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δ-8-四氢大麻酚、δ-9-四氢大麻酚和非那δ-8-四氢大麻酚甲基同系物在小鼠体内的代谢

In vivo metabolism of the methyl homologues of delta-8-tetrahydrocannabinol, delta-9-tetrahydrocannabinol and abn-delta-8-tetrahydrocannabinol in the mouse.

作者信息

Brown N K, Harvey D J

机构信息

University Department of Pharmacology, Oxford, UK.

出版信息

Biomed Environ Mass Spectrom. 1988 Apr 1;15(7):389-98. doi: 10.1002/bms.1200150706.

Abstract

Methyl-delta-8-tetrahydrocannabinol (methyl-delta-8-THC), methyl-delta-9-THC and abn-methyl-delta-8-THC were synthesized by condensation of orcinol and (1S)-cis-verbenol and were administered to male Charles River CD-1 mice. Extracted hepatic metabolites were isolated by chromatography on Sephadex LH-20 and examined by gas chromatography/mass spectrometry as trimethylsilyl (TMS), (2H9)TMS and methyl ester/TMS derivatives. In addition, metabolic fractions were reduced with lithium aluminium deuteride to convert carboxylic acids to alcohols for structural correlation. Metabolites from methyl-delta-8-THC were similar with respect to the positions substituted to those produced by higher homologues; the major metabolite was methyl-delta-8-THC-11-oic acid. abn-Methyl-delta-8-THC was metabolized in a different manner. The location of the aromatic methyl group at the position adjacent to ring fusion appeared to inhibit metabolism at C(11) to a considerable extent and also to reduce the amount of the resulting alcohol from being oxidized to a carboxylic acid. This caused other metabolic pathways to become dominant, with the result that a compound containing a hydroxy group at the gem-methyl position was the major metabolite. Hydroxylation at this position has not been confirmed with any other cannabinoid, although it is thought to result in trace concentrations of hydroxy metabolites from some compounds. Metabolism of methyl-delta-9-THC was also similar to that of the higher homologues, with the exception that less metabolism occurred at C(8) and a higher percentage of the total metabolic fraction was accounted for by the 11-oic acid metabolite. Minor metabolites were mainly dihydroxy compounds and hydroxylated derivatives of delta-9-THC-11-oic acid.

摘要

通过邻苯二酚和(1S)-顺式马鞭草烯醇的缩合反应合成了甲基-δ-8-四氢大麻酚(methyl-delta-8-THC)、甲基-δ-9-四氢大麻酚和异常甲基-δ-8-四氢大麻酚,并将其给予雄性查尔斯河CD-1小鼠。通过在葡聚糖凝胶LH-20上进行色谱分离来分离提取的肝脏代谢物,并通过气相色谱/质谱法作为三甲基硅烷基(TMS)、(2H9)TMS和甲酯/TMS衍生物进行检测。此外,用氘代氢化铝锂还原代谢组分,将羧酸转化为醇以进行结构关联。甲基-δ-8-THC的代谢物在取代位置方面与较高同系物产生的代谢物相似;主要代谢物是甲基-δ-8-THC-11-酸。异常甲基-δ-8-THC以不同的方式代谢。与环融合相邻位置的芳香甲基的位置似乎在很大程度上抑制了C(11)处的代谢,并且还减少了所得醇被氧化为羧酸的量。这导致其他代谢途径占主导地位,结果是在偕甲基位置含有羟基的化合物成为主要代谢物。尽管认为某些化合物会产生痕量浓度的羟基代谢物,但尚未在任何其他大麻素中证实该位置的羟基化。甲基-δ-9-THC的代谢也与较高同系物相似,不同之处在于C(8)处的代谢较少,并且11-酸代谢物在总代谢组分中所占的百分比更高。次要代谢物主要是二羟基化合物和δ-9-THC-11-酸的羟基化衍生物。

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