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通过“鸡尾酒”法评估人身上安替比林、己巴比妥和茶碱的代谢之间的关系。

Relationship between the metabolism of antipyrine, hexobarbitone and theophylline in man as assessed by a 'cocktail' approach.

作者信息

Schellens J H, van der Wart J H, Danhof M, van der Velde E A, Breimer D D

机构信息

Center for Bio-Pharmaceutical Sciences, Division of Pharmacology, Leiden, The Netherlands.

出版信息

Br J Clin Pharmacol. 1988 Oct;26(4):373-84. doi: 10.1111/j.1365-2125.1988.tb03394.x.

Abstract
  1. Three model substrates for the characterization of drug oxidation activity, antipyrine (AP), hexobarbitone (HB) and theophylline (TH), were administered to 26 healthy volunteers on two different occasions: in the first experiment a combination of AP (250 mg) and HB (250 mg) was given and in the second experiment TH (150 mg) was added to the former combination. 2. Plasma concentrations of AP, HB and TH and urinary excretion of TH and the three main metabolites of AP (3-hydroxymethylantipyrine: HMA, norantipyrine: NORA and 4-hydroxyantipyrine: OHA) were determined and the intrinsic clearance (CLint) of the three substrates and the clearance to the formation of AP metabolites were calculated. 3. The correlation coefficients between CLHB and CL-greater than metabolites of AP were highest for CL-greater than HMA and CL-greater than NORA (greater than 0.80) and lowest for CL-greater than OHA (0.63). High correlation coefficients also were found between CLTH and CL-greater than OHA (0.89) and CL-greater than HMA (0.80). 4. Ideal relationships, defined by a slope of the orthogonal regression line equal to unity, did exist between CLHB and CL-greater than HMA as well as CL-greater than NORA and between CLTH and CLAP as well as CL-greater than OHA. 5. Based on the results of correlation and regression analysis it can be concluded that isozymes of the cytochrome P-450 system responsible for the oxidation of HB and formation of HMA and NORA are very closely related and also that isozymes responsible for the oxidation of TH and formation of OHA show a very close relation. 6. With this strategy of simultaneous administration of substrates ('cocktail' approach) it seems possible to characterize and correlate activities of different P-450 isozymes and to investigate their in vivo substrate selectivity without the disturbing influence of intra-individual variation in drug oxidation.
摘要
  1. 为了表征药物氧化活性,给26名健康志愿者在两种不同情况下施用了三种模型底物,即安替比林(AP)、己巴比妥(HB)和茶碱(TH):在第一个实验中,给予AP(250毫克)和HB(250毫克)的组合,在第二个实验中,将TH(150毫克)添加到前一种组合中。2. 测定了AP、HB和TH的血浆浓度以及TH的尿排泄量和AP的三种主要代谢物(3-羟甲基安替比林:HMA、去甲安替比林:NORA和4-羟基安替比林:OHA),并计算了三种底物的内在清除率(CLint)以及AP代谢物形成的清除率。3. CLHB与CL大于AP代谢物之间的相关系数,对于CL大于HMA和CL大于NORA最高(大于0.80),对于CL大于OHA最低(0.63)。在CLTH与CL大于OHA(0.89)和CL大于HMA(0.80)之间也发现了高相关系数。4. 由正交回归线斜率等于1定义的理想关系,确实存在于CLHB与CL大于HMA以及CL大于NORA之间,以及CLTH与CLAP以及CL大于OHA之间。5. 根据相关性和回归分析结果可以得出结论,负责HB氧化以及HMA和NORA形成的细胞色素P-450系统同工酶密切相关,并且负责TH氧化以及OHA形成的同工酶也显示出非常密切的关系。6. 采用这种同时施用底物的策略(“鸡尾酒”方法),似乎有可能表征和关联不同P-450同工酶的活性,并研究它们在体内的底物选择性,而不受药物氧化个体内变异的干扰影响。

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