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The discovery of taranabant, a selective cannabinoid-1 receptor inverse agonist for the treatment of obesity.

机译:taranabant的发现,一种选择性的大麻素1受体反向激动剂,用于治疗肥胖症。

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The cannabinoid-1 receptor (CB1R) has emerged as one of the most important targets for the treatment of obesity. Pioneering studies with rimonabant helped to validate animal models of food intake reduction and weight loss and made the connection to weight loss in the clinic. A novel, acyclic amide was identified from a high throughput screen (HTS) of the Merck sample collection and found to be a potent and selective CB1R inhibitor. Further optimization led to more potent compounds that were orally active in reducing food intake and weight loss in diet-induced obese (DIO) rats. However, many of these analogues exhibited a high potential for bioactivation and the formation of reactive intermediates and covalent protein binding. Identification of the products of oxidative metabolism guided medicinal chemistry efforts to minimize the formation of these unwanted products. These efforts resulted in the identification of the CB1R inverse agonist, taranabant, which is currently in Phase-III clinical studies for the treatment of obesity. This mini-review will describe some of the medicinal chemistry strategies that were followed from the original high throughput screen hit to the discovery of taranabant.
机译:大麻素1受体(CB1R)已成为治疗肥胖症的最重要靶标之一。利莫那班的开创性研究有助于验证减少食物摄入和减轻体重的动物模型,并在临床上将其与减轻体重联系起来。从默克样品收集的高通量筛选(HTS)中鉴定出一种新型的无环酰胺,它是一种有效的选择性CB1R抑制剂。进一步的优化导致了更有效的化合物,这些化合物在减少饮食诱导的肥胖(DIO)大鼠的食物摄入和减轻体重方面具有口服活性。但是,这些类似物中的许多都表现出很高的生物激活潜力,活性中间体的形成和共价蛋白结合。氧化代谢产物的鉴定指导了药物化学工作,以尽量减少这些不需要的产物的形成。这些努力导致鉴定出CB1R反向激动剂taranabant,该药物目前正在治疗肥胖的III期临床研究中。这份小型回顾将描述一些药物化学策略,从最初的高通量筛选到发现他拉班特,这些药物所遵循的策略。

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