2003
DOI: 10.1016/s0003-9861(02)00548-9
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Substrate selectivity of human cytochrome P450 2C9: importance of residues 476, 365, and 114 in recognition of diclofenac and sulfaphenazole and in mechanism-based inactivation by tienilic acid

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Cited by 100 publications
(97 citation statements)
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References 59 publications
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“…Studies with sulfaphenazole, a well known competitive inhibitor of CYP2C9, and a high affinity substrate of CYP2C9 exhibited a K i value of 0.3 M and IC 50 of 0.6 M (Mancy et al, 1996;Ha-Duong et al, 2001a;Melet et al, 2003). The IC 50 value (0.84 M) we obtained for the inhibition of thioether sulfoxidation of disulfoton by sulfaphenazole indicates that these thioether substrates are competing for the same catalytic site as other high affinity CYP2C9 substrates.…”
Section: In Vitro Thioether Sulfoxidation In Humansmentioning
confidence: 66%
See 1 more Smart Citation
“…Studies with sulfaphenazole, a well known competitive inhibitor of CYP2C9, and a high affinity substrate of CYP2C9 exhibited a K i value of 0.3 M and IC 50 of 0.6 M (Mancy et al, 1996;Ha-Duong et al, 2001a;Melet et al, 2003). The IC 50 value (0.84 M) we obtained for the inhibition of thioether sulfoxidation of disulfoton by sulfaphenazole indicates that these thioether substrates are competing for the same catalytic site as other high affinity CYP2C9 substrates.…”
Section: In Vitro Thioether Sulfoxidation In Humansmentioning
confidence: 66%
“…Considerable interest has recently been focused on CYP2C subfamily members not only because of their involvement in the oxidation of a number of clinically used drugs but also due to the discovery of numerous polymorphic forms and substrate recognition sites within these isoforms. Molecular modeling techniques have also been employed to derive predictive models for CYP2C substrates, particularly CYP2C9 (Mancy et al, 1995;Mancy et al, 1996;Poli-Scaife et al, 1997;Ha-Duong et al, 2001b;Melet et al, 2003). The thioether compounds used in the present study were not previously known as CYP2C substrates and do not fit well within the previous predictive models for CYP2C isoform substrates.…”
Section: Ethyl] Phosphorodithioate) and Sulprofos (O-ethyl O-[4-(metmentioning
confidence: 99%
“…With the exception of ticlopidine/CYP2C19 and rotonavir/CYP3A, for those combinations where inactivation was expected the percentage of decrease in activity was at least 30%. These include furafylline and zileuton (CYP1A2) (Racha et al, 1998;Lu et al, 2003), ticlopidine, PPP, and N,NЈ,NЉ-triethylenethiophosphoramide (thioTEPA) (CYP2B6) (Chun et al, 2000;Richter et al, 2004Richter et al, , 2005, desethylamiodarone (CYP2C8) (Polasek et al, 2004), tienilic acid (CYP2C9) (Melet et al, 2003), methylenedioxymethamphetamine (MDMA) and paroxetine (CYP2D6) (Bertelsen et al, 2003;Heydari et al, 2004), and diltiazem, erythromycin, and verapamil (CYP3A) (Mayhew et al, 2000;McConn et al, 2004;Wang et al, 2004;Ernest et al, 2005). With a few exceptions (e.g., desethylamiodarone, thioTEPA), these compounds did not show appreciable inactivation for other P450 enzymes.…”
Section: Downloaded Frommentioning
confidence: 99%
“…e) 4′-Hydroxylation of diclofenac-Diclofenac hydroxylation by CYP2C9 was carried out using a previously reported protocol [46] (15 μM substrate, 20 nM CYP2C9, 10 min at 28°C…”
Section: Origins Of Recombinant Cytochromes P450mentioning
confidence: 99%