Glomerular endothelial cell heterogeneity in Alport syndrome

Glomerular endothelial cell heterogeneity in Alport syndrome

Abstract Glomerular endothelial cells (GEC) are a crucial component of the glomerular physiology and their damage contributes to the progression of chronic kidney diseases. How GEC affect the pathology of Alport syndrome (AS) however, is unclear. We characterized GEC from wild type (WT) and col4α5 k...

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Main Authors: Hasmik Soloyan, Matthew Thornton, Valentina Villani, Patrick Khatchadourian, Paolo Cravedi, Andrea Angeletti, Brendan Grubbs, Roger De Filippo, Laura Perin, Sargis Sedrakyan
Format: Article
Language:English
Published: Nature Publishing Group 2020-07-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-020-67588-0
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spelling doaj-a65b9cc1a4f24bcc8215f165c1aea6a82021-07-11T11:22:15ZengNature Publishing GroupScientific Reports2045-23222020-07-0110111810.1038/s41598-020-67588-0Glomerular endothelial cell heterogeneity in Alport syndromeHasmik Soloyan0Matthew Thornton1Valentina Villani2Patrick Khatchadourian3Paolo Cravedi4Andrea Angeletti5Brendan Grubbs6Roger De Filippo7Laura Perin8Sargis Sedrakyan9GOFARR Laboratory for Organ Regenerative Research and Cell Therapeutics in Urology, Division of Urology, The Saban Research Institute, Children’s Hospital Los Angeles, University of Southern CaliforniaMaternal Fetal Medicine Division, University of Southern CaliforniaGOFARR Laboratory for Organ Regenerative Research and Cell Therapeutics in Urology, Division of Urology, The Saban Research Institute, Children’s Hospital Los Angeles, University of Southern CaliforniaGOFARR Laboratory for Organ Regenerative Research and Cell Therapeutics in Urology, Division of Urology, The Saban Research Institute, Children’s Hospital Los Angeles, University of Southern CaliforniaDivision of Nephrology, Department of Medicine, Icahn School of Medicine At Mount SinaiNephrology Dialysis and Renal Transplantation Unit, S. Orsola University HospitalMaternal Fetal Medicine Division, University of Southern CaliforniaGOFARR Laboratory for Organ Regenerative Research and Cell Therapeutics in Urology, Division of Urology, The Saban Research Institute, Children’s Hospital Los Angeles, University of Southern CaliforniaGOFARR Laboratory for Organ Regenerative Research and Cell Therapeutics in Urology, Division of Urology, The Saban Research Institute, Children’s Hospital Los Angeles, University of Southern CaliforniaGOFARR Laboratory for Organ Regenerative Research and Cell Therapeutics in Urology, Division of Urology, The Saban Research Institute, Children’s Hospital Los Angeles, University of Southern CaliforniaAbstract Glomerular endothelial cells (GEC) are a crucial component of the glomerular physiology and their damage contributes to the progression of chronic kidney diseases. How GEC affect the pathology of Alport syndrome (AS) however, is unclear. We characterized GEC from wild type (WT) and col4α5 knockout AS mice, a hereditary disorder characterized by progressive renal failure. We used endothelial-specific Tek-tdTomato reporter mice to isolate GEC by FACS and performed transcriptome analysis on them from WT and AS mice, followed by in vitro functional assays and confocal and intravital imaging studies. Biopsies from patients with chronic kidney disease, including AS were compared with our findings in mice. We identified two subpopulations of GEC (dimtdT and brighttdT) based on the fluorescence intensity of the TektdT signal. In AS mice, the brighttdT cell number increased and presented differential expression of endothelial markers compared to WT. RNA-seq analysis revealed differences in the immune and metabolic signaling pathways. In AS mice, dimtdT and brighttdT cells had different expression profiles of matrix-associated genes (Svep1, Itgβ6), metabolic activity (Apom, Pgc1α) and immune modulation (Apelin, Icam1) compared to WT mice. We confirmed a new pro-inflammatory role of Apelin in AS mice and in cultured human GEC. Gene modulations were identified comparable to the biopsies from patients with AS and focal segmental glomerulosclerosis, possibly indicating that the same mechanisms apply to humans. We report the presence of two GEC subpopulations that differ between AS and healthy mice or humans. This finding paves the way to a better understanding of the pathogenic role of GEC in AS progression and could lead to novel therapeutic targets.https://doi.org/10.1038/s41598-020-67588-0
collection DOAJ
language English
format Article
sources DOAJ
author Hasmik Soloyan
Matthew Thornton
Valentina Villani
Patrick Khatchadourian
Paolo Cravedi
Andrea Angeletti
Brendan Grubbs
Roger De Filippo
Laura Perin
Sargis Sedrakyan
spellingShingle Hasmik Soloyan
Matthew Thornton
Valentina Villani
Patrick Khatchadourian
Paolo Cravedi
Andrea Angeletti
Brendan Grubbs
Roger De Filippo
Laura Perin
Sargis Sedrakyan
Glomerular endothelial cell heterogeneity in Alport syndrome
Scientific Reports
author_facet Hasmik Soloyan
Matthew Thornton
Valentina Villani
Patrick Khatchadourian
Paolo Cravedi
Andrea Angeletti
Brendan Grubbs
Roger De Filippo
Laura Perin
Sargis Sedrakyan
author_sort Hasmik Soloyan
title Glomerular endothelial cell heterogeneity in Alport syndrome
title_short Glomerular endothelial cell heterogeneity in Alport syndrome
title_full Glomerular endothelial cell heterogeneity in Alport syndrome
title_fullStr Glomerular endothelial cell heterogeneity in Alport syndrome
title_full_unstemmed Glomerular endothelial cell heterogeneity in Alport syndrome
title_sort glomerular endothelial cell heterogeneity in alport syndrome
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2020-07-01
description Abstract Glomerular endothelial cells (GEC) are a crucial component of the glomerular physiology and their damage contributes to the progression of chronic kidney diseases. How GEC affect the pathology of Alport syndrome (AS) however, is unclear. We characterized GEC from wild type (WT) and col4α5 knockout AS mice, a hereditary disorder characterized by progressive renal failure. We used endothelial-specific Tek-tdTomato reporter mice to isolate GEC by FACS and performed transcriptome analysis on them from WT and AS mice, followed by in vitro functional assays and confocal and intravital imaging studies. Biopsies from patients with chronic kidney disease, including AS were compared with our findings in mice. We identified two subpopulations of GEC (dimtdT and brighttdT) based on the fluorescence intensity of the TektdT signal. In AS mice, the brighttdT cell number increased and presented differential expression of endothelial markers compared to WT. RNA-seq analysis revealed differences in the immune and metabolic signaling pathways. In AS mice, dimtdT and brighttdT cells had different expression profiles of matrix-associated genes (Svep1, Itgβ6), metabolic activity (Apom, Pgc1α) and immune modulation (Apelin, Icam1) compared to WT mice. We confirmed a new pro-inflammatory role of Apelin in AS mice and in cultured human GEC. Gene modulations were identified comparable to the biopsies from patients with AS and focal segmental glomerulosclerosis, possibly indicating that the same mechanisms apply to humans. We report the presence of two GEC subpopulations that differ between AS and healthy mice or humans. This finding paves the way to a better understanding of the pathogenic role of GEC in AS progression and could lead to novel therapeutic targets.
url https://doi.org/10.1038/s41598-020-67588-0
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