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Absorption distribution metabolic fate and elimination of pefloxacin mesylate in mice rats dogs monkeys and humans.

机译:甲磺酸培氟沙星在小鼠大鼠狗猴子和人类中的吸收分布代谢命运和消除。

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摘要

Pefloxacin mesylate is well absorbed by the oral route. The antimicrobial activity in dog, cynomolgus monkey, and human plasma was essentially due to unchanged drug which respectively accounted for 64, 94, and 84% of the total activity (ratios derived from relative area under the curve [AUC] values). Half-lives ranged from 1.9 h in mice to 8.6 h in humans. Protein binding was weak, about 20% in plasma. Except in brain, concentrations in most of the organs and tissues tested in rats and dogs were higher than the plasma levels. Microbiological activity in urine was mainly due to pefloxacin and norfloxacin, the N-desmethyl metabolite. The norfloxacin/pefloxacin ratios were 0 in mice, ca. 1 in rats and dogs, 1.6 in cynomolgus monkeys, and 2.3 in humans. The principal urinary compounds were unchanged drug in mice, pefloxacin glucuronide and pefloxacin N-oxide in rats and dogs, norfloxacin and pefloxacin in monkeys, and pefloxacin N-oxide and norfloxacin in humans. The urinary recovery of identified metabolites was 29.5% of the dose in mice, 37.8% in rats, 36.3% in dogs, 26.5% in monkeys, and 58.9% in humans. Biliary excretion occurred and was extensive in rats and dogs, mainly as a glucuronide conjugate of the drug. In rat and human bile, the main active compound was unchanged pefloxacin.
机译:甲磺酸培氟沙星通过口服途径吸收良好。狗,食蟹猴和人血浆中的抗微生物活性基本上是由于未改变的药物引起的,它们分别占总活性的64%,94%和84%(比例来自曲线[AUC]值下的相对面积)。半衰期从小鼠的1.9小时到人类的8.6小时不等。蛋白结合较弱,在血浆中约为20%。除大脑外,在大鼠和狗中测试的大多数器官和组织中的浓度都高于血浆水平。尿液中的微生物活性主要归因于培氟沙星和诺氟沙星(N-去甲基代谢产物)。在小鼠中,诺氟沙星/培氟沙星的比率为0,约等于1。在大鼠和狗中为1,在食蟹猴中为1.6,在人类中为2.3。尿中的主要化合物是小鼠不变的药物,大鼠和狗中的培氟沙星葡糖醛酸和培氟沙星N-氧化物,猴子的诺氟沙星和培氟沙星以及人类的佩氟沙星N-氧化物和诺氟沙星。所确定的代谢产物的尿回收率是小鼠的29.5%,大鼠的37.8%,狗的36.3%,猴子的26.5%和人的58.9%。胆汁排泄发生在大鼠和狗中并且广泛存在,主要是作为药物的葡糖醛酸结合物。在大鼠和人胆汁中,主要活性化合物是不变的培氟沙星。

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