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新型喹诺酮类抗生素曲伐沙星在斯普拉格-道利大鼠和比格犬体内的代谢与排泄。胆管插管对排泄途径的影响。

Metabolism and excretion of trovafloxacin, a new quinolone antibiotic, in Sprague-Dawley rats and beagle dogs. Effect of bile duct cannulation on excretion pathways.

作者信息

Dalvie D K, Khosla N B, Navetta K A, Brighty K E

机构信息

Drug Metabolism Department, Pfizer, Inc., Groton, CT 06340, USA.

出版信息

Drug Metab Dispos. 1996 Nov;24(11):1231-40.

PMID:8937858
Abstract

The excretion and metabolism of trovafloxacin was investigated after administration of a single oral dose of [14C]trovafloxacin to Sprague-Dawley rats and beagle dogs. The bile was the major route of excretion in rats (59% of the dose). Trovafloxacin was extensively metabolized in this species, and only 3% of the dose was excreted unchanged. Glucuronidation and acetylation were the major metabolic pathways involved in the elimination, and no oxidative metabolites were detected in rats. In dogs, 97.6 and 2.7% of the dose was recovered in feces and urine, respectively, in 72 hr. However, excretion studies in bile duct-cannulated dogs revealed that 28.2% of the radioactivity was recovered in bile, whereas 45.6% was in urine. This suggested that bile duct cannulation had affected the disposition of trovafloxacin. Analysis of bile and urine of bile duct-cannulated dogs by LC/MS/MS indicated that glucuronidation was the major metabolic pathway in dogs as well. Two novel metabolites were identified in the bile of this species. One was confirmed as a pyrroline analog of trovafloxacin (M7), and the second was tentatively identified as the hydroxycarboxylic acid analog (M6). The differences in metabolism of trovafloxacin in the bile duct-cannulated and noncannulated dogs were investigated by comparison of the metabolite profiles in urine and feces of these animals. Although the metabolites in urine were similar, the extracts of fecal samples obtained from noncannulated animals revealed the presence of N-acetyltrovafloxacin (M3). Incubation of trovafloxacin with cecal contents of dogs under anaerobic conditions suggested the involvement of intestinal microflora in the formation of this metabolite. Metabolite M3 was absent from fecal extracts of bile duct-cannulated dogs, suggesting that surgery had affected the metabolism of trovafloxacin by gut microflora.

摘要

给斯普拉格 - 道利大鼠和比格犬单次口服一剂[¹⁴C]曲伐沙星后,对其排泄和代谢情况进行了研究。胆汁是大鼠排泄的主要途径(占给药剂量的59%)。曲伐沙星在该物种中被广泛代谢,只有3%的给药剂量以原形排泄。葡萄糖醛酸化和乙酰化是参与消除过程的主要代谢途径,在大鼠中未检测到氧化代谢物。在犬中,72小时内分别有97.6%和2.7%的给药剂量在粪便和尿液中回收。然而,对胆管插管犬的排泄研究表明,28.2%的放射性在胆汁中回收,而45.6%在尿液中。这表明胆管插管影响了曲伐沙星的处置。通过LC/MS/MS对胆管插管犬的胆汁和尿液进行分析表明,葡萄糖醛酸化也是犬的主要代谢途径。在该物种的胆汁中鉴定出两种新的代谢物。一种被确认为曲伐沙星的吡咯啉类似物(M7),另一种被初步鉴定为羟基羧酸类似物(M6)。通过比较这些动物尿液和粪便中的代谢物谱,研究了胆管插管犬和未插管犬中曲伐沙星代谢的差异。虽然尿液中的代谢物相似,但从未插管动物获得的粪便样品提取物显示存在N - 乙酰曲伐沙星(M3)。在厌氧条件下将曲伐沙星与犬盲肠内容物一起孵育表明肠道微生物群参与了该代谢物的形成。胆管插管犬的粪便提取物中没有代谢物M3,这表明手术影响了肠道微生物群对曲伐沙星的代谢。

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