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大鼠和犬体内14C-0-[3-(4-(2-甲氧基苯基)-1-哌嗪基)-2-羟丙基]-3-甲氧基苯甲醛肟二盐酸盐及其去甲基代谢物的肠肝循环

Enterohepatic circulation in rat and dog of 14C-0-[3-(4-less than 2-methoxyphenyl greater than-1-piperazinyl)-2-hydroxypropyl]-3-methoxy-benzaldoxim dihydrochloride and it's demethylated metabolite.

作者信息

Paul H, Illing A, House E S

出版信息

Eur J Drug Metab Pharmacokinet. 1981;6(4):303-12. doi: 10.1007/BF03189530.

Abstract

14C-0-[3-(4- less than 2-methoxyphenyl greater than -1-piperazinyl)-2-hydroxypropyl]-3-methoxybenzaldoxim dihydrochloride (HWA 923) was well absorbed (approximately 80%) in rat and dog. In normal animals 37-48% of the radioactivity from a 2 mg/kg of body weight oral or parenteral dose was excreted in the urine, and 48-50% in the faeces. When 14C-HWA 923 was given orally to rats with biliary cannulae, only approximately 10% of the dose was excreted in the urine and approximately 68% appeared in the bile. If bile, collected from animals given 14C-HWA 923, was re-infused intraduodenally into surgically prepared rats, approximately 12% was re-excreted in the urine, and approximately 55% re-excreted in the bile. There were considerably higher levels of radioactivity present in rat blood following intravenous administration of 14C-HWA 923 than after an oral dose, suggesting that radioactivity given via the oral route might be excreted directly into the bile without reaching the systemic circulation. In dog, a significant "first-pass" effect was seen for HWA 923. In a surgically prepared dog, where the bile collection was intermittent, 32% of the dose was excreted in the urine and 46% in the bile. An estimated 73% of the dose would have been present in bile, if continuous collection had taken place. In rat, the major urinary metabolite (up to 40% of the urinary radioactivity) was identified, after specific hydrolysis with beta-glucuronidase, as a demethylated product of HWA 923 by co-chromatography in four solvent systems. This metabolite was present, in rat bile as the conjugates (approximately 40% of the biliary radioactivity), together with significant quantities (approximately 20%) of conjugated HWA 923. The two products were also found on hydrolysis o bile, using gut microflora. Similar results were obtained from dog samples. It is postulated that hydrolysis of the glucuronides of unchanged HWA 923 and its demethylated metabolite by gut micro-flora results in enterohepatic circulation of these two compounds in rat and dog.

摘要

14C - 0 - [3 - (4 - <2 - 甲氧基苯基> - 1 - 哌嗪基) - 2 - 羟丙基] - 3 - 甲氧基苯甲醛肟二盐酸盐(HWA 923)在大鼠和犬体内吸收良好(约80%)。在正常动物中,以2mg/kg体重的口服或非肠道给药剂量,37% - 48%的放射性物质经尿液排泄,48% - 50%经粪便排泄。当给有胆管插管的大鼠口服14C - HWA 923时,仅约10%的剂量经尿液排泄,约68%出现在胆汁中。如果将给14C - HWA 923的动物收集的胆汁经十二指肠再注入手术制备的大鼠体内,约12%会再次经尿液排泄,约55%再次经胆汁排泄。静脉注射14C - HWA 923后大鼠血液中的放射性水平明显高于口服给药后,这表明经口服途径给予的放射性物质可能直接排泄到胆汁中而未进入体循环。在犬体内,观察到HWA 923有显著的“首过”效应。在一只手术制备的犬中,胆汁收集是间歇性的,32%的剂量经尿液排泄,46%经胆汁排泄。如果进行连续收集,估计73%的剂量会出现在胆汁中。在大鼠体内,经β - 葡萄糖醛酸酶特异性水解后,主要的尿液代谢产物(高达尿液放射性的40%)通过在四种溶剂系统中的共色谱法被鉴定为HWA 923的去甲基化产物。这种代谢产物在大鼠胆汁中以缀合物形式存在(约占胆汁放射性的40%),同时还有大量(约20%)的缀合HWA 923。使用肠道微生物群对胆汁进行水解时也发现了这两种产物。从犬的样本中也得到了类似结果。据推测,肠道微生物群对未改变的HWA 923及其去甲基化代谢产物的葡萄糖醛酸苷的水解导致了这两种化合物在大鼠和犬体内的肠肝循环。

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