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Development and potential role of type-2 sodium-glucose transporter inhibitors for management of type 2 diabetes

机译:2型钠葡萄糖转运蛋白抑制剂的开发及其在2型糖尿病治疗中的潜在作用

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摘要

There is a recognized need for new treatment options for type 2 diabetes mellitus (T2DM). Recovery of glucose from the glomerular filtrate represents an important mechanism in maintaining glucose homeostasis and represents a novel target for the management of T2DM. Recovery of glucose from the glomerular filtrate is executed principally by the type 2 sodium-glucose cotransporter (SGLT2). Inhibition of SGLT2 promotes glucose excretion and normalizes glycemia in animal models. First reports of specifically designed SGLT2 inhibitors began to appear in the second half of the 1990s. Several candidate SGLT2 inhibitors are currently under development, with four in the later stages of clinical testing. The safety profile of SGLT2 inhibitors is expected to be good, as their target is a highly specific membrane transporter expressed almost exclusively within the renal tubules. One safety concern is that of glycosuria, which could predispose patients to increased urinary tract infections. So far the reported safety profile of SGLT2 inhibitors in clinical studies appears to confirm that the class is well tolerated. Where SGLT2 inhibitors will fit in the current cascade of treatments for T2DM has yet to be established. The expected favorable safety profile and insulin-independent mechanism of action appear to support their use in combination with other antidiabetic drugs. Promotion of glucose excretion introduces the opportunity to clear calories (80–90 g [300–400 calories] of glucose per day) in patients that are generally overweight, and is expected to work synergistically with weight reduction programs. Experience will most likely lead to better understanding of which patients are likely to respond best to SGLT2 inhibitors, and under what circumstances.
机译:对于2型糖尿病(T2DM)的新治疗选择存在公认的需求。从肾小球滤出液中回收葡萄糖代表了维持葡萄糖稳态的重要机制,并且是管理T2DM的新靶标。从肾小球滤液中回收葡萄糖主要由2型钠-葡萄糖共转运蛋白(SGLT2)执行。在动物模型中,SGLT2的抑制作用可促进葡萄糖排泄并使血糖正常化。特别设计的SGLT2抑制剂的第一批报告开始出现在1990年代的后半期。目前正在开发几种候选SGLT2抑制剂,其中四种在临床测试的后期阶段。 SGLT2抑制剂的安全性有望得到改善,因为它们的靶标是几乎只在肾小管内表达的高度特异性的膜转运蛋白。一个安全隐患是糖尿症,它可能使患者更易发生尿路感染。到目前为止,临床研究中已报道的SGLT2抑制剂的安全性概况似乎证实了该类药物的耐受性良好。 SGLT2抑制剂适合目前的T2DM治疗方案的地方尚未确定。预期的有利安全性和不依赖胰岛素​​的作用机制似乎支持它们与其他抗糖尿病药联合使用。促进葡萄糖排泄为一般超重的患者清除卡路里(每天80-90 g [300-400卡]的葡萄糖)提供了机会,并且有望与减肥计划协同工作。经验极有可能使您更好地了解哪些患者可能对SGLT2抑制剂的反应最佳,以及在何种情况下。

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