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Bone marrow stem cells-derived microvesicles protect against renal injury in the mouse remnant kidney model

机译:源自骨髓干细胞的微泡可在小鼠残余肾脏模型中预防肾脏损伤

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Aims: Several studies have demonstrated administration of mesenchymal stem cells (MSC) could reverse kidney injury by paracrine mechanisms rather than by MSC transdifferentiation. Recently, a few researchers found microvesicles (MV) derived from MSC might be a paracrine mechanism for cell-to-cell communication. The aim of this study was to investigate the repair effects of MV in a 5/6 subtotal nephrectomy (Nx) mice model. Methods: The animals were randomly divided into four groups: Control, Nx, Nx + MSC and Nx + MV group. MSC were injected (1 × 10 6/mouse) through caudal vein in Nx + MSC group at the second day after the surgery and MV were injected (30 μg/mouse) through caudal vein in Nx + MV group on alternate days. Mice were killed on day 7 after the first time of administration. Blood urea nitrogen (BUN), serum creatinine (Scr), uric acid (UA) and proteinuria were evaluated. Histopathology of kidney was analysed. Results: In Nx mice, the levels of Scr, UA and proteinuria were significantly decreased with administration of MV and MSC (P 0.05). The remnant kidneys of MV and MSC-treated Nx mice showed less fibrosis, interstitial lymphocyte infiltrates and less or absent tubular atrophy compared with the untreated Nx group. The Histological Score of Kidney in untreated mice was 3.13 ± 0.74, while in the MSC-treated group it was 1.67 ± 0.47 and in the MV-treated group it was 1.80 ± 0.44, nearly preserving normal morphology of the kidney (P 0.01). Conclusion: This study showed MV protects against renal injury induced by 5/6 Nx, which could mimic the role of MSC in kidney repair. The research showed a newly potential therapeutic approach to kidney diseases.
机译:目的:多项研究表明,间充质干细胞(MSC)的使用可以通过旁分泌机制而不是通过MSC转分化来逆转肾脏损伤。最近,一些研究人员发现,源自MSC的微泡(MV)可能是细胞间通信的旁分泌机制。这项研究的目的是调查MV在5/6次全肾切除术(Nx)小鼠模型中的修复作用。方法:将动物随机分为四组:对照组,Nx,Nx + MSC和Nx + MV组。术后第二天,Nx + MSC组通过尾静脉注射MSC(1×10 6 /只),隔日隔Nx + MV组通过尾静脉注射MV(30μg/只)。第一次给药后第7天杀死小鼠。评估血尿素氮(BUN),血清肌酐(Scr),尿酸(UA)和蛋白尿。分析了肾脏的组织病理学。结果:在Nx小鼠中,MV和MSC的使用显着降低了Scr,UA和蛋白尿的水平(P <0.05)。与未治疗的Nx组相比,MV和MSC治疗的Nx小鼠的残余肾脏显示较少的纤维化,间质淋巴细胞浸润以及较少或没有肾小管萎缩。未治疗小鼠的肾脏组织学评分为3.13±0.74,而MSC治疗组为1.67±0.47,MV治疗组为1.80±0.44,几乎保持了肾脏的正常形态(P <0.01) 。结论:这项研究表明,MV可预防5/6 Nx引起的肾脏损伤,这可以模仿MSC在肾脏修复中的作用。研究表明,一种新的潜在治疗肾脏疾病的方法。

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