嘌呤霉素氨基核苷肾病患者尿浓度缺陷与蛋白尿的关系。

Pub Date : 2020-12-01 Epub Date: 2020-12-28 DOI:10.5049/EBP.2020.18.2.31
Chor Ho Jo, Sua Kim, Gheun-Ho Kim
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引用次数: 1

摘要

背景:嘌呤霉素氨基核苷(PA)可诱导大鼠肾病综合征,蛋白尿是肾小球病变小管间质损伤的重要介质。我们假设肾小球蛋白尿可能影响小管功能,如尿浓度,并研究尿浓度缺陷是否与嘌呤霉素氨基核苷肾病(PAN)中的蛋白尿相关。我们还调查了依那普利的缺陷反应。方法:单次腹腔注射PA (150mg/kg BW)诱导雄性sd大鼠肾小球蛋白尿。在其中一半的大鼠中,每天在食物混合物中给予依那普利(35mg/kg BW),持续两周。动物实验结束后,取肾进行免疫印迹分析和组织病理学检查。结果:与对照组相比,pa处理大鼠出现严重的蛋白尿、多尿和较低的尿渗透压。PA处理诱导了显著的小管间质损伤,水通道蛋白-1和Na-K-2Cl 2型共转运蛋白(NKCC2)的蛋白丰度显著降低。蛋白尿与肾脏骨桥蛋白表达显著相关,与肾水通道蛋白-1、水通道蛋白-2和NKCC2表达负相关。小管间质损伤程度与蛋白尿、尿量和骨桥蛋白表达显著相关,与尿渗透压和肾水通道蛋白-1、水通道蛋白-2和NKCC2表达负相关。服用依那普利和不服用依那普利的pa处理大鼠在参数上没有显著差异。结论:肾小球蛋白尿与肾小管间质损伤及水利尿有关。下调水通道蛋白-1和NKCC2可损害逆流增殖并引起PAN尿浓度缺陷。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Association of Proteinuria with Urinary Concentration Defect in Puromycin Aminonucleoside Nephrosis.

Association of Proteinuria with Urinary Concentration Defect in Puromycin Aminonucleoside Nephrosis.

Association of Proteinuria with Urinary Concentration Defect in Puromycin Aminonucleoside Nephrosis.

Association of Proteinuria with Urinary Concentration Defect in Puromycin Aminonucleoside Nephrosis.

Background: Puromycin aminonucleoside (PA) can induce nephrotic syndrome in rats, and proteinuria is an important mediator of tubulointerstitial injury in glomerulopathy. We assumed that glomerular proteinuria may affect tubular function, such as urinary concentration, and investigated whether a urinary concentration defect is associated with proteinuria in puromycin aminonucleoside nephrosis (PAN). We also investigated the defect response to enalapril.

Methods: Glomerular proteinuria was induced by a single intraperitoneal injection of PA (150mg/kg BW) in male Sprague-Dawley rats. In a half of these rats, enalapril (35mg/kg BW) was administered daily in a food mixture for two weeks. After the animal experiment, kidneys were harvested for immunoblot analysis and histopathologic examination.

Results: Compared with the control group, PA-treated rats had severe proteinuria, polyuria, and a lower urine osmolality. PA treatment induced remarkable tubulointerstitial injury and significant reductions in protein abundances of aquaporin-1 and Na-K-2Cl co-transporter type 2 (NKCC2). Proteinuria significantly correlated with osteopontin expression in the kidney and inversely correlated with renal expression of aquaporin-1, aquaporin-2, and NKCC2. The degree of tubulointerstitial injury significantly correlated with proteinuria, urine output, and osteopontin expression and inversely correlated with urine osmolality and renal expression of aquaporin-1, aquaporin-2, and NKCC2. No significant differences in parameters were found between PA-treated rats with and without enalapril.

Conclusion: In PAN, glomerular proteinuria was associated with tubulointerstitial injury and water diuresis. Downregulation of aquaporin-1 and NKCC2 can impair countercurrent multiplication and cause a urinary concentration defect in PAN.

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