Should GLP-1 receptor agonist therapy be used to treat obesity in Bardet-Biedl syndrome?

Jeremy W Tomlinson
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Abstract

Bardet-Biedl syndrome (BBS) is a complex genetic condition that can affect multiple organ systems, frequently causing pigmentary retinopathy, renal abnormalities, polydactyly, and obesity. Metabolic disturbances including obesity, unsuppressed appetite, and an increased risk of type 2 diabetes (T2D) present clinical management challenges. In this issue of the JCI, Singh et al. present a mouse model of a specific BBS subtype with genetic deletion of the Bbs5 gene. The model recapitulates many of the clinical features observed in patients living with BBS5 and sheds light on adipocyte biology, as well as the hypothalamic mechanisms driving hunger- and food-seeking behaviors that fuel the adverse metabolic phenotype. Importantly, exogenous GLP-1 receptor agonist treatment suppressed both appetite and weight, opening opportunities for direct translation into the clinical setting.
是否应该使用GLP-1受体激动剂治疗Bardet-Biedl综合征的肥胖?
Bardet-Biedl综合征(BBS)是一种复杂的遗传性疾病,可影响多器官系统,常引起色素视网膜病变、肾脏异常、多指畸形和肥胖。代谢紊乱包括肥胖、未抑制的食欲和2型糖尿病(T2D)风险增加,这些都是临床管理的挑战。在本期的JCI中,Singh等人提出了一种具有Bbs5基因基因缺失的特定BBS亚型小鼠模型。该模型概括了在BBS5患者中观察到的许多临床特征,并揭示了脂肪细胞生物学,以及驱动饥饿和寻找食物行为的下丘脑机制,这些行为加剧了不良的代谢表型。重要的是,外源性GLP-1受体激动剂治疗抑制食欲和体重,为直接转化为临床环境打开了机会。
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