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体内安替比林代谢产物形成与大鼠茶碱代谢的相关性。

Correlation between in vivo antipyrine metabolite formation and theophylline metabolism in rats.

机构信息

Center for Bio-Pharmaceutical Sciences, Division of Pharmacology, Sylvius Laboratories, University of Leiden, P.O. Box 9503, 2300 RA, Leiden, The Netherlands.

出版信息

Pharm Res. 1986 Jun;3(3):156-61. doi: 10.1023/A:1016361907787.

Abstract

Two model substrates for oxidative hepatic enzyme activity, viz. antipyrine (A) and theophylline (T), were given simultaneously to rats by iv administration. Blood concentrations of A and T were measured by a high-performance liquid chromatographic (HPLC) method. Urinary excretions of A, T, and the major metabolites arising from A-4-hydroxyantipyrine (OHA), norantipyrine (NORA), 3-hydroxymethylantipyrine (HMA), and 4,4'-dihydroxyantipyrine (DOHA)-and from T-1-methyluric acid (1-MU) and 1,3-dimethyluric acid (1,3-DMU)-were also determined by HPLC. It was found that the pharmacokinetic parameters obtained after the simultaneous administration of A and T at relatively low dose levels (A, 5.0 mg; and T, 1.3 mg) were not different from those obtained after the separate administration of A or T at the same dose level. In order to investigate whether the metabolic pathways of A and T are mediated by the same or closely related forms of the cytochrome P-450 system, metabolic clearances of A (CLA,M) and T (CLT,M) and the clearances for production of their various metabolites, obtained in untreated rats and in rats pretreated with 3-methylcholanthrene (MC) or with MC followed by 9-hydroxyellipticine (E), were correlated. These two compounds are a selective cytochrome P-448 inducer and inhibitor, respectively. Strong correlations were found between CLT,M and the clearances for production of OHA, NORA, and DOHA but not HMA. The best correlation, however, was observed between CLT,M and CLOHA, not only when all data points were taken into account (r = 0.99), but also in separate pretreatment groups (r ranging from 0.87 to 0.92). Moreover, the slopes of these correlation lines varied only slightly among groups, while the intercepts were not significantly different from zero. In the separate pretreatment groups, the correlation coefficients for the correlations between CLT,M and the clearance for production of the other metabolites of A were considerably lower, while the slopes of the correlation lines varied substantially. Clearances for production of the metabolites of T were strongly correlated with each other (r = 0.99) and with CLOHA (r = 0.95). It can be concluded that theophylline metabolism and formation of OHA are mediated by the same or very similar forms of cytochrome P-450, whereas formation of the other major metabolites of A is not or only partly. The study of the various pathways of metabolism after simultaneous administration of drugs is a powerful tool in the study of correlations in drug metabolism in vivo.

摘要

两种用于评估肝氧化酶活性的模型底物,即非那西丁(A)和茶碱(T),通过静脉注射同时给予大鼠。采用高效液相色谱法(HPLC)测定 A 和 T 的血药浓度。通过 HPLC 还测定了 A 的主要代谢物 4-羟基非那西丁(OHA)、去甲非那西丁(NORA)、3-羟甲基非那西丁(HMA)和 4,4'-二羟基非那西丁(DOHA)以及 T 的主要代谢物 1-甲基尿酸(1-MU)和 1,3-二甲基尿酸(1,3-DMU)的尿排泄率。结果发现,当以相对较低的剂量水平(A 为 5.0mg;T 为 1.3mg)同时给予 A 和 T 时,获得的药代动力学参数与单独给予 A 或 T 时获得的参数无差异。为了研究 A 和 T 的代谢途径是否由相同或密切相关的细胞色素 P-450 同工酶介导,在未处理的大鼠和用 3-甲基胆蒽(MC)预处理或用 MC 后用 9-羟基埃利替尼(E)预处理的大鼠中,分别对 A 的代谢清除率(CLA,M)和 T(CLT,M)以及产生其各种代谢物的清除率进行了相关性分析。这两种化合物分别是细胞色素 P-448 的选择性诱导剂和抑制剂。在 CLT,M 与 OHA、NORA 和 DOHA 的产生清除率之间发现了很强的相关性,但与 HMA 无关。然而,当考虑所有数据点时(r=0.99),最佳相关性观察到 CLT,M 与 CLOHA 之间,不仅如此,在单独的预处理组中(r 范围从 0.87 到 0.92)也是如此。此外,这些相关线的斜率在各组之间变化不大,而截距与零无显著差异。在单独的预处理组中,CLT,M 与 A 的其他代谢物产生清除率之间的相关性的相关系数要低得多,而相关线的斜率则有很大的变化。T 的代谢产物的清除率彼此强烈相关(r=0.99),与 CLOHA 也强烈相关(r=0.95)。可以得出结论,茶碱代谢和 OHA 的形成由相同或非常相似的细胞色素 P-450 同工酶介导,而 A 的其他主要代谢物的形成则不是或仅部分是。研究药物同时给药后的各种代谢途径是研究体内药物代谢相关性的有力工具。

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