Long-Term Endothelin-A Receptor Antagonism Provides Robust Renal Protection in Humanized Sickle Cell Disease Mice

Overview

Journal J Am Soc Nephrol

Specialty Nephrology

Date 2017 Mar 29

PMID 28348063

Citations 36

Authors

Malgorzata Kasztan

Brandon M Fox

Joshua S Speed

Carmen De Miguel

Eman Y Gohar

Tim M Townes

Abdullah Kutlar

Jennifer S Pollock

David M Pollock

Affiliations

Soon will be listed here.

Abstract

Sickle cell disease (SCD)-associated nephropathy is a major source of morbidity and mortality in patients because of the lack of efficacious treatments targeting renal manifestations of the disease. Here, we describe a long-term treatment strategy with the selective endothelin-A receptor (ET) antagonist, ambrisentan, designed to interfere with the development of nephropathy in a humanized mouse model of SCD. Ambrisentan preserved GFR at the level of nondisease controls and prevented the development of proteinuria, albuminuria, and nephrinuria. Microscopy studies demonstrated prevention of podocyte loss and structural alterations, the absence of vascular congestion, and attenuation of glomerulosclerosis in treated mice. Studies in isolated glomeruli showed that treatment reduced inflammation and oxidative stress. At the level of renal tubules, ambrisentan treatment prevented the increased excretion of urinary tubular injury biomarkers. Additionally, the treatment strategy prevented tubular brush border loss, diminished tubular iron deposition, blocked the development of interstitial fibrosis, and prevented immune cell infiltration. Furthermore, the prevention of albuminuria in treated mice was associated with preservation of cortical megalin expression. In a separate series of identical experiments, combined ET and ET receptor antagonism provided only some of the protection observed with ambrisentan, highlighting the importance of exclusively targeting the ET receptor in SCD. Our results demonstrate that ambrisentan treatment provides robust protection from diverse renal pathologies in SCD mice, and suggest that long-term ET receptor antagonism may provide a strategy for the prevention of renal complications of SCD.

Citing Articles

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Endothelin receptor antagonists in chronic kidney disease.

Smeijer J, Kohan D, Dhaun N, Noronha I, Liew A, Heerspink H Nat Rev Nephrol. 2024; 21(3):175-188.

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Comprehensive analysis of the endothelin system in the kidneys of mice, rats, and humans.

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End Organ Affection in Sickle Cell Disease.

Bathla T, Lotfollahzadeh S, Quisel M, Mehta M, Malikova M, Chitalia V Cells. 2024; 13(11.

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Endothelin System in Hypertension and Chronic Kidney Disease.

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