uPAR isoform 2 forms a dimer and induces severe kidney disease in mice
Changli Wei, … , M. Amin Arnaout, Jochen Reiser
Changli Wei, … , M. Amin Arnaout, Jochen Reiser
Published February 7, 2019
Citation Information: J Clin Invest. 2019;129(5):1946-1959. https://doi.org/10.1172/JCI124793.
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Research Article Nephrology

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

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.

Authors

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

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Figure 5

Glomerular β3 integrin expression is increased in msuPAR2-Tg mice.

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Glomerular β3 integrin expression is increased in msuPAR2-Tg mice. (A) R...
(A) RNA-Seq of msuPAR2-Tg mouse glomeruli. Differentially expressed genes are shown in the heatmap. Red, high transcript levels; blue, low transcript levels. n = 7 suPAR2-Tg mice; n = 3 littermate controls. Red arrow indicates Itgb3. (B) Differentially expressed pathways identified by gene-set enrichment analysis via DAVID. Numbers above the bars represent counts in percentage. (C and D) msuPAR2 induces β3 integrin activity on human podocytes. Cultured human podocytes were treated with purified msuPAR2 or msuPAR1 protein at 1 ng/ml and examined for β3 integrin activation, as indicated by AP5 staining intensity. Activated β3 integrin colocalized with paxillin. Controls received the same amount of BSA. Scale bars: 50 μm. *P < 0.05; **P < 0.01; ****P < 0.0001.