甲基乙二醛和晚期糖基化终产物受体与肥胖糖尿病ob/ob小鼠膀胱功能障碍有关的证据。

IF 3.7 2区 医学 Q1 PHYSIOLOGY
Akila L Oliveira, Matheus L Medeiros, Ana Carolina Ghezzi, Gabriel Alonso Dos Santos, Glaucia Coelho Mello, Fabiola Z Mónica, Edson Antunes
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引用次数: 1

摘要

糖尿病中的糖酵解超负荷导致高反应性二羰基化合物甲基乙二醛(MGO)的大量积累和晚期糖基化终产物(AGEs)的过量产生,这些终产物与其受体(RAGE)相互作用,导致糖尿病相关的大血管并发症。膀胱是与二羰基物质接触最多的器官,但对MGO AGEs RAGE途径对糖尿病相关膀胱功能障碍的重要性知之甚少。在此,我们旨在研究MGO-AGEs-RAGE通路在糖尿病雄性和雌性ob/ob小鼠与野生型(WT)瘦小鼠膀胱功能障碍中的作用。糖尿病ob/ob小鼠在饮用水中用AGE破乳剂(ALT-711,1mg/kg)治疗8wk。与野生型动物相比,雄性和雌性ob/ob小鼠表现出明显的高血糖和胰岛素抵抗,而液体摄入保持不变。膀胱组织中的总AGEs、MGO衍生的氢咪唑酮1和RAGE水平,以及血清中的荧光AGEs水平,在任何性别的ob/ob小鼠中都显著升高。ob/ob小鼠膀胱中的胶原蛋白含量也显著升高。清醒小鼠滤纸中的斑点分析显示,ob/ob小鼠的总空隙体积和每个空隙的体积显著增加,而斑点数量没有改变。ALT-711治疗显著降低ob/ob小鼠的MGO、AGEs、RAGE和胶原含量。此外,ALT-711治疗使ob/ob小鼠的每个空隙的体积正常化,并增加了斑点的数量。MGO在膀胱壁激活AGEs-RAGE通路可能有助于糖尿病相关膀胱功能障碍的发病机制。新的和值得注意的是,本文研究了甲基乙二醛(MGO)和晚期糖基化终产物(AGEs)在用AGE阻断剂ALT-711治疗糖尿病ob/ob小鼠膀胱功能障碍中的作用。糖尿病小鼠在血清和/或膀胱组织中表现出高水平的MGO、AGEs、AGEs受体(RAGE)和胶原,并且每个空隙的体积增加,所有这些都被ALT-711降低。膀胱壁中MGO-AGEs-RAGE通路的激活有助于糖尿病相关膀胱功能障碍的发病机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Evidence that methylglyoxal and receptor for advanced glycation end products are implicated in bladder dysfunction of obese diabetic ob/ob mice.

Glycolytic overload in diabetes causes large accumulation of the highly reactive dicarbonyl compound methylglyoxal (MGO) and overproduction of advanced glycation end products (AGEs), which interact with their receptors (RAGE), leading to diabetes-associated macrovascular complications. The bladder is an organ that stays most in contact with dicarbonyl species, but little is known about the importance of the MGO-AGEs-RAGE pathway to diabetes-associated bladder dysfunction. Here, we aimed to investigate the role of the MGO-AGEs-RAGE pathway in bladder dysfunction of diabetic male and female ob/ob mice compared with wild-type (WT) lean mice. Diabetic ob/ob mice were treated with the AGE breaker alagebrium (ALT-711, 1 mg/kg) for 8 wk in drinking water. Compared with WT animals, male and female ob/ob mice showed marked hyperglycemia and insulin resistance, whereas fluid intake remained unaltered. Levels of total AGEs, MGO-derived hydroimidazolone 1, and RAGE in bladder tissues, as well as fluorescent AGEs in serum, were significantly elevated in ob/ob mice of either sex. Collagen content was also markedly elevated in the bladders of ob/ob mice. Void spot assays in filter paper in conscious mice revealed significant increases in total void volume and volume per void in ob/ob mice with no alterations of spot number. Treatment with ALT-711 significantly reduced the levels of MGO, AGEs, RAGE, and collagen content in ob/ob mice. In addition, ALT-711 treatment normalized the volume per void and increased the number of spots in ob/ob mice. Activation of AGEs-RAGE pathways by MGO in the bladder wall may contribute to the pathogenesis of diabetes-associated bladder dysfunction.NEW & NOTEWORTHY The involvement of methylglyoxal (MGO) and advanced glycation end products (AGEs) in bladder dysfunction of diabetic ob/ob mice treated with the AGE breaker ALT-711 was investigated here. Diabetic mice exhibited high levels of MGO, AGEs, receptor for AGEs (RAGE), and collagen in serum and/or bladder tissues along with increased volume per void, all of which were reduced by ALT-711. Activation of the MGO-AGEs-RAGE pathway in the bladder wall contributes to the pathogenesis of diabetes-associated bladder dysfunction.

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来源期刊
CiteScore
8.40
自引率
7.10%
发文量
154
审稿时长
2-4 weeks
期刊介绍: The American Journal of Physiology - Renal Physiology publishes original manuscripts on timely topics in both basic science and clinical research. Published articles address a broad range of subjects relating to the kidney and urinary tract, and may involve human or animal models, individual cell types, and isolated membrane systems. Also covered are the pathophysiological basis of renal disease processes, regulation of body fluids, and clinical research that provides mechanistic insights. Studies of renal function may be conducted using a wide range of approaches, such as biochemistry, immunology, genetics, mathematical modeling, molecular biology, as well as physiological and clinical methodologies.
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