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Biotransformation of benzydamine by microsomes and precision-cut slices prepared from cattle liver.

机译:由牛肝制备的微粒体和精确切割的切片对苯乙胺进行生物转化。

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1. Benzydamine (BZ), a non-steroidal anti-inflammatory drug used in human and veterinary medicine, is not licensed for use in food-producing species. Biotransformation of BZ in cattle has not been reported previously and is investigated here using liver microsomes and precision-cut liver slices. 2. BZ was metabolized by cattle liver microsomes to benzydamine N-oxide (BZ-NO) and monodesmethyl-BZ (Nor-BZ). Both reactions followed Michaelis-Menten kinetics (Km = 76.4 +/- 16.0 and 58.9 +/- 0.4 microM Vmax = 6.5 +/- 0.8 and 7.4 +/- 0.5 nmolmg(-1) min(-1) respectively); sensitivity to heat and pH suggested that the N-oxidation is catalysed by the flavin-containing monooxygenases. 3. BZ-NO and Nor-BZ were the most abundant products derived from liver slice incubations, and nine other BZ metabolites were found and tentatively identified by LC-MS. Desbenzylated and hydroxylated BZ-NO analogues and a hydroxylated product of BZ were detected, which have been reported in other species. Product ion mass spectra of other metabolites, which are described here for the first time, indicated the formation of a BZ N- -glucuronide and five hydroxylated and N+-glucuronidated derivatives of BZ, BZ-NO and Nor-BZ. 4. The results indicate that BZ is extensively metabolized in cattle. Clearly, differences in metabolism compared with, for example, rat and human, will need to be considered in the event of submission for marketing authorization for use in food animals.
机译:1. Benzydamine(BZ)是一种用于人类和兽药的非甾体类抗炎药,未获许可用于食品生产物种。牛中BZ的生物转化以前尚未见报道,此处使用肝微粒体和精确切割的肝切片进行了研究。 2. BZ被牛肝微粒体代谢为苯扎明N-氧化物(BZ-NO)和一甲基-BZ(Nor-BZ)。两个反应均遵循Michaelis-Menten动力学(Km = 76.4 +/- 16.0和58.9 +/- 0.4 microM Vmax分别为6.5 +/- 0.8和7.4 +/- 0.5 nmolmg(-1)min(-1));对热和pH的敏感性表明N氧化是由含黄素的单加氧酶催化的。 3. BZ-NO和Nor-BZ是从肝切片培养物中获得的最丰富的产物,另外发现了9种BZ代谢物,并通过LC-MS初步鉴定。检测到去苄基和羟基化的BZ-NO类似物以及BZ的羟基化产物,这在其他物种中已有报道。此处首次描述的其他代谢物的产物离子质谱图表明形成了BZ N-葡糖醛酸苷和BZ,BZ-NO和Nor-BZ的五种羟基化和N +葡糖醛酸化的衍生物。 4.结果表明BZ在牛中被广泛代谢。显然,在提交用于食用动物的销售许可的情况下,将需要考虑与例如大鼠和人相比在新陈代谢方面的差异。

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