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氟桂利嗪在大鼠、狗和人体内的代谢比较:一项利用亚细胞肝组分和分离肝细胞进行的体外研究。

Comparative metabolism of flunarizine in rats, dogs and man: an in vitro study with subcellular liver fractions and isolated hepatocytes.

作者信息

Lavrijsen K, van Houdt J, van Dyck D, Hendrickx J, Bockx M, Hurkmans R, Meuldermans W, Le Jeune L, Lauwers W, Heykants J

机构信息

Department of Drug Metabolism and Pharmacokinetics, Janssen Research Foundation, Beerse, Belgium.

出版信息

Xenobiotica. 1992 Jul;22(7):815-36. doi: 10.3109/00498259209053143.

Abstract
  1. The biotransformation of 3H-flunarizine ((E)-1-[bis(4-fluorophenyl)methyl]-4-(3-phenyl-2-propenyl)piperazine dihydrochloride, FLUN) was studied in subcellular liver fractions (microsomes and 12,000 g fraction) and in suspensions or primary cell cultures of isolated hepatocytes of rats, dogs and man. The major in vitro metabolites were characterized by h.p.l.c. co-chromatography and/or by mass spectrometric analysis. 2. The kinetics of FLUN metabolism was studied in microsomes of dog and man. The metabolism followed linear Michaelis-Menten kinetics over the concentration range 0.1-20 microM FLUN. 3. A striking sex difference was observed for the in vitro metabolism of FLUN in rat. In male rats, oxidative N-dealkylation at one of the piperazine nitrogens, resulting in bis(4-fluorophenyl) methanol, was a major metabolic pathway, whereas aromatic hydroxylation at the phenyl of the cinnamyl moiety, resulting in hydroxy-FLUN, was a major metabolic pathway in female rats. In incubates with hepatocytes, these two metabolites were converted to the corresponding glucuronides. 4. In human subcellular fractions, aromatic hydroxylation to hydroxy-FLUN was the major metabolic pathway. In primary cell cultures of human hepatocytes, oxidative N-dealkylation at the 1- and 4-piperazine nitrogen and glucuronidation of bis(4-fluorophenyl)methanol were observed. The in vitro metabolism of FLUN in humans, resembled more than in female rats and in dogs than that in male rats. 5. The present in vitro results are compared with data of previous in vivo studies in rats and dogs. The use of subcellular fractions and/or isolated hepatocytes for the study of species differences in the biotransformation of xenobiotics is discussed.
摘要
  1. 研究了3H-氟桂利嗪((E)-1-[双(4-氟苯基)甲基]-4-(3-苯基-2-丙烯基)哌嗪二盐酸盐,FLUN)在大鼠、犬和人的肝亚细胞组分(微粒体和12,000 g组分)以及分离的肝细胞悬液或原代细胞培养物中的生物转化。通过高效液相色谱共色谱法和/或质谱分析对主要的体外代谢产物进行了表征。2. 在犬和人的微粒体中研究了FLUN的代谢动力学。在0.1 - 20 μM FLUN浓度范围内,代谢遵循线性米氏动力学。3. 在大鼠中观察到FLUN体外代谢存在显著的性别差异。在雄性大鼠中,哌嗪氮之一的氧化N-去烷基化生成双(4-氟苯基)甲醇是主要代谢途径,而在雌性大鼠中,肉桂基部分苯基的芳香羟基化生成羟基-FLUN是主要代谢途径。在肝细胞孵育物中,这两种代谢产物转化为相应的葡糖醛酸苷。4. 在人亚细胞组分中,芳香羟基化生成羟基-FLUN是主要代谢途径。在人肝细胞原代细胞培养物中,观察到1-和4-哌嗪氮处的氧化N-去烷基化以及双(4-氟苯基)甲醇的葡糖醛酸化。FLUN在人体内的体外代谢与雌性大鼠和犬的更相似,而与雄性大鼠的不同。5. 将目前的体外研究结果与先前在大鼠和犬体内研究的数据进行了比较。讨论了使用亚细胞组分和/或分离的肝细胞来研究异种生物转化中的物种差异。

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