A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells

Focal segmental glomerulosclerosis is a major cause of end stage renal disease. Many patients prove unresponsive to available therapies. An improved understanding of the molecular basis of the disease process could provide insights leading to novel therapeutic approaches. In this study we carried ou...

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Autores principales: Potter, Andrew S., Drake, Keri, Brunskill, Eric W., Potter, S. Steven
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6713350/
https://www.ncbi.nlm.nih.gov/pubmed/31461442
http://dx.doi.org/10.1371/journal.pone.0216261
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author Potter, Andrew S.
Drake, Keri
Brunskill, Eric W.
Potter, S. Steven
author_facet Potter, Andrew S.
Drake, Keri
Brunskill, Eric W.
Potter, S. Steven
author_sort Potter, Andrew S.
collection PubMed
description Focal segmental glomerulosclerosis is a major cause of end stage renal disease. Many patients prove unresponsive to available therapies. An improved understanding of the molecular basis of the disease process could provide insights leading to novel therapeutic approaches. In this study we carried out an RNA-seq analysis of the altered gene expression patterns of podocytes, mesangial cells and glomerular endothelial cells of the bigenic Cd2ap+/-, Fyn-/- mutant mouse model of FSGS. In the podocytes we observed upregulation of many genes related to the Tgfβ family/pathway, including Gdnf, Tgfβ1, Tgfβ2, Snai2, Vegfb, Bmp4, and Tnc. The mutant podocytes also showed upregulation of Acta2, a marker of smooth muscle and associated with myofibroblasts, which are implicated in driving fibrosis. GO analysis of the podocyte upregulated genes identified elevated protein kinase activity, increased expression of growth factors, and negative regulation of cell adhesion, perhaps related to the observed podocyte loss. Both podocytes and mesangial cells showed strong upregulation of aldehyde dehydrogenase genes involved in the synthesis of retinoic acid. Similarly, the Cd2ap+/-, Fyn-/- mesangial cells, as well as podocytes in other genetic models, and the glomeruli of human FSGS patients, all show upregulation of the serine protease Prss23, with the common thread suggesting important functionality. Another gene with strong upregulation in the Cd2ap+/-, Fyn-/- mutant mesangial cells as well as multiple other mutant mouse models of FSGS was thrombospondin, which activates the secreted inactive form of Tgfβ. The Cd2ap+/-, Fyn-/- mutant endothelial cells showed elevated expression of genes involved in cell proliferation, angioblast migration, angiogenesis, and neovasculature, all consistent with the formation of new blood vessels in the diseased glomerulus. The resulting global definition of the perturbed molecular pathways in the three major cell types of the mutant glomerulus provide deeper understanding of the molecular pathogenic pathways.
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spelling pubmed-67133502019-09-04 A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells Potter, Andrew S. Drake, Keri Brunskill, Eric W. Potter, S. Steven PLoS One Research Article Focal segmental glomerulosclerosis is a major cause of end stage renal disease. Many patients prove unresponsive to available therapies. An improved understanding of the molecular basis of the disease process could provide insights leading to novel therapeutic approaches. In this study we carried out an RNA-seq analysis of the altered gene expression patterns of podocytes, mesangial cells and glomerular endothelial cells of the bigenic Cd2ap+/-, Fyn-/- mutant mouse model of FSGS. In the podocytes we observed upregulation of many genes related to the Tgfβ family/pathway, including Gdnf, Tgfβ1, Tgfβ2, Snai2, Vegfb, Bmp4, and Tnc. The mutant podocytes also showed upregulation of Acta2, a marker of smooth muscle and associated with myofibroblasts, which are implicated in driving fibrosis. GO analysis of the podocyte upregulated genes identified elevated protein kinase activity, increased expression of growth factors, and negative regulation of cell adhesion, perhaps related to the observed podocyte loss. Both podocytes and mesangial cells showed strong upregulation of aldehyde dehydrogenase genes involved in the synthesis of retinoic acid. Similarly, the Cd2ap+/-, Fyn-/- mesangial cells, as well as podocytes in other genetic models, and the glomeruli of human FSGS patients, all show upregulation of the serine protease Prss23, with the common thread suggesting important functionality. Another gene with strong upregulation in the Cd2ap+/-, Fyn-/- mutant mesangial cells as well as multiple other mutant mouse models of FSGS was thrombospondin, which activates the secreted inactive form of Tgfβ. The Cd2ap+/-, Fyn-/- mutant endothelial cells showed elevated expression of genes involved in cell proliferation, angioblast migration, angiogenesis, and neovasculature, all consistent with the formation of new blood vessels in the diseased glomerulus. The resulting global definition of the perturbed molecular pathways in the three major cell types of the mutant glomerulus provide deeper understanding of the molecular pathogenic pathways. Public Library of Science 2019-08-28 /pmc/articles/PMC6713350/ /pubmed/31461442 http://dx.doi.org/10.1371/journal.pone.0216261 Text en © 2019 Potter et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Potter, Andrew S.
Drake, Keri
Brunskill, Eric W.
Potter, S. Steven
A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
title A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
title_full A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
title_fullStr A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
title_full_unstemmed A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
title_short A bigenic mouse model of FSGS reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
title_sort bigenic mouse model of fsgs reveals perturbed pathways in podocytes, mesangial cells and endothelial cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6713350/
https://www.ncbi.nlm.nih.gov/pubmed/31461442
http://dx.doi.org/10.1371/journal.pone.0216261
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