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δ-11-四氢大麻酚在小鼠、大鼠、豚鼠、兔、仓鼠、沙鼠和猫体内的体外代谢

In vitro metabolism of delta-11-tetrahydrocannabinol in the mouse, rat, guinea pig, rabbit, hamster, gerbil and cat.

作者信息

Harvey D J, Brown N K

机构信息

University Department of Pharmacology, Oxford, UK.

出版信息

Comp Biochem Physiol C Comp Pharmacol Toxicol. 1990;96(1):65-9. doi: 10.1016/0742-8413(90)90045-b.

Abstract
  1. Liver microsomes were prepared from rats, rabbits, guinea pigs, hamsters, gerbils, a cat and three strains of mice, and were incubated with delta-11-tetrahydrocannabinol (delta-11-THC). The extracted metabolites were separated by chromatography on Sephadex LH-20 and examined by gas chromatography and combined gas chromatography/mass spectrometry. 2. Eleven metabolites were identified; these were formed by aliphatic hydroxylation of all positions of the pentyl chain, allylic hydroxylation at C-10 and C-8 (alpha and beta), and by the epoxide-diol pathway. 3. The ratio of the metabolites varied considerably between the species. Mice and rats favoured hydroxylation at C-8-alpha with very little hydroxylation of the pentyl chain. 4. In the guinea pig, however, hydroxylation of the pentyl chain, particularly at C-4', produced the major metabolites; very little hydroxylation occurred at C-8. 5. Side-chain hydroxylation was also favoured by the gerbil. 6. In the cat and hamster, 8-beta-hydroxylation was by far the major metabolic route, accounting, in the cat, for nearly 70% of the recovered metabolites. 7. The rabbit, on the other hand, favoured the epoxide-diol pathway with over 70% of the recovered metabolites being accounted for by the 9,11-dihydro-diols. 8. The results emphasise the need to make appropriate choices of animal models for metabolic and toxicological studies in humans.
摘要
  1. 从大鼠、兔子、豚鼠、仓鼠、沙鼠、一只猫和三个品系的小鼠中制备肝微粒体,并将其与δ-11-四氢大麻酚(δ-11-THC)一起孵育。提取的代谢产物通过Sephadex LH-20柱色谱进行分离,然后通过气相色谱以及气相色谱/质谱联用进行检测。2. 鉴定出了11种代谢产物;这些产物是由戊基链所有位置的脂肪族羟基化、C-10和C-8(α和β)处的烯丙基羟基化以及环氧化物-二醇途径形成的。3. 不同物种之间代谢产物的比例差异很大。小鼠和大鼠倾向于在C-8-α处发生羟基化,而戊基链的羟基化很少。4. 然而,在豚鼠中,戊基链的羟基化,特别是在C-4'处,产生了主要的代谢产物;在C-8处几乎没有羟基化发生。5. 沙鼠也倾向于侧链羟基化。6. 在猫和仓鼠中,8-β-羟基化是迄今为止主要的代谢途径,在猫中,这一途径产生的代谢产物占回收代谢产物的近70%。7. 另一方面,兔子倾向于环氧化物-二醇途径,回收的代谢产物中有超过70%是9,11-二氢二醇。8. 这些结果强调了在人类代谢和毒理学研究中选择合适动物模型的必要性。

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