uPAR isoform 2 forms a dimer and induces severe kidney disease in mice

uPAR 亚型 2 形成二聚体,并在小鼠中诱发严重的肾脏疾病。

阅读:4
作者:Changli Wei ,Jing Li ,Brian D Adair ,Ke Zhu ,Jian Cai ,Michael Merchant ,Beata Samelko ,Zhongji Liao ,Kwi Hye Koh ,Nicholas J Tardi ,Ranadheer R Dande ,Shuangxin Liu ,Jianchao Ma ,Salvatore Dibartolo ,Stefan Hägele ,Vasil Peev ,Salim S Hayek ,David J Cimbaluk ,Melissa Tracy ,Jon Klein ,Sanja Sever ,Sanford J Shattil ,M Amin Arnaout ,Jochen Reiser
期刊:Journal of Clinical Investigation影响因子:13.300
时间:2019起止号:2019 Apr 2;129(5):1946-1959.
doi:10.1172/JCI124793种属: Mouse
研究方向: 信号转导

Abstract

Soluble urokinase plasminogen activator receptor (suPAR) is an immune-derived circulating signaling molecule that has been implicated in chronic kidney disease, such as focal segmental glomerulosclerosis (FSGS). Typically, native uPAR (isoform 1) translates to a 3-domain protein capable of binding and activating integrins, yet the function of additional isoforms generated by alternative splicing is unknown. Here, we characterized mouse uPAR isoform 2 (msuPAR2), encoding domain I and nearly one-half of domain II, as a dimer in solution, as revealed by 3D electron microscopy structural analysis. In vivo, msuPAR2 transgenic mice exhibited signs of severe renal disease characteristic of FSGS with proteinuria, loss of kidney function, and glomerulosclerosis. Sequencing of the glomerular RNAs from msuPAR2-Tg mice revealed a differentially expressed gene signature that includes upregulation of the suPAR receptor Itgb3, encoding β3 integrin. Crossing msuPAR2-transgenic mice with 3 different integrin β3 deficiency models rescued msuPAR2-mediated kidney function. Further analyses indicated a central role for β3 integrin and c-Src in msuPAR2 signaling and in human FSGS kidney biopsies. Administration of Src inhibitors reduced proteinuria in msuPAR2-transgenic mice. In conclusion, msuPAR2 may play an important role in certain forms of scarring kidney disease. Keywords: Chronic kidney disease; Integrins; Nephrology; Protein kinases.

特别声明

1、本页面内容包含部分的内容是基于公开信息的合理引用;引用内容仅为补充信息,不代表本站立场。

2、若认为本页面引用内容涉及侵权,请及时与本站联系,我们将第一时间处理。

3、其他媒体/个人如需使用本页面原创内容,需注明“来源:[生知库]”并获得授权;使用引用内容的,需自行联系原作者获得许可。

4、投稿及合作请联系:info@biocloudy.com。