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Phenotypic changes and cell cycle activation in early tubulointerstitial injury of rat adriamycin nephrosis.

机译:大鼠阿霉素肾病早期肾小管间质损伤的表型变化和细胞周期激活。

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Tubular response, including phenotypic changes against a variety of injuries, is an initial event that promotes tubulointerstitial injuries. Using the progressive kidney disease model of rat adriamycin (ADR) nephrosis, the present study focused on the cell cycle activation and phenotypic changes that occur in the tubuli in early tubulointerstitial injury in ADR nephrosis. At 12 weeks, experimental animals developed overt nephrosis with tubulointerstitial injury, which correlated well with the degree of proteinuria and incidence of glomerulosclerosis. Initial pathology of the tubuli showed a slight dilatation of tubuli, which tended to occur in individual nephrons. Immunohistochemistry demonstrated that vimentin-positive tubuli and osteopontin (OPN)-positive tubuli were associated mostly with proliferating cell nuclear antigen expression. Protein levels of OPN in the renal cortex were correlated with the level of proteinuria by western blotting. Vimentin- and OPN-expressing tubuli were tightly associated with a peritubular influx of alpha-smooth muscle actin (SMA)-positive cells or ED-1-positive cells. In addition, we found thrombomodulin+/ TUNEL+ (dUTP-biotin nick-end labeling) peritubular endothelial cells and ED-1+/alpha-SMA+ cells at an early stage among interstitial inflammatory cells. These results suggest that cell cycle activation in tubular cells forms the background for the phenotypic tubular changes that are involved in chronic tubulointerstitial injury in ADR nephrosis.
机译:肾小管反应,包括针对各种损伤的表型改变,是促进肾小管间质损伤的最初事件。使用大鼠阿霉素(ADR)肾病的进行性肾脏疾病模型,本研究集中于ADR肾病早期肾小管间质损伤中肾小管中的细胞周期激活和表型变化。在第12周,实验动物出现明显的肾小管间质损伤,这与蛋白尿程度和肾小球硬化的发生率密切相关。肾小管的初始病理显示肾小管轻微扩张,这往往发生在单个肾单位中。免疫组织化学表明波形蛋白阳性小管和骨桥蛋白(OPN)阳性小管主要与增殖细胞核抗原表达有关。通过蛋白质印迹,肾皮质中OPN的蛋白质水平与蛋白尿水平相关。表达波形蛋白和OPN的肾小管与α平滑肌肌动蛋白(SMA)阳性细胞或ED-1阳性细胞的肾小管周流入紧密相关。此外,我们发现间质性炎症细胞中的血栓调节蛋白+ / TUNEL +(dUTP-生物素缺口末端标记)肾小管内皮细胞和ED-1 + /α-SMA+细胞处于早期。这些结果表明,肾小管细胞的细胞周期激活形成了表型肾小管变化的背景,该表型肾小管变化涉及ADR肾病的慢性肾小管间质损伤。

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