Endothelial mitochondrial oxidative stress determines podocyte depletion in segmental glomerulosclerosis
Ilse Daehn, … , Borje Haraldsson, Erwin P. Bottinger
Ilse Daehn, … , Borje Haraldsson, Erwin P. Bottinger
Published March 3, 2014
Citation Information: J Clin Invest. 2014;124(4):1608-1621. https://doi.org/10.1172/JCI71195.
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Research Article Nephrology

Endothelial mitochondrial oxidative stress determines podocyte depletion in segmental glomerulosclerosis

Abstract

Focal segmental glomerular sclerosis (FSGS) is a primary kidney disease that is commonly associated with proteinuria and progressive loss of glomerular function, leading to development of chronic kidney disease (CKD). FSGS is characterized by podocyte injury and depletion and collapse of glomerular capillary segments. Progression of FSGS is associated with TGF-β activation in podocytes; however, it is not clear how TGF-β signaling promotes disease. Here, we determined that podocyte-specific activation of TGF-β signaling in transgenic mice and BALB/c mice with Adriamycin-induced glomerulosclerosis is associated with endothelin-1 (EDN1) release by podocytes, which mediates mitochondrial oxidative stress and dysfunction in adjacent endothelial cells via paracrine EDN1 receptor type A (EDNRA) activation. Endothelial dysfunction promoted podocyte apoptosis, and inhibition of EDNRA or scavenging of mitochondrial-targeted ROS prevented podocyte loss, albuminuria, glomerulosclerosis, and renal failure. We confirmed reciprocal crosstalk between podocytes and endothelial cells in a coculture system. Biopsies from patients with FSGS exhibited increased mitochondrial DNA damage, consistent with EDNRA-mediated glomerular endothelial mitochondrial oxidative stress. Our studies indicate that segmental glomerulosclerosis develops as a result of podocyte-endothelial crosstalk mediated by EDN1/EDNRA-dependent mitochondrial dysfunction and suggest that targeting the reciprocal interaction between podocytes and endothelia may provide opportunities for therapeutic intervention in FSGS.

Authors

Ilse Daehn, Gabriella Casalena, Taoran Zhang, Shaolin Shi, Franz Fenninger, Nicholas Barasch, Liping Yu, Vivette D’Agati, Detlef Schlondorff, Wilhelm Kriz, Borje Haraldsson, Erwin P. Bottinger

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Figure 4

TGF-β signaling in podocytes induces oxidative stress specifically in endothelial cells.

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TGF-β signaling in podocytes induces oxidative stress specifically in en...
(A) Representative double-immunofluorescence images of 8-oxoG (green), endothelial cell marker CD31 (red), and merge showing colocalization. (B) Representative double-immunofluorescence images of 8-oxoG (green), podocyte marker synaptopodin (red), and merge in glomeruli of a day 4 Dox-treated PodTgfbr1 mouse showing no colocalization in podocytes. (C) 8-oxoG (green) and endothelial cell marker CD31 (red) in glomeruli of kidney biopsies from subjects diagnosed with FSGS. Higher-magnification images showing capillary loops are shown on the bottom row (arrows) (original magnification, ×63). (D) Immunofluorescence staining showing TUNEL and isolectin localization with DAPI in untreated mice and mice treated with Dox for 7 days. Arrows depict nuclear TUNEL with DAPI- and isolectin-positive endothelial cells. (E) Quantification of TUNEL- and isolectin-positive cells per glomeruli in untreated PodTgfbr1 mice and in PodTgfbr1 mice treated with Dox for 4 or 7 days (*P < 0.05; mean ± SD). Original magnification, ×63 (A, B, C [bottom row], and D); ×40 (C [top row]).