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@inproceedings{560182,
author = {Hadašová, Eva and Dostálek, Miroslav and Juřica, Jan and Tomandl, Josef and Minaříková, Veronika},
address = {Antalya (Turecko)},
booktitle = {19th European Workshop on Drug Metabolism. Abstract & Program Book.},
keywords = {drug metabolism; methamphetamine; dextromethorphan; midazolam; CYP2D6; CYP3A4; pharmacokinetics;},
language = {eng},
location = {Antalya (Turecko)},
pages = {194-194},
publisher = {Tubitak},
title = {METHAMPHETAMINE-INDUCED CHANGES IN DEXTROMETHORPHAN AND MIDAZOLAM METABOLISM IN RATS: A PHARMACOKINETIC STUDY},
year = {2004}
}
TY - JOUR
ID - 560182
AU - Hadašová, Eva - Dostálek, Miroslav - Juřica, Jan - Tomandl, Josef - Minaříková, Veronika
PY - 2004
TI - METHAMPHETAMINE-INDUCED CHANGES IN DEXTROMETHORPHAN AND MIDAZOLAM METABOLISM IN RATS: A PHARMACOKINETIC STUDY
PB - Tubitak
CY - Antalya (Turecko)
KW - drug metabolism
KW - methamphetamine
KW - dextromethorphan
KW - midazolam
KW - CYP2D6
KW - CYP3A4
KW - pharmacokinetics;
N2 - Methamphetamine (pervitine) is one of the most frequently abused substances. The drug is metabolized by the hepatic cytochromes P450, mainly by CYP2D and CYP3A. The present pharmacokinetic study in the rat investigated the possible influence of methamphetamine on metabolic fates of model substrates for CYP3A1/2 and CYP2D1/2. The pharmacokinetic analysis showed a marked stimulatory effect of methamphetamine on CYP2D1/2, as it was previously demonstrated by us in the isolated perfused rat liver. Similarly, the midazolam kinetics (marker of CYP3A1/2 activity) showed a significantly increased CYP3A-mediated metabolism. The results may have clinical impact in pharmacotherapy of methamphetamine abusers.
ER -
HADAŠOVÁ, Eva, Miroslav DOSTÁLEK, Jan JUŘICA, Josef TOMANDL a Veronika MINAŘÍKOVÁ. METHAMPHETAMINE-INDUCED CHANGES IN DEXTROMETHORPHAN AND MIDAZOLAM METABOLISM IN RATS: A PHARMACOKINETIC STUDY. In \textit{19th European Workshop on Drug Metabolism. Abstract \&{} Program Book.}. Antalya (Turecko): Tubitak, 2004, s.~194-194.
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