MiR-200a ameliorates peritoneal fibrosis and functional deterioration in a rat model of peritoneal dialysis

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作者
Xin Wei
Yi Bao
Xiaojiang Zhan
Li Zhang
Guojun Hao
Jing Zhou
Qinkai Chen
机构
[1] The First Affiliated Hospital of Nanchang University,Department of Nephrology
[2] The First Affiliated Hospital of Guizhou Medical University,Department of Nephrology
[3] Zhongshan City People’s Hospital,Department of Nephrology
[4] Zhongshan Hospital of Sun Yat-sen University,undefined
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Peritoneal dialysis; Peritoneal fibrosis; MiR-200a; Zeb1/2;
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摘要
Peritoneal fibrosis is recognised as the main cause of the technical failure of peritoneal dialysis (PD), and currently, there are no specific and effective anti-fibrosis therapies. We have found that miR-200a is down-regulated in a rat model of PD-related peritoneal fibrosis (PF) and could inhibit transforming growth factor beta 1 (TGF-β1)-induced epithelial-mesenchymal transition (EMT) in peritoneal mesothelial cells by target ZEB1/2. However, its treatment role in vivo is still largely unclear. In this study, we examined the therapeutic potential for miR-200a on PD-related PF in a rat model of PD induced by daily infusion of 4.25% dextrose-containing dialysate. Male Sprague–Dawley rats were divided into four groups: control group, PD group, PD + miR-agomir-NC group, and PD + miR-200a-agomir group (n = 5 in each group). MiR-200a agomir was delivered into the peritoneum by intra-peritoneal injection on days 10 and 20 after PD. We found that treatment with miR-200a agomir significantly reduced the collagen volume fraction (CVF) of the peritoneum and prevented peritoneal dysfunction. The up-regulation of the EMT marker (decreased E-cadherin and increased α-smooth muscle actin) and extracellular matrix (fibronectin and collagen I) was significantly ameliorated by miR-200a in the PD + miR-200a-agomir group. Furthermore, we demonstrated that miR-200a inhibition of PF in vivo was associated with the suppression of ZEB1 and 2, which were proved to be the target of miR-200a in our previous study. In conclusion, results from the present study suggest that treatment with miR-200a may represent a novel and effective therapy for PD-related PF.
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页码:889 / 896
页数:7
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