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单独口服别嘌醇或与苯溴马隆联合应用后,人体中别嘌醇及其代谢产物氧嘌呤醇的动力学。采用气相色谱-质谱联用技术同时测定次黄嘌呤和黄嘌呤。

Kinetics of allopurinol and its metabolite oxypurinol after oral administration of allopurinol alone or associated with benzbromarone in man. Simultaneous assay of hypoxanthine and xanthine by gas chromatography-mass spectrometry.

作者信息

Lartigue-Mattei C, Chabard J L, Ristori J M, Bussiere J L, Bargnoux H, Petit J, Berger J A

机构信息

Laboratoire de Chimie analytique et de spectrométrie de masse, Faculté de Pharmacie, Clermont-Ferrand, France.

出版信息

Fundam Clin Pharmacol. 1991;5(7):621-33. doi: 10.1111/j.1472-8206.1991.tb00751.x.

DOI:10.1111/j.1472-8206.1991.tb00751.x
PMID:1778540
Abstract

Allopurinol, oxypurinol, hypoxanthine and xanthine were assayed simultaneously using a highly specific method combining gas chromatography and mass spectrometry. Two hypo-uricaemic prescriptions were compared: i) 300 mg of allopurinol (AL); and ii) 100 mg of allopurinol plus 20 mg of benzbromarone (AL + BZB). When administered acutely, their effects on blood uric acid levels were similar. Analysis of the pharmacokinetic parameters of allopurinol and its metabolite after each treatment showed dose-linearity for the metabolite but not for the drug itself. The area under the concentration time curve for allopurinol was 40.3 +/- 9.3 mumol l-1 h after AL, against 8.4 +/- 3.9 mumol-1 h after AL + BZB, while for oxypurinol it was 948.0 +/- 125.4 mumol l-1 h after AL and 285.2 +/- 77.9 mumol l-1 h after AL + BZB. The difference in dosage form may partly account for this difference, but the benzbromarone also seems to be involved. Its role on the blood uric acid lowering action of the drug association is complex. Although benzbromarone appreciably favors the elimination of oxypurinol, which should result in a weakening of its hypo-uricaemic action, this is offset by enhanced elimination of hypoxanthine and xanthine. Renal clearance of xanthine was significantly increased under AL + BZB (173.1 +/- 65.6 ml/min against 112.2 +/- 32.9 ml/min after AL). Similarly, blood xanthine levels were proportionately higher in the presence of benzbromarone. The action of the two agents may thus be synergistic and not antagonistic, a pharmacological justification for the therapeutic use of this drug association.

摘要

采用气相色谱和质谱联用的高特异性方法同时测定了别嘌醇、氧嘌呤醇、次黄嘌呤和黄嘌呤。比较了两种降尿酸处方:i)300mg别嘌醇(AL);ii)100mg别嘌醇加20mg苯溴马隆(AL + BZB)。急性给药时,它们对血尿酸水平的影响相似。对每种治疗后别嘌醇及其代谢物的药代动力学参数分析表明,代谢物呈剂量线性,而药物本身并非如此。AL组别嘌醇的浓度-时间曲线下面积为40.3±9.3μmol·l⁻¹·h,AL + BZB组为8.4±3.9μmol·l⁻¹·h;而氧嘌呤醇在AL组为948.0±125.4μmol·l⁻¹·h,在AL + BZB组为285.2±77.9μmol·l⁻¹·h。剂型差异可能部分解释了这种差异,但苯溴马隆似乎也有影响。其对药物联合降血尿酸作用的影响较为复杂。虽然苯溴马隆明显促进氧嘌呤醇的消除,这可能会削弱其降尿酸作用,但次黄嘌呤和黄嘌呤消除的增强抵消了这一作用。在AL + BZB组,黄嘌呤的肾清除率显著增加(173.1±65.6ml/min,而AL组为112.2±32.9ml/min)。同样,在有苯溴马隆存在时,血中黄嘌呤水平相应更高。因此,这两种药物的作用可能是协同而非拮抗的,这为这种药物联合治疗的应用提供了药理学依据。

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