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大麻二酚醇作为大麻二酚在哺乳动物体内的一种新代谢产物。

Cannabielsoin as a new metabolite of cannabidiol in mammals.

作者信息

Yamamoto I, Gohda H, Narimatsu S, Watanabe K, Yoshimura H

机构信息

Department of Hygienic Chemistry, Faculty of Pharmaceutical Sciences, Hokuriku University, Kanazawa, Japan.

出版信息

Pharmacol Biochem Behav. 1991 Nov;40(3):541-6. doi: 10.1016/0091-3057(91)90360-e.

Abstract

Cannabielsoin (CBE) was identified as a novel metabolite of cannabidiol (CBD) in the guinea pig in vivo and in vitro. Its formation by liver microsomes of guinea pigs needed NADPH and molecular oxygen, and was inhibited with SKF 525-A, metyrapone and alpha-naphthoflavone, indicating participation of cytochrome P-450 (P-450). The CBE-forming activity was highest in guinea pigs, followed by mice, rabbits and rats. In the rat, sex difference was found in the CBE formation (male greater than female). CBD monomethylether (CBDM) was also biotransformed to CBE monomethylether (CBEM) in the guinea pig in vivo and in vitro. When CBD dimethylether (CBDD) was employed as substrate, 1S,2R-epoxy-CBDD was identified. The results suggest that CBD and CBDM are biotransformed by P-450 to CBE-type metabolites via 1S,2R-epoxides. In pharmacological studies using mice, CBDD and 1S,2R-epoxy-CBD-2',6'-diacetate produced hypothermia, and CBD, CBDM and CBEM prolonged pentobarbital-induced sleep. Moreover, 1S,2R-epoxy-CBD-2',6'-diacetate was examined in the Ames test, but had no mutagenicity.

摘要

大麻二酚醇(CBE)在豚鼠体内和体外被鉴定为大麻二酚(CBD)的一种新型代谢产物。豚鼠肝脏微粒体形成CBE需要NADPH和分子氧,且会被SKF 525 - A、甲吡酮和α - 萘黄酮抑制,表明细胞色素P - 450(P - 450)参与其中。形成CBE的活性在豚鼠中最高,其次是小鼠、兔子和大鼠。在大鼠中,发现CBE形成存在性别差异(雄性大于雌性)。CBD单甲醚(CBDM)在豚鼠体内和体外也会生物转化为CBE单甲醚(CBEM)。当使用CBD二甲醚(CBDD)作为底物时,鉴定出了1S,2R - 环氧 - CBDD。结果表明,CBD和CBDM通过P - 450经1S,2R - 环氧化物生物转化为CBE型代谢产物。在使用小鼠的药理学研究中,CBDD和1S,2R - 环氧 - CBD - 2',6' - 二乙酸酯会导致体温过低,而CBD、CBDM和CBEM会延长戊巴比妥诱导的睡眠时间。此外,对1S,2R - 环氧 - CBD - 2',6' - 二乙酸酯进行了艾姆斯试验,但它没有致突变性。

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