肾近端小管细胞对葡萄糖的反应中纤连蛋白积累是多元醇途径依赖性的。

Renal proximal tubular cell fibronectin accumulation in response to glucose is polyol pathway dependent.

作者信息

Morrisey K, Steadman R, Williams J D, Phillips A O

机构信息

Institute of Nephrology, University of Wales College of Medicine, Cardiff Royal Infirmary, Newport Road, Cardiff, Wales, United Kingdom.

出版信息

Kidney Int. 1999 Jan;55(1):160-7. doi: 10.1046/j.1523-1755.1999.00248.x.

DOI:10.1046/j.1523-1755.1999.00248.x

PMID:9893124

Abstract

BACKGROUND

Thickening and reduplication of the tubular basement membrane have been reported as early events in diabetic nephropathy. In this study, we have examined the polar requirements of proximal tubular cells for the d-glucose-stimulated accumulation of fibronectin and the mechanism by which this occurred, with particular emphasis on the polyol pathway.

METHODS

To determine the polarity of fibronectin generation in response to glucose, LLC-PK1 cells were grown on porous tissue culture inserts. Monolayer confluence was determined by serial measurement of transepithelial resistance. Confluent cells were growth arrested by serum deprivation, and all experiments were performed under serum-free conditions.

RESULTS

Application of 25 mm d-glucose to either the apical or basolateral aspect of LLC-PK1 cells led to fibronectin accumulation in the basolateral compartment. This reached statistical significance 24 hours following apical addition of glucose (2.6-fold increase compared with 5 mm d-glucose, P = 0.0025, N = 6 vs. N = 4 controls) and 12 hours after the basolateral addition of glucose (2.5-fold increase compared with 5 mm d-glucose, P = 0.03, N = 6 vs. N = 4 controls). Exposure of cells to glucose at either their apical or basolateral aspect leads to accumulation of intracellular glucose and polyol pathway activation, as assessed by sorbitol accumulation. The increase in fibronectin concentration in response to glucose was inhibited by the aldose reductase inhibitor sorbinil. At a dose of 100 micron sorbinil, there was a 59% inhibition of fibronectin accumulation in response to apical glucose (P = 0.004, N = 3 sorbinil vs. N = 4 controls) and a 66% inhibition in response to basolateral glucose (P = 0.008, N = 3 sorbinil vs. N = 4 controls) 48 hours after the addition of the inhibitor. Furthermore, fibronectin accumulation was also demonstrated following both the apical and basolateral addition of 1 mm sorbitol, but not following the addition of 25 mm galactose to either aspect of the cells. Following the addition of sorbitol, there was a 2. 8-fold increase in fibronectin 48 hours after apical stimulation (P = 0.01, N = 3 treated vs. N = 4 control) and a 2.27-fold increase following basolateral stimulation (P = 0.04, N = 3 treated vs. N = 4 control) at 24 hours.

CONCLUSIONS

In summary, these data demonstrate that fibronectin generation in response to glucose was nonpolar in terms of application of glucose but was polar in terms of fibronectin accumulation. The mechanisms of glucose-induced modulation of fibronectin were mediated by polyol pathway activation and were more specifically related to the metabolism of sorbitol to fructose.

摘要

背景

肾小管基底膜增厚和重复已被报道为糖尿病肾病的早期事件。在本研究中，我们研究了近端肾小管细胞对d-葡萄糖刺激的纤连蛋白积累的极性需求及其发生机制，特别强调了多元醇途径。

方法

为了确定响应葡萄糖时纤连蛋白生成的极性，LLC-PK1细胞生长在多孔组织培养插入物上。通过连续测量跨上皮电阻来确定单层汇合情况。汇合细胞通过血清剥夺使其生长停滞，所有实验均在无血清条件下进行。

结果

将25 mM d-葡萄糖应用于LLC-PK1细胞的顶端或基底外侧，导致基底外侧隔室中纤连蛋白积累。在顶端添加葡萄糖后24小时达到统计学显著性（与5 mM d-葡萄糖相比增加2.6倍，P = 0.0025，N = 6对N = 4对照），在基底外侧添加葡萄糖后12小时达到统计学显著性（与5 mM d-葡萄糖相比增加2.5倍，P = 0.03，N = 6对N = 4对照）。细胞在其顶端或基底外侧暴露于葡萄糖会导致细胞内葡萄糖积累和多元醇途径激活，通过山梨醇积累评估。醛糖还原酶抑制剂索比尼尔抑制了响应葡萄糖时纤连蛋白浓度的增加。在剂量为100 μM索比尼尔时，在添加抑制剂48小时后，对顶端葡萄糖响应的纤连蛋白积累有59%的抑制（P = 0.004，N = 3索比尼尔对N = 4对照），对基底外侧葡萄糖响应有66%的抑制（P = 0.008，N = 3索比尼尔对N = 4对照）。此外，在顶端和基底外侧添加1 mM山梨醇后也证明了纤连蛋白积累，但在细胞的任何一侧添加25 mM半乳糖后未出现这种情况。添加山梨醇后，在顶端刺激48小时后纤连蛋白增加2.8倍（P = 0.01，N = 3处理对N = 4对照），在基底外侧刺激24小时后增加2.27倍（P = 0.04，N = 3处理对N = 4对照）。