血清缺乏时抑制钠-葡萄糖共转运体-2 可通过 AMPK/AKT/FOXO 信号通路增加肝脏葡萄糖生成

IF 3.9 3区医学 Q2 ENDOCRINOLOGY & METABOLISM

Endocrinology and Metabolism Pub Date : 2024-02-01 Epub Date: 2024-01-03 DOI:10.3803/EnM.2023.1786

Jinmi Lee, Seok-Woo Hong, Min-Jeong Kim, Yu-Mi Lim, Sun Joon Moon, Hyemi Kwon, Se Eun Park, Eun-Jung Rhee, Won-Young Lee

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引用次数: 0

摘要

背景：钠依赖性葡萄糖共转运体2（SGLT2）介导肾近曲小管对葡萄糖的重吸收，SGLT2抑制剂被用作治疗2型糖尿病的药物。本研究旨在阐明 SGLT2 抑制剂在血清剥夺和血清补充状态下对肝脏葡萄糖代谢的影响和机制。方法：用 SGLT2 抑制剂 empagliflozin 和 dapagliflozin 处理 Huh7 细胞，研究 SGLT2 对肝脏葡萄糖摄取的影响。为了研究 SGLT2 抑制剂在血清缺失和血清补充条件下对葡萄糖代谢的调节作用，用 SGLT2 小干扰 RNA（siRNA）转染 HepG2 细胞，在无血清的杜氏改良鹰培养基中培养 16 小时，然后在补充或不补充 10%胎牛血清的培养基中培养 8 小时：结果：SGLT2 抑制剂剂量依赖性地降低了肝脏对葡萄糖的摄取。血清剥夺增加了葡萄糖生成基因过氧化物酶体增殖激活受体γ共激活剂1α（PGC-1α）、葡萄糖6-磷酸酶（G6pase）和磷酸烯醇丙酮酸羧激酶（PEPCK）的表达水平，在转染了SGLT2 siRNA的细胞中，血清剥夺期间这些基因的表达水平进一步增加。在血清缺失期间用 siRNA 抑制 SGLT2 会诱导转录因子叉头盒 O 类 1（FOXO1）的核定位，降低核磷酸化-AKT（p-AKT）和 p-FOXO1 蛋白的表达，并增加磷酸化腺苷酸单磷酸激活蛋白激酶（p-AMPK）蛋白的表达。然而，用 AMPK 抑制剂化合物 C 处理可逆转血清剥夺期间转染 SGLT2 siRNA 的细胞中核 p- AKT 和 p-FOXO1 蛋白表达水平的降低，并降低 p-AMPK 和 PEPCK 蛋白表达水平：这些数据表明，SGLT2 在肝细胞中介导葡萄糖摄取，血清剥夺期间抑制 SGLT2 可通过 AMPK/AKT/FOXO1 信号通路增加葡萄糖生成。

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Inhibition of Sodium-Glucose Cotransporter-2 during Serum Deprivation Increases Hepatic Gluconeogenesis via the AMPK/AKT/FOXO Signaling Pathway.

Backgruound: Sodium-dependent glucose cotransporter 2 (SGLT2) mediates glucose reabsorption in the renal proximal tubules, and SGLT2 inhibitors are used as therapeutic agents for treating type 2 diabetes mellitus. This study aimed to elucidate the effects and mechanisms of SGLT2 inhibition on hepatic glucose metabolism in both serum deprivation and serum supplementation states.

Methods: Huh7 cells were treated with the SGLT2 inhibitors empagliflozin and dapagliflozin to examine the effect of SGLT2 on hepatic glucose uptake. To examine the modulation of glucose metabolism by SGLT2 inhibition under serum deprivation and serum supplementation conditions, HepG2 cells were transfected with SGLT2 small interfering RNA (siRNA), cultured in serum-free Dulbecco's modified Eagle's medium for 16 hours, and then cultured in media supplemented with or without 10% fetal bovine serum for 8 hours.

Results: SGLT2 inhibitors dose-dependently decreased hepatic glucose uptake. Serum deprivation increased the expression levels of the gluconeogenesis genes peroxisome proliferator-activated receptor gamma co-activator 1 alpha (PGC-1α), glucose 6-phosphatase (G6pase), and phosphoenolpyruvate carboxykinase (PEPCK), and their expression levels during serum deprivation were further increased in cells transfected with SGLT2 siRNA. SGLT2 inhibition by siRNA during serum deprivation induces nuclear localization of the transcription factor forkhead box class O 1 (FOXO1), decreases nuclear phosphorylated-AKT (p-AKT), and p-FOXO1 protein expression, and increases phosphorylated-adenosine monophosphate-activated protein kinase (p-AMPK) protein expression. However, treatment with the AMPK inhibitor, compound C, reversed the reduction in the protein expression levels of nuclear p- AKT and p-FOXO1 and decreased the protein expression levels of p-AMPK and PEPCK in cells transfected with SGLT2 siRNA during serum deprivation.

Conclusion: These data show that SGLT2 mediates glucose uptake in hepatocytes and that SGLT2 inhibition during serum deprivation increases gluconeogenesis via the AMPK/AKT/FOXO1 signaling pathway.

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来源期刊

Endocrinology and Metabolism Medicine-Endocrinology, Diabetes and Metabolism

CiteScore

6.60

自引率

5.90%

发文量

145

审稿时长

24 weeks

期刊介绍： The aim of this journal is to set high standards of medical care by providing a forum for discussion for basic, clinical, and translational researchers and clinicians on new findings in the fields of endocrinology and metabolism. Endocrinology and Metabolism reports new findings and developments in all aspects of endocrinology and metabolism. The topics covered by this journal include bone and mineral metabolism, cytokines, developmental endocrinology, diagnostic endocrinology, endocrine research, dyslipidemia, endocrine regulation, genetic endocrinology, growth factors, hormone receptors, hormone action and regulation, management of endocrine diseases, clinical trials, epidemiology, molecular endocrinology, neuroendocrinology, neuropeptides, neurotransmitters, obesity, pediatric endocrinology, reproductive endocrinology, signal transduction, the anatomy and physiology of endocrine organs (i.e., the pituitary, thyroid, parathyroid, and adrenal glands, and the gonads), and endocrine diseases (diabetes, nutrition, osteoporosis, etc.).