Shp2 Associates with and Enhances Nephrin Tyrosine Phosphorylation and Is Necessary for Foot Process Spreading in Mouse Models of Podocyte Injury

Verma, Rakesh; Venkatareddy, Madhusudan; Kalinowski, Anne; Patel, Sanjeevkumar R.; Salant, David J.; Garg, Puneet

doi:10.1128/mcb.00956-15

Cited by 34 publications

(62 citation statements)

References 68 publications

(119 reference statements)

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“…Functional integrity of the glomerular filter cannot be assessed with the protamine sulfate model of podocyte injury, as the animals are sacrificed following the experiment. SHP-2-deleted mouse podocytes subjected to the nephrotoxic serum demonstrated that proteinuria is reduced in addition to the absence of foot process effacement [25]. Similar observations have been made when focal adhesion regulatory proteins, such as focal adhesion kinase (FAK), Crk, and uPAR, are deleted in the mouse [24,36,37].…”

Section: The Podocyte Effacement Processsupporting

confidence: 62%

“…Both are seen markedly less in FSGS compared with membranous nephropathy and minimal change disease, suggesting that there may be important differences in their signaling processes [24]. Lower levels of phospho-SHP-2 staining were observed in the glomerulus from biopsy samples from FSGS patients compared with those from patients with membranous and minimal change disease [25]. The discrepancy could be explained by a decrease in the number of podocytes in FSGS at the time of biopsy; alternatively, there could be distinct signaling pathways involved in the different proteinuric glomerular diseases.…”

Section: Podocyte: Links To Glomerular Basement Membranementioning

confidence: 92%

“…Efforts to identify a process to downregulate nephrin signaling during podocyte injury have focused on SHP-2, a phosphatase that is found within the cytoplasm, and is known to be associated with phosphorylated nephrin during podocyte development and injury. However, when nephrin and SHP-2 were put together in vitro, they were found to upregulate nephrin phosphorylation rather than decrease it, suggesting a role in the activation of Src kinases [25]. Furthermore, mice models with SHP-2 deleted from the podocytes were protected from injury with protamine sulfate [25].…”

Section: The Podocyte Effacement Processmentioning

confidence: 95%

“…However, when nephrin and SHP-2 were put together in vitro, they were found to upregulate nephrin phosphorylation rather than decrease it, suggesting a role in the activation of Src kinases [25]. Furthermore, mice models with SHP-2 deleted from the podocytes were protected from injury with protamine sulfate [25]. Functional integrity of the glomerular filter cannot be assessed with the protamine sulfate model of podocyte injury, as the animals are sacrificed following the experiment.…”

Section: The Podocyte Effacement Processmentioning

confidence: 99%

“…Nephrin can also become tyrosine phosphorylated in cases of podocyte injury (e.g., protamine sulfate exposure), allowing the podocyte foot processes to remodify their actin structure to some extent [24,25]. While it is known that there is an upregulation of tyrosine phosphorylation in glomerular injury, the identity of the other tyrosine kinases in addition to Src kinases that might be involved remains unclear.…”

Section: The Role Of Nephrin In Actin Dynamicsmentioning

confidence: 99%

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A Review of Podocyte Biology

Garg¹

2018

Am J Nephrol

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209

169

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Background: Podocyte biology is a developing science that promises to help improve understanding of the mechanistic nature of multiple diseases associated with proteinuria. Proteinuria in nephrotic syndrome has been linked to mechanistic dysfunctions in the renal glomerulus involving the function of podocyte epithelial cells, including podocyte foot process effacement. Summary: Developments in imaging technology are improving knowledge of the detailed structure of the human renal glomerulus and cortex. Podocyte foot processes attach themselves to the glomerular capillaries at the glomerular basement membrane (GBM) forming intercellular junctions that form slit diaphragm filtration barriers that help maintain normal renal function. Damage in this area has been implicated in glomerular disease. Injured podocytes undergo effacement whereby they lose their structure and spread out, leading to a reduction in filtration barrier function. Effacement is typically associated with the presence of proteinuria in focal segmental glomerulosclerosis, minimal change disease, and diabetes. It is thought to be due to a breakdown in the actin cytoskeleton of the foot processes, complex contractile apparatuses that allow podocytes to dynamically reorganize according to changes in filtration requirements. The process of podocyte depletion correlates with the development of glomerular sclerosis and chronic kidney disease. Focal adhesion complexes that interact with the underlying GBM bind the podocytes within the glomerular structure and prevent their detachment. Key Messages: Knowledge of glomerular podocyte biology is helping to advance our understanding of the science and mechanics of the glomerular filtering process, opening the way to a variety of new potential applications for clinical targeting.

