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Orally active ghrelin receptor inverse agonists and their actions on a rat obesity model

机译:口服活性生长素释放肽受体反向激动剂及其对大鼠肥胖模型的作用

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摘要

A series of 2-alkylamino nicotinamide analogs was prepared as orally active ghrelin receptor (ghrelinR) inverse agonists. Starting from compound 1, oral bioavailability was improved by modifying metabolically unstable sites and reducing molecular weight. Brain-permeable compound 33 and compound 24 with low brain permeability were tested in rat models of obesity; 30 mg/kg of compound 33 suppressed weight gain. PK/PD analysis revealed that the anti-obesity effect of ghrelinR inverse agonists depends on their brain concentrations. (C) 2015 Elsevier Ltd. All rights reserved.
机译:制备一系列2-烷基氨基烟酰胺类似物作为口服活性生长素释放肽受体(ghrelinR)反向激动剂。从化合物1开始,通过修饰代谢不稳定的部位并降低分子量,可以提高口服生物利用度。在肥胖症大鼠模型中测试了具有低脑通透性的脑通透性化合物33和化合物24; 30 mg / kg的化合物33抑制了体重增加。 PK / PD分析显示,ghrelinR反向激动剂的抗肥胖作用取决于他们的大脑浓度。 (C)2015 Elsevier Ltd.保留所有权利。

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