首页> 外文期刊>Japanese Journal of Pharmacology >STUDIES ON METABOLIC FATE OF A NEW ANTIALLERGIC AGENT, AZELASTINE (4- (p-CHLOROBENZYL) -2- [N-METHYLPERHYDROAZEPINYL- (4)] -1- (2H) - PHTHALAZINONE HYDROCHLORIDE)
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STUDIES ON METABOLIC FATE OF A NEW ANTIALLERGIC AGENT, AZELASTINE (4- (p-CHLOROBENZYL) -2- [N-METHYLPERHYDROAZEPINYL- (4)] -1- (2H) - PHTHALAZINONE HYDROCHLORIDE)

机译:新型抗超服剂,偶氮子(4-(氯苄苯)-2- [N-甲基氯酰脲酰脲酰己二氨基乙烯 - (4)] -1-(2H) - 盐酸盐的代谢命运研究

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References(15) Cited-By(12) The metabolic fate of a new antiallergic agent, azelastine (4- (p-chlorobenzyl) - 2- [N-methylperhydroazepinyl- (4)] -1- (2H) -phthalazinone hydrochloride) in rats and guinea pigs was investigated using its 14C-labelled compound. The blood level of radioactivity reached the maximum at 1-1.5 hr after oral administration, indicating the rapid absorption of the drug from gastrointestinal tract. A high concentration of radioactivity was detected in the lung of both species following either oral or intravenous administration. The major pathway of excretion of radioactivity was by way into feces, in both species. The radioactivity excreted in feces was attributable to that which was excreted in bile and exsorbed into gastrointegtinal tract. When the drug was given to pregnant rats, the concentration of radioactivity in the fetus was significantly lower than those in placenta and uterus, indicating the limited placental transfer of the drug. The successive oral administration of the drug in lower doses exerted no effect on the activity of microsomal drug-metabolizing enzymes of rat liver, while in higher doses, had a slight effect.
机译:引用(15)引用(12)新的抗超服剂,偶氮子(4-(氯苄基) - 2- [N-甲基氯酰脲酰己戊二氨基 - (4)] -1-(2H)-phalthalazinone盐酸盐)的代谢命运)在大鼠和豚鼠中使用其14℃标记的化合物进行研究。口服给药后1-1.5小时的放射性血液水平达到最大值,表明药物来自胃肠道的快速吸收。在口服或静脉内给药后,在两种物种的肺部检测到高浓度的放射性。在两种物种中,放射性排泄的主要途径是粪便。在粪便中排出的放射性可归因于胆汁中排出的排泄物并将其浸入胃食记道中。当药物给予孕大鼠时,胎儿中放射性浓度明显低于胎盘和子宫,表明药物的有限胎盘转移。较低剂量的药物的连续口服给药对大鼠肝脏的微粒体药物代谢酶的活性没有影响,而在更高剂量的同时具有轻微的效果。

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