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14C-舒马曲坦经鼻给药后在比格犬体内的吸收、药效学、代谢及排泄情况。

off absorption, pharmacodynamics, metabolism and excretion of 14C-sumatriptan following intranasal administration to the beagle dog.

作者信息

Barrow A, Dixon C M, Saynor D A, Perren M J, Stowe R, Smith I

机构信息

Bioanalysis and Drug Metabolism Division, GlaxoWellcome Research and Development, Ware, Herts, U.K.

出版信息

Biopharm Drug Dispos. 1997 Jul;18(5):443-58. doi: 10.1002/(sici)1099-081x(199707)18:5<443::aid-bdd35>3.0.co;2-d.

Abstract

The pharmacodynamics, pharmacokinetics, metabolism, and excretion of 14C-sumatriptan have been studied in the beagle dog following administration by the intranasal and other routes. The pharmacological response which was monitored, an increase in carotid arterial vascular resistance, correlated with the plasma levels of unchanged sumatriptan following intranasal, intravenous, or intraduodenal administration to the anaesthetised dog. The pharmacokinetics and metabolism of sumatriptan were then confirmed in conscious male and female dogs. Intranasal administration of 14C-sumatriptan resulted in rapid absorption of part of the dose. The overall bioavailability of sumatriptan was 40-50%. Sumatriptan was eliminated from plasma with a half-life of 1.5 or 1.9 h after intravenous or intranasal dosage respectively. Radioactivity was largely excreted in urine (up to 75% of the dose) with small amounts in the bile and faeces after intravenous and intranasal dosing, as sumatriptan and a major metabolite. The results from these studies suggest that intranasal administration provides a viable method for delivering sumatriptan to the systemic circulation.

摘要

在比格犬中,通过鼻内及其他途径给药后,对14C-舒马曲坦的药效学、药代动力学、代谢及排泄情况进行了研究。所监测的药理反应为颈动脉血管阻力增加,在对麻醉犬进行鼻内、静脉内或十二指肠内给药后,该反应与未改变的舒马曲坦血浆水平相关。随后在清醒的雄性和雌性犬中证实了舒马曲坦的药代动力学和代谢情况。鼻内给予14C-舒马曲坦导致部分剂量快速吸收。舒马曲坦的总体生物利用度为40%-50%。静脉内或鼻内给药后,舒马曲坦从血浆中消除的半衰期分别为1.5小时或1.9小时。静脉内和鼻内给药后,放射性主要经尿液排泄(高达剂量的75%),少量经胆汁和粪便排泄,排泄物为舒马曲坦及其一种主要代谢产物。这些研究结果表明,鼻内给药为将舒马曲坦递送至体循环提供了一种可行的方法。

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