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New developments in diabetes management: Medications of the 21st century

机译:糖尿病管理的新发展:21世纪的药物

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Background Suboptimal blood glucose control among patients with type 2 diabetes continues to support the need for new pharmacologic approaches. Objective The purpose of this commentary was to highlight newly available and soon-to-be available agents that are promising tools for targeting specific pathophysiologic pathways in the management of diabetes. Methods Published evidence to support the application of novel incretin-based therapies, dipeptidyl peptidase (DPP)-4 inhibitors, sodium-glucose cotransporter (SGLT)-2 inhibitors, other oral agents and insulins for managing specific aspects of type 2 diabetes, as well as disadvantages associated with those novel medications, are discussed. Results Several new glucagon-like peptide (GLP)-1 receptor agonists with different time frames of action, although each has unique advantages and disadvantages, have been through clinical trials. Examples of these are lixisenatide and albiglutide. Currently available DPP-4 inhibitor agents, important for inhibiting the breakdown of endogenous GLP-1, have not been associated with weight gain or hypoglycemia. SGLT-2 inhibitors, which do not depend on insulin secretion or insulin action, may be advantageous in that they appear to be broadly efficacious at all stages of diabetes. New insulin analogues, such as degludec and U-500, improve glycemic control without contributing to hypoglycemia. Conclusions Advances in pharmacologic options offer the promise of improving glycemic control for longer periods, with limited glycemic fluctuations, hypoglycemia, and weight gain. However, the effectiveness of these agents ultimately depends on their availability to providers managing the health care of patients at high risk for poor diabetes outcomes and patients' use of them as directed. Long-term effectiveness and safety trials are ongoing.
机译:背景2型糖尿病患者的血糖控制欠佳,继续支持对新药理学方法的需求。目的本评论的目的是强调新近可用和即将上市的药物,这些药物有望成为针对糖尿病管理中特定病理生理途径的工具。方法已发表的证据支持新的基于肠降血糖素的疗法,二肽基肽酶(DPP)-4抑制剂,钠葡萄糖共转运蛋白(SGLT)-2抑制剂,其他口服药物和胰岛素在2型糖尿病特定方面的治疗。讨论了与那些新型药物相关的缺点。结果几种具有不同作用时限的新型胰高血糖素样肽(GLP)-1受体激动剂,尽管每种都有独特的优缺点,但已经通过临床试验进行了研究。这些的例子是利西拉来肽和阿比鲁肽。对于抑制内源性GLP-1的分解很重要的目前可用的DPP-4抑制剂与体重增加或血糖过低无关。不依赖于胰岛素分泌或胰岛素作用的SGLT-2抑制剂可能是有利的,因为它们在糖尿病的所有阶段似乎都具有广泛的疗效。新的胰岛素类似物,例如degludec和U-500,可改善血糖控制,而不会导致低血糖症。结论药理学选择的进展为长期改善血糖控制,有限的血糖波动,低血糖和体重增加提供了希望。但是,这些药物的有效性最终取决于提供者的可用性,这些提供者可以管理糖尿病风险较高的高风险患者的医疗保健,并按指示使用患者。长期有效性和安全性试验正在进行中。

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