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用于鉴定肾保护化合物的人足细胞损伤慢性肾脏病模型的建立。

Implementation of a human podocyte injury model of chronic kidney disease for profiling of renoprotective compounds.

机构信息

Renal Discovery, Global Pharmaceutical Research and Development, AbbVie, 1 North Waukegan Road, North Chicago, IL 60064, USA.

Renal Discovery, Global Pharmaceutical Research and Development, AbbVie, 1 North Waukegan Road, North Chicago, IL 60064, USA.

出版信息

Eur J Pharmacol. 2017 Nov 15;815:219-232. doi: 10.1016/j.ejphar.2017.09.006. Epub 2017 Sep 9.

Abstract

Degradation of podocyte structural integrity and function are hallmarks of proteinuric chronic kidney disease. In vivo, injury of podocytes manifests itself in the form of disruption of foot process morphology and associated cytoskeletal architecture, de-differentiation, and loss of adhesion to the glomerular basement membrane. Given the critical role played by this highly specialized cell type in maintaining glomerular filtration, there is a need for improved physiologically relevant cellular models that enable detection of disease-relevant indicators of podocyte perturbation. We have addressed this need by evaluating a subclone of conditionally immortalized human podocytes through quantitative benchmarking against freshly isolated primary human podocytes. Benchmarking was performed by measuring key phenotypic parameters, expression of podocyte specific proteins and multiparametric responses to stressors that model different aspects of podocyte perturbation. We subsequently employed the subcloned cells to profile the protective activity of structurally distinct adenosine kinase inhibitors. Our results support the translatability of our cellular model and set the stage for broader screening of renoprotective compounds with a view to eventually treat proteinuric kidney disease.

摘要

足细胞结构完整性和功能的降解是蛋白尿性慢性肾脏病的标志。在体内,足细胞的损伤表现为足突形态的破坏和相关细胞骨架结构的去分化,以及与肾小球基底膜的黏附丧失。鉴于这种高度特化的细胞类型在维持肾小球滤过方面的关键作用,需要改进与生理相关的细胞模型,以检测足细胞扰动的相关疾病指标。我们通过对条件永生化的人足细胞亚克隆进行定量基准测试,与新鲜分离的原代人足细胞进行比较,从而满足了这一需求。基准测试通过测量关键表型参数、足细胞特异性蛋白的表达以及模拟足细胞扰动不同方面的应激多参数反应来进行。随后,我们使用亚克隆细胞来分析结构不同的腺苷激酶抑制剂的保护活性。我们的结果支持我们的细胞模型的可转化性,并为更广泛的筛选具有肾脏保护作用的化合物奠定了基础,以期最终治疗蛋白尿性肾病。

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