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Drug Therapy in Obesity: A Review of Current and Emerging Treatments

机译:肥胖症的药物治疗:对当前和新发现的审查

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Whilst the prevalence of obesity continues to increase at an alarming rate worldwide, the personal and economic burden of obesity-related complications becomes ever more important. Whilst dietary and lifestyle measures remain the fundamental focus of the patient to counter obesity, more frequently pharmacological and/or surgical interventions are required. Nevertheless, these therapies are often limited by weight loss efficacy, side effects, surgical risks and frequently obesity relapse. Currently, only five drug therapies are approved for the specific treatment of obesity. However, our understanding of the pathophysiology of obesity and of gut hormones has developed precipitously over the last 20–30?years. As a result, there has been a recent movement to create and use analogues that manipulate these gut hormones to support weight loss. In this article we review the efficacy of the currently approved drug therapies and discuss future potential drug mechanisms and early clinical trial results exploring these budding avenues. We discuss the use of glucagon-like peptide-1 (GLP-1) analogues as monotherapy and unimolecular dual or triple agonists that exploit the GLP-1 receptor and/or the gastric inhibitory peptide (GIP) receptor and/or the glucagon receptor. We also explore the use of sodium-glucose co-transporter-2 (SGLT-2) inhibitors, amylin mimetics, leptin analogues, ghrelin antagonists and centrally acting agents to suppress appetite [neuropeptide Y (NPY) antagonists, melanocortin-4 receptor (MC4R) agonists and cannabinoid-1 receptor antagonists]. Whilst further evidence is required to support their clinical use, preclinical and early clinical trial results are encouraging.
机译:虽然肥胖的患病率在全球范围内令人震惊的速度继续增加,但肥胖相关的并发症的个人和经济负担变得更加重要。虽然饮食和生活方式措施仍然是患者对抗肥胖的基本焦点,但需要更频繁的药理学和/或手术干预。然而,这些疗法通常受重量损失功效,副作用,手术风险和经常肥胖复发的限制。目前,只有五种药物疗法被批准用于肥胖的具体治疗。然而,我们对肥胖症和肠道荷尔蒙的病理生理学的理解已经在过去20-30中急剧发展了。结果,最近的一个运动来创造和使用操纵这些肠道激素来支持减肥的类似物。在本文中,我们审查了目前批准的药物疗法的疗效,并讨论了未来的潜在药物机制和早期临床试验结果,探索这些崭露头角的途径。我们讨论了胰高血糖素类肽-1(GLP-1)类似物作为单药治疗和单疗法的双重或三重激动剂,其利用GLP-1受体和/或胃抑制肽(GIP)受体和/或胰高血糖素受体。我们还探讨了钠葡萄糖共转运蛋白-2(SGLT-2)抑制剂,淀粉蛋白模拟物,瘦素类似物,Ghrelin拮抗剂和中央作用剂来抑制食欲[神经肽Y(NPY)拮抗剂,Melanocortin-4受体(MC4R )激动剂和大麻素-1受体拮抗剂]。虽然需要进一步的证据来支持其临床使用,但临床前和早期的临床试验令人鼓舞。

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