Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa: Unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder

LeiriaL.O.; SollonC.; BáuF.R.; MónicaF.Z.; DAnconaC.L.; DeNucciG.; GrantA.D.; AnhêG.F.; AntunesE.

首页> 外文期刊>The Journal of Physiology >Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa: Unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder

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Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa: Unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder

机译：胰岛素通过PI3K / AKT / eNOS途径激活粘膜使膀胱松弛：肥胖相关的过度活动性膀胱炎的原因是未反应的蛋白反应依赖性胰岛素抵抗

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We aimed to investigate the role of insulin in the bladder and its relevance for the development of overactive bladder (OAB) in insulin-resistant obese mice. Bladders from male individuals who were involved in multiple organ donations were used. C57BL6/J mice were fed with a high-fat diet for 10 weeks to induce insulin-resistant obesity. Concentration-response curves to insulin were performed in human and mouse isolated mucosa-intact and mucosa-denuded bladders. Cystometric study was performed in terminally anaesthetized mice. Western blot was performed in bladders to detect phosphorylated endothelial NO synthase (eNOS) (Ser1177) and the phosphorylated protein kinase AKT (Ser473), as well as the unfolded protein response (UPR) markers TRIB3, CHOP and ATF4. Insulin (1-100 nm) produced concentration-dependent mouse and human bladder relaxations that were markedly reduced by mucosal removal or inhibition of the PI3K/AKT/eNOS pathway. In mouse bladders, insulin produced a 3.0-fold increase in cGMP levels (P < 0.05) that was prevented by PI3K/AKT/eNOS pathway inhibition. Phosphoinositide 3-kinase (PI3K) inhibition abolished insulin-induced phosphorylation of AKT and eNOS in bladder mucosa. Obese mice showed greater voiding frequency and non-voiding contractions, indicating overactive detrusor smooth muscle. Insulin failed to relax the bladder or to increase cGMP in the obese group. Insulin-stimulated AKT and eNOS phosphorylation in mucosa was also impaired in obese mice. The UPR markers TRIB3, CHOP and ATF4 were increased in the mucosa of obese mice. The UPR inhibitor 4-phenyl butyric acid normalized all the functional and molecular parameters in obese mice. Our data show that insulin relaxes human and mouse bladder via activation of the PI3K/AKT/eNOS pathway in the bladder mucosa. Endoplasmic reticulum stress-dependent insulin resistance in bladder contributes to OAB in obese mice.

机译：我们旨在调查胰岛素在膀胱中的作用及其与胰岛素抵抗性肥胖小鼠过度活动性膀胱（OAB）的发展相关性。使用来自参与多个器官捐赠的男性个体的膀胱。给C57BL6 / J小鼠喂食高脂饮食10周，以诱导胰岛素抵抗性肥胖症。在人和小鼠分离的完整粘膜和裸露粘膜的膀胱中绘制了对胰岛素的浓度-响应曲线。在最终麻醉的小鼠中进行了膀胱测量。在膀胱中进行蛋白质印迹，以检测磷酸化的内皮一氧化氮合酶（eNOS）（Ser1177）和磷酸化的蛋白激酶AKT（Ser473），以及未折叠的蛋白应答（UPR）标记TRIB3，CHOP和ATF4。胰岛素（1-100 nm）产生浓度依赖性的小鼠和人膀胱松弛，其通过粘膜去除或抑制PI3K / AKT / eNOS途径而明显减少。在小鼠膀胱中，胰岛素产生的cGMP水平增加了3.0倍（P <0.05），这可以通过PI3K / AKT / eNOS途径抑制来阻止。磷酸肌醇3激酶（PI3K）的抑制作用消除了胰岛素诱导的膀胱粘膜中AKT和eNOS的磷酸化。肥胖小鼠表现出更大的排尿频率和无孔收缩，表明逼尿肌平滑肌过度活跃。肥胖组胰岛素未能使膀胱松弛或增加cGMP。肥胖小鼠的胰岛素刺激粘膜中的AKT和eNOS磷酸化也受损。 UPR标记TRIB3，CHOP和ATF4在肥胖小鼠的粘膜中增加。 UPR抑制剂4-苯基丁酸可以使肥胖小鼠的所有功能和分子参数正常化。我们的数据表明，胰岛素通过激活膀胱粘膜中的PI3K / AKT / eNOS途径使人和小鼠的膀胱放松。膀胱内质网应激依赖的胰岛素抵抗导致肥胖小鼠的OAB。

