Reduced nephrin tyrosine phosphorylation impairs podocyte force transmission and accelerates detachment in disease

Casey Williamson; Claire Martin; Jothi Dinesh Kumar; Peihua Lu; Laura A. New; Alice Y. Wang; Nils Michael Kronenberg; Malte Christian Gather; Paul Andrew Reynolds; Nina Jones

doi:10.1016/j.isci.2025.112673

Reduced nephrin tyrosine phosphorylation impairs podocyte force transmission and accelerates detachment in disease

Casey Williamson, Claire Martin, Jothi Dinesh Kumar, Peihua Lu, Laura A. New, Alice Y. Wang, Nils Michael Kronenberg, Malte Christian Gather, Paul Andrew Reynolds, Nina Jones^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

Abstract

Podocytes are specialized kidney cells that form the slit diaphragm (SD), an intercellular filtration barrier against plasma protein loss. The SD is subject to significant mechanical strain which can be amplified in disease, leading to podocyte detachment. One key SD protein that might intercept mechanical strain and transmit adhesion signals is nephrin, although its influence on podocyte force transmission remains uncharacterized. Using immunoblotting and elastic resonator interference stress microscopy (ERISM), we demonstrate that nephrin clustering induces rapid podocyte force transmission and adhesion protein activation (paxillin, FAK, and p130Cas), which require nephrin tyrosine phosphorylation at its three YDxV motifs. Furthermore, using a model of diabetic nephropathy to amplify mechanical stress in vivo, we show that abolishing phosphorylation at YDxV tyrosines leads to exacerbated proteinuria, glomerular hypertrophy, and podocyte detachment. Altogether, this study links nephrin phosphorylation with force transmission, which is likely critical to maintaining podocyte adhesion during many renal pathologies.

Original language	English
Article number	112673
Pages (from-to)	1-19
Number of pages	19
Journal	iScience
Volume	28
Issue number	6
Early online date	14 May 2025
DOIs	https://doi.org/10.1016/j.isci.2025.112673
Publication status	Published - 20 Jun 2025

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10.1016/j.isci.2025.112673Licence: CC BY

Williamson-2025-Reduced-nephrin-tyrosine-iScience-28-112673-CCBY
Copyright © 2025 The Authors. Published by Elsevier Inc. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
Final published version, 8.71 MBLicence: CC BY

Resonant and shaped photonics for under: Resonant and shaped photonics for understanding the physical and biomedical world
Dholakia, K. (PI) & Gather, M. C. (CoI)
1/08/17 → 31/07/22
Project: Standard
iTFM: Interference Traction Force Microscopy (iTFM) for Bioimaging of Cellular Forces
Reynolds, P. A. (PI)
BBSRC
1/08/17 → 31/10/18
Project: Standard
Interference Traction Force Microscopy: Interference Traction Force Microscopy (iTFM) for Bioimaging of Cellular Forces
Gather, M. C. (PI)
BBSRC
1/07/17 → 30/09/18
Project: Standard

Cite this

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title = "Reduced nephrin tyrosine phosphorylation impairs podocyte force transmission and accelerates detachment in disease",

abstract = "Podocytes are specialized kidney cells that form the slit diaphragm (SD), an intercellular filtration barrier against plasma protein loss. The SD is subject to significant mechanical strain which can be amplified in disease, leading to podocyte detachment. One key SD protein that might intercept mechanical strain and transmit adhesion signals is nephrin, although its influence on podocyte force transmission remains uncharacterized. Using immunoblotting and elastic resonator interference stress microscopy (ERISM), we demonstrate that nephrin clustering induces rapid podocyte force transmission and adhesion protein activation (paxillin, FAK, and p130Cas), which require nephrin tyrosine phosphorylation at its three YDxV motifs. Furthermore, using a model of diabetic nephropathy to amplify mechanical stress in vivo, we show that abolishing phosphorylation at YDxV tyrosines leads to exacerbated proteinuria, glomerular hypertrophy, and podocyte detachment. Altogether, this study links nephrin phosphorylation with force transmission, which is likely critical to maintaining podocyte adhesion during many renal pathologies.",

author = "Casey Williamson and Claire Martin and Kumar, {Jothi Dinesh} and Peihua Lu and New, {Laura A.} and Wang, {Alice Y.} and Kronenberg, {Nils Michael} and Gather, {Malte Christian} and Reynolds, {Paul Andrew} and Nina Jones",

