The Pathophysiological Basis of Diabetic Kidney Protection by Inhibition of SGLT2 and SGLT1.

Kidney and dialysis Pub Date : 2022-06-01 Epub Date: 2022-06-18 DOI:10.3390/kidneydial2020032
Yuji Oe, Volker Vallon
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引用次数: 1

Abstract

SGLT2 inhibitors can protect the kidneys of patients with and without type 2 diabetes mellitus and slow the progression towards end-stage kidney disease. Blocking tubular SGLT2 and spilling glucose into the urine, which triggers a metabolic counter-regulation similar to fasting, provides unique benefits, not only as an anti-hyperglycemic strategy. These include a low hypoglycemia risk and a shift from carbohydrate to lipid utilization and mild ketogenesis, thereby reducing body weight and providing an additional energy source. SGLT2 inhibitors counteract hyperreabsorption in the early proximal tubule, which acutely lowers glomerular pressure and filtration and thereby reduces the physical stress on the filtration barrier, the filtration of tubule-toxic compounds, and the oxygen demand for tubular reabsorption. This improves cortical oxygenation, which, together with lesser tubular gluco-toxicity and improved mitochondrial function and autophagy, can reduce pro-inflammatory, pro-senescence, and pro-fibrotic signaling and preserve tubular function and GFR in the long-term. By shifting transport downstream, SGLT2 inhibitors more equally distribute the transport burden along the nephron and may mimic systemic hypoxia to stimulate erythropoiesis, which improves oxygen delivery to the kidney and other organs. SGLT1 inhibition improves glucose homeostasis by delaying intestinal glucose absorption and by increasing the release of gastrointestinal incretins. Combined SGLT1 and SGLT2 inhibition has additive effects on renal glucose excretion and blood glucose control. SGLT1 in the macula densa senses luminal glucose, which affects glomerular hemodynamics and has implications for blood pressure control. More studies are needed to better define the therapeutic potential of SGLT1 inhibition to protect the kidney, alone or in combination with SGLT2 inhibition.

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抑制SGLT2和SGLT1对糖尿病肾保护的病理生理基础。
SGLT2抑制剂可以保护2型糖尿病患者和非2型糖尿病患者的肾脏,减缓终末期肾病的进展。阻断管状SGLT2并将葡萄糖溢出到尿液中,这触发了类似于禁食的代谢反调节,提供了独特的益处,不仅是一种抗高血糖策略。这些包括低血糖风险,从碳水化合物到脂质利用的转变和轻度的生酮,从而减轻体重并提供额外的能量来源。SGLT2抑制剂对抗早期近端小管的高重吸收,从而急剧降低肾小球压力和滤过,从而减少滤过屏障的物理应激、小管毒性化合物的过滤和小管重吸收的需氧量。这改善了皮质氧合,减少了小管糖毒性,改善了线粒体功能和自噬,可以减少促炎、促衰老和促纤维化信号,长期保持小管功能和GFR。通过向下游转移运输,SGLT2抑制剂更均匀地沿肾元分配运输负担,并可能模拟全身性缺氧刺激红细胞生成,从而改善肾和其他器官的氧气输送。抑制SGLT1通过延缓肠道葡萄糖吸收和增加胃肠道肠促胰岛素的释放来改善葡萄糖稳态。联合抑制SGLT1和SGLT2对肾糖排泄和血糖控制具有加性作用。黄斑致密区SGLT1感知腔内葡萄糖,影响肾小球血流动力学并影响血压控制。需要更多的研究来更好地确定SGLT1抑制单独或联合SGLT2抑制保护肾脏的治疗潜力。
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