten
ISSN Quelle:2045-2322
Abstract:Transdermal fentanyl is widely used to control pain in cancer patients. The high pharmacokinetic variability of fentanyl is assumed to be due to cytochrome P450 3A-mediated (CYP3A) N-dealkylation to norfentanyl in humans. However, recently published clinical studies question the importance of the described metabolic pathway. In this small study in palliative cancer patients under real-life clinical conditions, the influence of CYP3A on fentanyl variability was investigated. In addition to the determination of midazolam plasma concentration to reveal CYP3A activity, plasma concentrations of fentanyl and its metabolite, norfentanyl, were measured in identical blood samples of 20 patients who participated in an ongoing trial and had been on transdermal fentanyl. Fentanyl, norfentanyl, midazolam, and 1′-OH-midazolam were quantified by liquid chromatography/tandem mass spectrometry. Plasma concentrations of fentanyl and norfentanyl exhibited a large variability. Mean estimated total clearance of fentanyl and mean metabolic clearance of midazolam (as a marker of CYP3A activity) were 75.5 and 36.3 L/h. Both clearances showed a weak correlation and hence a minimal influence of CYP3A on fentanyl elimination.
DOI:doi:10.1038/s41598-019-51279-6
URL:Kostenfrei: Volltext ; Verlag: https://doi.org/10.1038/s41598-019-51279-6
 Kostenfrei: Volltext: https://www.nature.com/articles/s41598-019-51279-6
 DOI: https://doi.org/10.1038/s41598-019-51279-6
Datenträger:Online-Ressource
Sprache:eng
K10plus-PPN:1685085881
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