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A novel in vivo method to quantify slit diaphragm protein abundance in murine proteinuric kidney disease

机译:一种定量在鼠蛋白尿肾病中裂隙隔膜蛋白丰度的体内新方法

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摘要

Injury of the glomerular filter causes proteinuria by disrupting the sensitive interplay of the glomerular protein network. To date, studies of the expression and trafficking of glomerular proteins have been mostly limited to in vitro or histologic studies. Here, we report a novel in vivo biotinylation assay that allows the quantification of surface expression of glomerular proteins in mice. Kidneys were perfused in situ with biotin before harvest. Afterwards glomeruli were isolated and lyzed. The protein of interest was separated by immunoprecipitation and the amount of surface-expressed protein was quantified by Western blot analysis with streptavidin staining. As proof-of-concept, we examined the presence of nephrin in the slit diaphragm in two well-established murine models of proteinuric kidney disease: nephrotoxic nephritis and adriamycin nephropathy. In proteinuric animals, significantly less nephrin was detected in the slit diaphragm. When proteinuria decreased once again during the course of disease, the amount of surface nephrin returned to the baseline. Our present results suggest that our assay is a valuable tool to study the glomerular filter in proteinuric kidney diseases. Note that the assay is not limited to proteins expressed in the slit diaphragm, and all surface proteins that are accessible to biotin perfusion and immunoprecipitation qualify for this analysis.
机译:肾小球滤膜的损伤通过破坏肾小球蛋白网络的敏感相互作用而引起蛋白尿。迄今为止,肾小​​球蛋白表达和运输的研究主要限于体外或组织学研究。在这里,我们报告了一种新型的体内生物素化测定法,该测定法可以定量小鼠中肾小球蛋白的表面表达。收获前,肾脏用生物素原位灌注。之后,分离肾小球并裂解。通过免疫沉淀分离目的蛋白质,并通过链霉亲和素染色的蛋白质印迹分析定量表面表达的蛋白质的量。作为概念验证,我们在两个公认的蛋白尿性肾脏疾病的小鼠模型中检查了缝隙隔膜中nephrin的存在:肾毒性肾炎和阿霉素肾病。在蛋白尿动物中,在缝隙隔膜中检出的肾素明显减少。当在疾病过程中蛋白尿再次减少时,表面肾素的量恢复到基线。我们目前的结果表明,我们的测定是研究蛋白尿性肾脏疾病中肾小球滤过器的有价值的工具。请注意,该测定法不仅限于在缝隙隔膜中表达的蛋白质,并且所有可进行生物素灌注和免疫沉淀的表面蛋白质均可用于此分析。

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