Godschall Elizabeth N, Gungul Taha Bugra, Sajonia Isabelle R, Buyukaksakal Aleyna K, Li Orien Dong-Ang, Ogilvie Sophia, Keeler Austin B, Tian Guilian, Koita Omar, Shi Yu, Deutsch Tyler C J, Crook Maisie, Zhang YuChen, Conley Nicholas J, Webster Addison N, Calhan O Yipkin, Liu Weile, Akkoub Amani, Malik Karan, West Kaleigh I, Michel-Le Sara, Karthikeyan Arun, van Gerven Grace, Beier Kevin T, Zweifel Larry S, Patel Manoj K, Campbell John N, Deppmann Christopher D, Güler Ali D
bioRxiv. 2025 Jun 14:2024.12.12.628169. doi: 10.1101/2024.12.12.628169.
Glucagon-like peptide-1 receptor agonists (GLP1RAs) effectively reduce body weight and improve metabolic outcomes, yet established peptide-based therapies require injections and complex manufacturing. Small-molecule GLP1RAs promise oral bioavailability and scalable manufacturing, but their selective binding to human versus rodent receptors has limited mechanistic studies. Here, we developed humanized GLP1R mouse models to investigate how small-molecule GLP1RAs influence feeding behavior. This approach revealed that these compounds regulate both homeostatic and hedonic feeding through parallel neural circuits. Beyond engaging canonical hypothalamic and hindbrain networks that control metabolic homeostasis, GLP1RAs recruit a discrete population of Glp1r-expressing neurons in the central amygdala, which selectively suppress the consumption of palatable foods by reducing dopamine release in the nucleus accumbens. Stimulating these central amygdalar neurons curtail hedonic feeding, whereas targeted deletion of the receptor in this cell population specifically diminishes the anorectic efficacy of GLP1RAs for reward-driven intake. These findings reveal a dedicated neural circuit through which small molecule GLP1RAs modulate reward processing, suggesting broad therapeutic potential in conditions of dysregulated dopamine signaling including substance use disorder and binge eating.
胰高血糖素样肽-1受体激动剂(GLP1RAs)能有效减轻体重并改善代谢指标,但现有的基于肽的疗法需要注射且生产复杂。小分子GLP1RAs有望实现口服生物利用度和可扩展生产,但其与人源和啮齿动物受体的选择性结合限制了机制研究。在此,我们开发了人源化GLP1R小鼠模型,以研究小分子GLP1RAs如何影响进食行为。该方法揭示,这些化合物通过平行神经回路调节稳态性进食和享乐性进食。除了激活控制代谢稳态的经典下丘脑和后脑网络外,GLP1RAs还招募了中央杏仁核中一群表达Glp1r的离散神经元,这些神经元通过减少伏隔核中的多巴胺释放来选择性抑制美味食物的摄入。刺激这些中央杏仁核神经元可减少享乐性进食,而在该细胞群体中靶向删除该受体则会特异性降低GLP1RAs对奖励驱动性摄入的厌食效果。这些发现揭示了一条小分子GLP1RAs调节奖励处理的专用神经回路,提示在多巴胺信号失调的病症(包括物质使用障碍和暴饮暴食)中具有广泛的治疗潜力。
