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Allosteric modulators of cannabinoid receptor 1: developing compounds for improved specificity

机译:大麻素受体1的变构调节剂:制育化合物,可改善特异性

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The cannabinoid receptor 1 (CB1) is a G protein-coupled receptor (GPCR) that is located primarily in the central nervous system. CB1 is a therapeutic target which may impact pathways to mediate pain, neurodegenerative disorders, hunger, and drug-seeking behavior. Despite these benefits, development of orthosteric therapeutic compounds, which target the endogenous ligand-binding site of CB1, has been challenging due to detrimental side effects including psychoactivity, depression, and suicidal thoughts. However, CB1 also has an allosteric binding site(s), which is topographically distinct from the orthosteric site. Allosteric modulation of CB1 has a number of potential advantages including providing a mechanism for more precise control of downstream pathways and circumventing these side effects. In this review, we summarize the concept of allosteric modulation and focus on the structure–activity relationship studies of the well-characterized allosteric modulators, ORG27569 and PSNCBAM-1 and their derivatives, and a few other recent modulators. We review studies on the properties of these modulators on CB1 signaling in cells and their effects in vivo. While many current allosteric modulators also produce complex outcomes, they provide new advances for the design of CB1 centered therapeutics
机译:大麻素受体1(CB1)是G蛋白偶联受体(GPCR),其主要位于中枢神经系统。 CB1是一种治疗靶标,可能影响静止疼痛,神经变性障碍,饥饿和寻求药物行为的途径。尽管有这些益处,但靶向CB1的内源性配体结合位点的正向治疗化合物,由于包括心理活动,抑郁和自杀思想等有害副作用,这一直挑战。然而,CB1还具有颠覆性粘合位点,其拓扑粘结位点与矫形位点不同。 CB1的变构调制具有许多潜在的优点,包括提供一种更精确控制下游途径的机制并避免这些副作用。在这篇综述中,我们总结了变构调制的概念,并专注于具有良好表征的崩解调节剂,ORG27569和PSNCBAM-1及其衍生物的结构 - 活性关系研究,以及其他几个最近调节剂。我们审查了对细胞中CB1信号传导的这些调节剂的性质及其在体内效应的研究。虽然许多目前的颠振调制器也会产生复杂的结果,但它们为CB1中心的治疗剂设计提供了新的进展

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