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恒河猴(猕猴属)体内14C标记的琥珀酸多西拉敏(敏克静)的代谢

Metabolism of 14C-labeled doxylamine succinate (Bendectin) in the rhesus monkey (Macaca mulatta).

作者信息

Slikker W, Holder C L, Lipe G W, Korfmacher W A, Thompson H C, Bailey J R

出版信息

J Anal Toxicol. 1986 May-Jun;10(3):87-92. doi: 10.1093/jat/10.3.87.

Abstract

The time-course of the metabolic fate of [14C]doxylamine was determined after the p.o. administration of 13 mg/kg doxylamine succinate as Bendectin plus [14C]doxylamine succinate to the rhesus monkey. Urine and plasma samples were analyzed by reversed-phase high performance liquid chromatography (HPLC), chemical derivatization, and mass spectrometry. The cumulative 48-hr urinary metabolic profile contained 81% of the administered radiolabeled dose and consisted of at least six radiolabeled peaks. They were peak 1: unknown polar metabolites (8% of dose); peak 2: 2-[1-phenyl-1-(2-pyridinyl)ethoxy] acetic acid, 1-[1-phenyl-1(2-pyridinyl)ethoxy] methanol, and another minor metabolite(s) (31%); peak 3: doxylamine-N-oxide (1%); peak 4a: N,N-didesmethyldoxylamine (17%); peak 4b: doxylamine (4%); and peak 5: N-desmethyldoxylamine (20%). The plasma metabolic profile was the same as the urinary profile except for the absence of doxylamine-N-oxide. The maximum plasma concentrations and elapsed time to attain these concentrations were as follows. Peak 1: 540 ng/mL, 4 hr; peak 2: 1700 ng/mL, 1 hr; peak 4a: 430 ng/mL, 4 hr; peak 4b: 930 ng/mL, 2 hr; and peak 5: 790 ng/mL, 2 hr. These data suggest that in the monkey, doxylamine metabolism follows at least four pathways: a minor pathway to the N-oxide; a minor pathway to unknown polar metabolites; a major pathway to mono- and didesmethyldoxylamine via successive N-demethylation; and a major pathway to side-chain cleavage products (peak 2) via direct side-chain oxidation and/or deamination.

摘要

在恒河猴口服给予13mg/kg琥珀酸多西拉敏(作为复方苯乙哌啶加[14C]琥珀酸多西拉敏)后,测定了[14C]多西拉敏的代谢转归时间进程。尿液和血浆样本通过反相高效液相色谱(HPLC)、化学衍生化和质谱法进行分析。48小时累积尿代谢图谱包含给药放射性标记剂量的81%,由至少六个放射性标记峰组成。它们分别是:峰1:未知极性代谢物(剂量的8%);峰2:2-[1-苯基-1-(2-吡啶基)乙氧基]乙酸、1-[1-苯基-1(2-吡啶基)乙氧基]甲醇和另一种次要代谢物(31%);峰3:多西拉敏-N-氧化物(1%);峰4a:N,N-去二甲基多西拉敏(17%);峰4b:多西拉敏(4%);峰5:N-去甲基多西拉敏(20%)。血浆代谢图谱与尿液图谱相同,只是没有多西拉敏-N-氧化物。达到这些浓度的最大血浆浓度和经过时间如下:峰1:540ng/mL,4小时;峰2:1700ng/mL,1小时;峰4a:430ng/mL,4小时;峰4b:930ng/mL,2小时;峰5:790ng/mL,2小时。这些数据表明,在猴子体内,多西拉敏的代谢至少遵循四条途径:一条生成N-氧化物的次要途径;一条生成未知极性代谢物的次要途径;一条通过连续N-去甲基化生成单去甲基和双去甲基多西拉敏的主要途径;以及一条通过直接侧链氧化和/或脱氨基生成侧链裂解产物(峰2)的主要途径。

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