The Structure-Function Relationships of Classical Cannabinoids: CB1/CB2 Modulation.

Perspectives in medicinal chemistry Pub Date : 2016-06-28 eCollection Date: 2016-01-01 DOI:10.4137/PMC.S32171

Eric W Bow, John M Rimoldi

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Abstract

The cannabinoids are members of a deceptively simple class of terpenophenolic secondary metabolites isolated from Cannabis sativa highlighted by (-)-Δ(9)-tetrahydrocannabinol (THC), eliciting distinct pharmacological effects mediated largely by cannabinoid receptor (CB1 or CB2) signaling. Since the initial discovery of THC and related cannabinoids, synthetic and semisynthetic classical cannabinoid analogs have been evaluated to help define receptor binding modes and structure-CB1/CB2 functional activity relationships. This perspective will examine the classical cannabinoids, with particular emphasis on the structure-activity relationship of five regions: C3 side chain, phenolic hydroxyl, aromatic A-ring, pyran B-ring, and cyclohexenyl C-ring. Cumulative structure-activity relationship studies to date have helped define the critical structural elements required for potency and selectivity toward CB1 and CB2 and, more importantly, ushered the discovery and development of contemporary nonclassical cannabinoid modulators with enhanced physicochemical and pharmacological profiles.

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经典大麻素的结构-功能关系：CB1/CB2 调节。

大麻素是从大麻（Cannabis sativa）中分离出来的萜酚类次生代谢物，其特征是 (-)-Δ(9)-tetrahydrocannabinol (THC)，主要通过大麻素受体（CB1 或 CB2）信号传导产生不同的药理作用。自最初发现四氢大麻酚和相关大麻素以来，已对合成和半合成的经典大麻素类似物进行了评估，以帮助确定受体结合模式和结构-CB1/CB2 功能活性关系。本视角将研究经典大麻素，尤其侧重于五个区域的结构-活性关系：C3 侧链、酚羟基、芳香 A 环、吡喃 B 环和环己烯 C 环。迄今为止，累积的结构-活性关系研究已帮助确定了对 CB1 和 CB2 的效力和选择性所需的关键结构元素，更重要的是，为发现和开发理化和药理特征更强的当代非经典大麻素调节剂开辟了道路。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Perspectives in medicinal chemistry

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