note = "Funding: This work was supported by the Canadian Institutes of Health Research (PJT-148731 to N.J.), Kidney Foundation of Canada (KFOC190002; to N.J.), the Canada Research Chairs Program (to N.J.), the Biotechnology and Biological Sciences Research Council (BB/P027148/1; to M.C.G and P.R.) and the Engineering and Physical Science Research Council (EP/P030017/1; to M.C.G.). Support to C.R.W. was provided by the National Sciences and Engineering Research Council of Canada Postgraduate Scholarship – Doctoral (NSERC PGS D) and a Graduate Entrance Excellence Scholarship from the University of Guelph College of Biological Sciences.",

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AU - Williamson, Casey

AU - Martin, Claire

AU - Kumar, Jothi Dinesh

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AU - New, Laura A.

AU - Wang, Alice Y.

AU - Kronenberg, Nils Michael

AU - Gather, Malte Christian

AU - Reynolds, Paul Andrew

AU - Jones, Nina

N1 - Funding: This work was supported by the Canadian Institutes of Health Research (PJT-148731 to N.J.), Kidney Foundation of Canada (KFOC190002; to N.J.), the Canada Research Chairs Program (to N.J.), the Biotechnology and Biological Sciences Research Council (BB/P027148/1; to M.C.G and P.R.) and the Engineering and Physical Science Research Council (EP/P030017/1; to M.C.G.). Support to C.R.W. was provided by the National Sciences and Engineering Research Council of Canada Postgraduate Scholarship – Doctoral (NSERC PGS D) and a Graduate Entrance Excellence Scholarship from the University of Guelph College of Biological Sciences.

PY - 2025/6/20

Y1 - 2025/6/20

N2 - Podocytes are specialized kidney cells that form the slit diaphragm (SD), an intercellular filtration barrier against plasma protein loss. The SD is subject to significant mechanical strain which can be amplified in disease, leading to podocyte detachment. One key SD protein that might intercept mechanical strain and transmit adhesion signals is nephrin, although its influence on podocyte force transmission remains uncharacterized. Using immunoblotting and elastic resonator interference stress microscopy (ERISM), we demonstrate that nephrin clustering induces rapid podocyte force transmission and adhesion protein activation (paxillin, FAK, and p130Cas), which require nephrin tyrosine phosphorylation at its three YDxV motifs. Furthermore, using a model of diabetic nephropathy to amplify mechanical stress in vivo, we show that abolishing phosphorylation at YDxV tyrosines leads to exacerbated proteinuria, glomerular hypertrophy, and podocyte detachment. Altogether, this study links nephrin phosphorylation with force transmission, which is likely critical to maintaining podocyte adhesion during many renal pathologies.

AB - Podocytes are specialized kidney cells that form the slit diaphragm (SD), an intercellular filtration barrier against plasma protein loss. The SD is subject to significant mechanical strain which can be amplified in disease, leading to podocyte detachment. One key SD protein that might intercept mechanical strain and transmit adhesion signals is nephrin, although its influence on podocyte force transmission remains uncharacterized. Using immunoblotting and elastic resonator interference stress microscopy (ERISM), we demonstrate that nephrin clustering induces rapid podocyte force transmission and adhesion protein activation (paxillin, FAK, and p130Cas), which require nephrin tyrosine phosphorylation at its three YDxV motifs. Furthermore, using a model of diabetic nephropathy to amplify mechanical stress in vivo, we show that abolishing phosphorylation at YDxV tyrosines leads to exacerbated proteinuria, glomerular hypertrophy, and podocyte detachment. Altogether, this study links nephrin phosphorylation with force transmission, which is likely critical to maintaining podocyte adhesion during many renal pathologies.

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DO - 10.1016/j.isci.2025.112673

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Reduced nephrin tyrosine phosphorylation impairs podocyte force transmission and accelerates detachment in disease

Abstract

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Projects

Resonant and shaped photonics for under: Resonant and shaped photonics for understanding the physical and biomedical world

iTFM: Interference Traction Force Microscopy (iTFM) for Bioimaging of Cellular Forces

Interference Traction Force Microscopy: Interference Traction Force Microscopy (iTFM) for Bioimaging of Cellular Forces

Cite this