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抑制肾脏葡萄糖重吸收作为糖尿病患者的一种新治疗方法。

Inhibition of renal glucose reabsorption as a novel treatment for diabetes patients.

作者信息

Cersosimo Eugenio, Solis-Herrera Carolina, Triplitt Curtis

机构信息

Health Science Center San Antonio, University of Texas, Texas.

出版信息

J Bras Nefrol. 2014 Jan-Mar;36(1):80-92. doi: 10.5935/0101-2800.20140014.

DOI:10.5935/0101-2800.20140014
PMID:24676619
Abstract

UNLABELLED

The importance of the kidney in glucose homeostasis has been recognized for many years. Recent observations indicating a greater role of renal glucose metabolism in various physiologic and pathologic conditions have rekindled the interest in renal glucose handling as a potential target for the treatment of diabetes. The enormous capacity of the proximal tubular cells to reabsorb the filtered glucose load entirely, utilizing the sodium-glucose co-transporter system (primarily SGLT-2), became the focus of attention. Original studies conducted in experimental animals with the nonspecific SGLT inhibitor phlorizin showed that hyperglycemia after pancreatectomy decreased as a result of forced glycosuria. Subsequently, several compounds with more selective SGLT-2 inhibition properties ("second-generation") were developed. Some agents made it into pre-clinical and clinical trials and a few have already been approved for commercial use in the treatment of type 2 diabetes. In general, a 6-month period of therapy with SGLT-2 inhibitors is followed by a mean urinary glucose excretion rate of ~80 g/day accompanied by a decline in fasting and postprandial glucose with average decreases in HgA1C ~1.0%. Concomitant body weight loss and a mild but consistent drop in blood pressure also have been reported. In contrast, transient polyuria, thirst with dehydration and occasional hypotension have been described early in the treatment. In addition, a significant increase in the occurrence of uro-genital infections, particularly in women has been documented with the use of SGLT-2 inhibitors.

CONCLUSION

Although long-term cardiovascular, renal and bone/mineral effects are unknown SGLT-2 inhibitors, if used with caution and in the proper patient provide a unique insulin-independent therapeutic option in the management of obese type 2 diabetes patients.

摘要

未标注

肾脏在葡萄糖稳态中的重要性已被认识多年。最近的观察表明,肾脏葡萄糖代谢在各种生理和病理状况中发挥着更大的作用,这重新引发了人们对肾脏葡萄糖处理作为糖尿病潜在治疗靶点的兴趣。近端肾小管细胞利用钠-葡萄糖共转运系统(主要是SGLT-2)完全重吸收滤过的葡萄糖负荷的巨大能力成为了关注焦点。在实验动物中使用非特异性SGLT抑制剂根皮苷进行的原始研究表明,胰腺切除术后的高血糖症因强制性糖尿而降低。随后,开发了几种具有更具选择性的SGLT-2抑制特性的化合物(“第二代”)。一些药物进入了临床前和临床试验阶段,少数已被批准用于2型糖尿病的商业治疗。一般来说,使用SGLT-2抑制剂治疗6个月后,平均尿葡萄糖排泄率约为80克/天,同时空腹和餐后血糖下降,糖化血红蛋白平均下降约1.0%。还报告了伴随的体重减轻和血压轻度但持续下降。相比之下,治疗早期出现了短暂性多尿、口渴伴脱水以及偶尔的低血压。此外,使用SGLT-2抑制剂已记录到泌尿生殖系统感染的发生率显著增加,尤其是在女性中。

结论

尽管SGLT-2抑制剂的长期心血管、肾脏和骨骼/矿物质影响尚不清楚,但如果谨慎使用并针对合适的患者,它们在肥胖2型糖尿病患者的管理中提供了一种独特的非胰岛素依赖治疗选择。

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