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《The Journal of Physiology》 |2013年第9期|共15页
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LeiriaL.O.; SollonC.; BáuF.R.; MónicaF.Z.; DAnconaC.L.; DeNucciG.; GrantA.D.; AnhêG.F.; AntunesE.;
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正文语种 eng
中图分类人体生理学;
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1. Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa: Unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder [J] . LeiriaL.O., SollonC., BáuF.R., The Journal of Physiology . 2013,第9期

机译：胰岛素通过PI3K / AKT / eNOS途径激活粘膜使膀胱松弛：肥胖相关的过度活动性膀胱炎的原因是未反应的蛋白反应依赖性胰岛素抵抗
2. 1-Deoxynojirimycin Alleviates Insulin Resistance via Activation of Insulin Signaling PI3K/AKT Pathway in Skeletal Muscle of db/db Mice [J] . Cunyu Li, Derek J. McPhee, Guoping Peng, Molecules . 2015,第12期

机译：1-脱氧野rim霉素通过激活db / db小鼠骨骼肌中的胰岛素信号PI3K / AKT途径减轻胰岛素抵抗。
3. Activation of Vascular Protein Kinase C-{beta} Inhibits Akt-Dependent Endothelial Nitric Oxide Synthase Function in Obesity-Associated Insulin Resistance. [J] . Naruse K, Rask Madsen C, Takahara N, Diabetes . 2006,第3期

机译：血管蛋白激酶C-β的激活抑制了肥胖相关胰岛素抵抗中依赖Akt的内皮一氧化氮合酶功能。
4. THE E3 UBIQUITIN LIGASE CBL-B REVERSES MULTIDRUG RESISTANCE OF MCF-7/ADR CELLS THROUGH SUPPRESSION OF PI3K/AKT SIGNALING PATHWAY AND DOWN-REGULATION OF P-GLYCOPROTEIN [C] . Ye Zhang, Xiujuan Qu, Xuejun Hu, 2011 Asia-Pacific Conference of tumor biology and medicine . 2011

机译：E3泛素连接酶CBL-B通过抑制PI3K / AKT信号通路和P-糖蛋白下调逆转MCF-7 / ADR细胞的多药耐药性
5. Potential role of endoplasmic reticulum redox changes in endoplasmic reticulum stress and impaired protein folding in obesity-associated insulin resistance [D] . Sarkar, Deboleena 2013

机译：内质网氧化还原变化在内质网应激和蛋白质折叠受损在肥胖相关胰岛素抵抗中的潜在作用
6. Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa: unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder [O] . Luiz O Leiria, Carolina Sollon, Fernando R Báu, 2013

机译：胰岛素通过PI3K / AKT / eNOS途径激活粘膜使膀胱松弛：肥胖相关的过度活动性膀胱炎的原因是未反应的蛋白反应依赖性胰岛素抵抗
7. Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa:Unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder [O] . Leiria, Luiz O., Sollon, Carolina, Báu, Fernando R., 2013

机译：胰岛素通过粘膜中的PI3K / AKT / eNOS途径激活使膀胱松弛：未表达的蛋白质反应依赖性胰岛素抵抗是肥胖相关的膀胱过度活动的原因

Insulin relaxes bladder via PI3K/AKT/eNOS pathway activation in mucosa: Unfolded protein response-dependent insulin resistance as a cause of obesity-associated overactive bladder

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