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依普利酮对单侧输尿管梗阻大鼠对侧肾脏细胞增殖的抑制作用。

The Inhibitory Effect of Eplerenone on Cell Proliferation in the Contralateral Kidneys of Rats with Unilateral Ureteral Obstruction.

作者信息

Wang Cong-Hui, Wang Zheng, Liang Li-Juan, Wang Xiang-Ting, Ma Xue-Lian, Liu Bei-Bei, He Jia-Qi, Shimosawa Tatsuo, Xu Qing-You

机构信息

Graduate School, Hebei Medical University, Shijiazhang, China.

出版信息

Nephron. 2017;136(4):328-338. doi: 10.1159/000473702. Epub 2017 Apr 13.

Abstract

BACKGROUND

The unilateral ureteral obstruction (UUO) model not only induces renal interstitial fibrosis in the obstructed kidney but also induces injury in the contralateral kidney. We hypothesized that activation of the mineralocorticoid receptor (MR) may induce fibrosis in the early stage of UUO.

METHODS

Thirty male Sprague-Dawley rats weighting 200 ± 10 g were used in this study and randomly divided into 3 groups: a UUO group, a UUO and eplerenone group, and a sham group. The contralateral kidney and plasma were harvested for further study 10 days after surgery.

RESULTS

The level of plasma aldosterone (869.95 ± 55.851 pg/mL) was significantly higher in the UUO group than that in the sham group (478.581 ± 36.186 pg/mL vs. UUO, p < 0.05). The infiltrated inflammatory cells (F4/80) and deposited collagens were increased significantly in the contralateral kidneys in the UUO group compared to those in the sham group, which were decreased by eplerenone. However, proliferating cell nuclear antigen was increased 2.47 times in the UUO group compared to the sham group in the contralateral kidney (p < 0.01), and those changes are attenuated by eplerenone. The expression of SGK-1 protein and mRNA was upregulated in the contralateral kidney in the UUO group, which is suppressed by eplerenone treatment. NF-κB pathway effecters were also changed markedly in the contralateral kidney in the UUO group and partly reversed by eplerenone.

CONCLUSION

Aldosterone induces inflammatory cell proliferation via the MR/SGK-1 and NF-κB pathways and eventually leads to fibrosis in the contralateral kidney.

摘要

背景

单侧输尿管梗阻(UUO)模型不仅会在梗阻侧肾脏诱发肾间质纤维化,还会导致对侧肾脏损伤。我们推测盐皮质激素受体(MR)的激活可能在UUO早期诱发纤维化。

方法

本研究使用30只体重200±10 g的雄性Sprague-Dawley大鼠,随机分为3组:UUO组、UUO加依普利酮组和假手术组。术后10天采集对侧肾脏和血浆用于进一步研究。

结果

UUO组血浆醛固酮水平(869.95±55.851 pg/mL)显著高于假手术组(478.581±36.186 pg/mL,与UUO组相比,p<0.05)。与假手术组相比,UUO组对侧肾脏中浸润的炎性细胞(F4/80)和沉积的胶原蛋白显著增加,依普利酮可使其减少。然而,与假手术组相比,UUO组对侧肾脏中增殖细胞核抗原增加了2.47倍(p<0.01),依普利酮可减弱这些变化。UUO组对侧肾脏中SGK-1蛋白和mRNA的表达上调,依普利酮治疗可抑制这种上调。UUO组对侧肾脏中NF-κB信号通路效应分子也发生了明显变化,依普利酮可部分逆转这些变化。

结论

醛固酮通过MR/SGK-1和NF-κB信号通路诱导炎性细胞增殖,最终导致对侧肾脏纤维化。

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