GLP-1 physiology in obesity and development of incretin-based drugs for chronic weight management

IF 18.9 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM Nature metabolism Pub Date : 2024-08-19 DOI:10.1038/s42255-024-01113-9
Jens Juul Holst
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Abstract

The introduction of the highly potent incretin receptor agonists semaglutide and tirzepatide has marked a new era in the treatment of type 2 diabetes and obesity. With normalisation of glycated haemoglobin levels and weight losses around 15–25%, therapeutic goals that were previously unrealistic are now within reach, and clinical trials have documented that these effects are associated with reduced risk of cardiovascular events and premature mortality. Here, I review this remarkable development from the earliest observations of glucose lowering and modest weight losses with native glucagon-like peptide (GLP)-1 and short acting compounds, to the recent development of highly active formulations and new molecules. I will classify these agents as GLP-1-based therapies in the understanding that these compounds or combinations may have actions on other receptors as well. The physiology of GLP-1 is discussed as well as its mechanisms of actions in obesity, in particular, the role of sensory afferents and GLP-1 receptors in the brain. I provide details regarding the development of GLP-1 receptor agonists for anti-obesity therapy and discuss the possible mechanism behind their beneficial effects on adverse cardiovascular events. Finally, I highlight new pharmacological developments, including oral agents, and discuss important questions regarding maintenance therapy. Holst reflects on the development of GLP-1-based drugs for the therapy of obesity, from early observations to remarkable results in more recent clinical trials, discussing physiological, pharmacological and clinical considerations related to their use.

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肥胖症中的 GLP-1 生理机理以及开发基于增量素的慢性体重控制药物
强效增量素受体激动剂semaglutide和tirzepatide的问世标志着2型糖尿病和肥胖症治疗进入了一个新时代。随着糖化血红蛋白水平趋于正常和体重减轻约15%-25%,以前不切实际的治疗目标现在变得触手可及,临床试验证明,这些效果与心血管事件和过早死亡风险的降低有关。在此,我将回顾这一显著的发展,从最早观察到的使用原生胰高血糖素样肽(GLP)-1 和短效化合物降低血糖和适度减轻体重,到最近开发的高活性制剂和新分子。我将把这些药物归类为基于 GLP-1 的疗法,因为这些化合物或组合可能对其他受体也有作用。我将讨论 GLP-1 的生理学及其在肥胖症中的作用机制,特别是大脑中感觉传入和 GLP-1 受体的作用。我详细介绍了用于抗肥胖治疗的 GLP-1 受体激动剂的发展情况,并讨论了其对不良心血管事件产生有益影响的可能机制。最后,我重点介绍了包括口服药物在内的新药理学发展,并讨论了有关维持治疗的重要问题。
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来源期刊
Nature metabolism
Nature metabolism ENDOCRINOLOGY & METABOLISM-
CiteScore
27.50
自引率
2.40%
发文量
170
期刊介绍: Nature Metabolism is a peer-reviewed scientific journal that covers a broad range of topics in metabolism research. It aims to advance the understanding of metabolic and homeostatic processes at a cellular and physiological level. The journal publishes research from various fields, including fundamental cell biology, basic biomedical and translational research, and integrative physiology. It focuses on how cellular metabolism affects cellular function, the physiology and homeostasis of organs and tissues, and the regulation of organismal energy homeostasis. It also investigates the molecular pathophysiology of metabolic diseases such as diabetes and obesity, as well as their treatment. Nature Metabolism follows the standards of other Nature-branded journals, with a dedicated team of professional editors, rigorous peer-review process, high standards of copy-editing and production, swift publication, and editorial independence. The journal has a high impact factor, has a certain influence in the international area, and is deeply concerned and cited by the majority of scholars.
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