THE INFLUENCE OF THE SPARTEINE DEBRISOQUINE GENETIC-POLYMORPHISM ON THE DISPOSITION OF DEXFENFLURAMINE/

Authors
GROSS AS PHILLIPS AC RIEUTORD A SHENFIELD GM
Citation
As. Gross et al., THE INFLUENCE OF THE SPARTEINE DEBRISOQUINE GENETIC-POLYMORPHISM ON THE DISPOSITION OF DEXFENFLURAMINE/, British journal of clinical pharmacology, 41(4), 1996, pp. 311-317
Citations number
26
Categorie Soggetti
Pharmacology & Pharmacy
Journal title
British journal of clinical pharmacologyACNP
ISSN journal
03065251
Volume
41
Issue
4
Year of publication
1996
Pages
311 - 317
Database
ISI
SICI code
0306-5251(1996)41:4<311:TIOTSD>2.0.ZU;2-Z
Abstract
1 To determine whether dexfenfluramine is a substrate of cytochrome P4 50 2D6 (CYP2D6), its disposition has been studied in nine extensive (E M) and eight poor metabolizers (PM) of debrisoquine. 2 Following a 30 mg dose of dexfenfluramine hydrochloride, urine was collected in all s ubjects for 96 h post-dose and plasma samples were collected in 11 sub jects (six EMs and five PMs). Dexfenfluramine and nordexfenfluramine w ere measured in urine by h.p.l.c. and in plasma by g.c. 3 Urinary reco very of dexfenfluramine was greater in PMs than EMs (4136+/-1509 mu g vs 1986+/-792 mu g; 95% CI of difference 926-3374; P<0.05) whereas tha t of nordexfenfluramine was similar in both phenotypes (PM: 1753+/-411 mu g vs 1626+/-444 mu g), 4 Dexfenfluramine AUC was higher in PMs (67 7+/-348 mu g l(-1) h) than EMs (359+/-250 mu g l(-1) h). The apparent oral clearance of dexfenfluramine was greater in EMs than PMs (93.6+/- 42.4 l h(-1) vs 45.6+/-19.5 l h(-1); 95% CI of difference 1.2-94.7; P< 0.05). The renal clearance was similar in both phenotypes (EMs: 5.88+/ -2.83 l h(-1); PMs 6.60+/-2.01 l h(-1)), indicating that the higher ur inary recovery of dexfenfluramine in PMs reflects higher plasma concen trations, rather than phenotype differences in the renal handling, of dexfenfluramine. 5 The apparent nonrenal clearance of dexfenfluramine was substantially lower (P<0.05; 95% CI of difference 3.0-94.1) in PMs (39.0+/-19.5 l h(-1)) than EMs (87.6/-41.2 l h(-1)). 6 There was a si gnificant inverse correlation (r(s)=-0.776 95% CI -0.31--0.94; n=11; P =0.005) between the debrisoquine metabolic ratio and the apparent nonr enal clearance of dexfenfluramine. 7 PMs had a higher incidence of adv erse effects (nausea and vomiting) than EMs. 8 In conclusion, the meta bolism of dexfenfluramine is impaired in PMs. Thus CYP2D6, the isoenzy me deficient in poor metabolizers of debrisoquine, must catalyse at le ast one pathway of dexfenfluramine biotransformation.