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Section: The Podocyte Effacement Processsupporting

confidence: 62%

Section: Podocyte: Links To Glomerular Basement Membranementioning

confidence: 92%

Section: The Podocyte Effacement Processmentioning

confidence: 95%

Section: The Podocyte Effacement Processmentioning

confidence: 99%

Section: The Role Of Nephrin In Actin Dynamicsmentioning

confidence: 99%

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A Review of Podocyte Biology

Garg¹

2018

Am J Nephrol

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209

169

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Label‐free quantitative proteomic and phosphoproteomic analyses of renal biopsy tissues in membranous nephropathy

Luo

Meng

et al. 2021

Proteomics Clinical Apps

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Purpose Membranous nephropathy (MN) is a common cause of nephrotic syndrome in adults. However, the underlying mechanisms of its occurrence and development are not completely clear. Thus, it is essential to explore the mechanisms. Experimental design Here, we employed label‐free quantification and liquid chromatography‐tandem mass spectrometry analysis techniques to investigate the proteomic and phosphoproteomic alterations in renal biopsy tissues of MN patients. Samples were collected from 16 MN patients and 10 controls. Immunohistochemistry (IHC) was performed to validate the hub phosphoprotein. Results We focused on the changes in the phosphoproteome in MN group versus control group (CG). Totally, 1704 phosphoproteins containing 3241 phosphosites were identified and quantified. The phosphorylation levels of 216 phosphoproteins containing 297 phosphosites were differentially regulated in stage II MN group versus CG, and 333 phosphoproteins containing 461 phosphosites were differentially phosphorylated in stage III MN group versus CG. In each comparison, several differential phosphoproteins were factors, kinases and receptors involved in cellular processes, biological regulation and other biological processes. The subcellular location of most of the differential phosphoproteins was the nucleus. Protein–protein interaction analysis showed that the connections among the differential phosphoproteins were extremely complex, and several signalling pathways probably associated with MN were identified. The hub phosphoprotein was validated by IHC. Conclusions and clinical relevance This investigation can provide direct insight into the global phosphorylation events in MN group versus CG and may help to shed light on the potential pathogenic mechanisms of MN.

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Regulation of Nephrin Phosphorylation in Diabetes and Chronic Kidney Injury

Denhez

Geraldes

2017

Advances in Experimental Medicine and Biology

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Diabetes is the leading cause of microalbuminuria and end-stage renal failure in industrial countries. Disruption of the filtration barrier, seen in almost all nephrotic diseases and diabetes, is the result of the loss or effacement of the podocyte foot process, notably damage of proteins within the slit diaphragm such as nephrin. For many years, nephrin has been viewed as a structural component of the slit diaphragm. It is now well recognized that nephrin contains several tyrosine residues in its cytoplasmic domain, which influences the development of glomerular injury. In this review, we propose an overview of nephrin signaling pathways in kidney injury.

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Shp2 Associates with and Enhances Nephrin Tyrosine Phosphorylation and Is Necessary for Foot Process Spreading in Mouse Models of Podocyte Injury

Cited by 34 publications

References 68 publications

A Review of Podocyte Biology

A Review of Podocyte Biology

Label‐free quantitative proteomic and phosphoproteomic analyses of renal biopsy tissues in membranous nephropathy

Regulation of Nephrin Phosphorylation in Diabetes and Chronic Kidney Injury

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