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胰高血糖素样肽-2类似物在胃肠道疾病中的治疗潜力:当前认知、营养方面及未来展望

Therapeutic Potential of GLP-2 Analogs in Gastrointestinal Disorders: Current Knowledge, Nutritional Aspects, and Future Perspectives.

作者信息

Kounatidis Dimitris, Vallianou Natalia G, Tsilingiris Dimitrios, Christodoulatos Gerasimos Socrates, Geladari Eleni, Stratigou Theodora, Karampela Irene, Dalamaga Maria

机构信息

Departments of Internal Medicine and Endocrinology, Evangelismos General Hospital, 45-47 Ypsilantou Street, 10676, Athens, Greece.

First Department of Propaedeutic Internal Medicine, School of Medicine, National and Kapodistrian University of Athens, Laiko General Hospital, 17 St Thomas Street, 11527, Athens, Greece.

出版信息

Curr Nutr Rep. 2022 Dec;11(4):618-642. doi: 10.1007/s13668-022-00433-0. Epub 2022 Aug 6.

Abstract

PURPOSE OF REVIEW

Although Glucagon-like peptide (GLP)-1 receptor agonists have been used for almost two decades in the treatment of diabetes mellitus type 2 and, lately, in obesity, recent years have seen an increasing interest in the pharmacological agonism of other proglucagon-derived peptides, including GLP-2. Herein, we aimed to review the available evidence on the effects of GLP-2 agonism from animal and clinical studies. Furthermore, we summarize the current clinical applications of GLP-2 agonists among patients with intestinal failure associated with short bowel syndrome (SBS-IF) as well as potential future expansion of their indications to other intestinal disorders.

RECENT FINDINGS

Evidence from preclinical studies has highlighted the cellular trophic and functional beneficial actions of GLP-2 on small intestinal and colonic mucosa. Subsequently, pharmacologic agonism of GLP-2 has gathered interest for the treatment of patients with conditions pertaining to the loss of intestinal anatomical and/or functional integrity to a degree requiring parenteral support, collectively referred to as intestinal failure. GLP-2 analogs positively influence nutrient absorption in animal models and humans, although continued therapy is likely needed for sustained effects. The degradation-resistant GLP-2-analog teduglutide has received approval for the treatment of SBS-IF, in which it may decisively reduce patient dependency on parenteral support and improve quality of life. Another two longer-acting analogs, glepaglutide and apraglutide, are currently undergoing phase III clinical trials. The use of GLP-2 analogs is effective in the management of SBS-IF and may show promise in the treatment of other severe gastrointestinal disorders associated with loss of effective intestinal resorptive surface area.

摘要

综述目的

尽管胰高血糖素样肽(GLP)-1受体激动剂已用于治疗2型糖尿病近二十年,最近也用于治疗肥胖症,但近年来,人们对其他胰高血糖素衍生肽(包括GLP-2)的药理学激动作用越来越感兴趣。在此,我们旨在回顾动物和临床研究中关于GLP-2激动作用效果的现有证据。此外,我们总结了GLP-2激动剂在短肠综合征相关肠衰竭(SBS-IF)患者中的当前临床应用,以及其适应症未来可能扩展到其他肠道疾病的情况。

最新发现

临床前研究的证据突出了GLP-2对小肠和结肠黏膜的细胞营养和功能有益作用。随后,GLP-2的药理学激动作用引起了人们对治疗肠道解剖和/或功能完整性丧失到需要肠外支持程度的患者的兴趣,这些患者统称为肠衰竭。GLP-2类似物对动物模型和人类的营养吸收有积极影响,尽管可能需要持续治疗才能产生持续效果。抗降解的GLP-2类似物替度鲁肽已获批用于治疗SBS-IF,它可以决定性地减少患者对肠外支持的依赖并改善生活质量。另外两种长效类似物,格列鲁肽和阿普拉鲁肽,目前正在进行III期临床试验。GLP-2类似物在管理SBS-IF方面有效,并且在治疗其他与有效肠吸收表面积丧失相关的严重胃肠道疾病方面可能显示出前景。

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