A selective EP4 PGE2 receptor agonist alleviates disease in a new mouse model of X-linked nephrogenic diabetes insipidus
Jian Hua Li, … , Mark A. Knepper, Jürgen Wess
Jian Hua Li, … , Mark A. Knepper, Jürgen Wess
Published September 1, 2009
Citation Information: J Clin Invest. 2009;119(10):3115-3126. https://doi.org/10.1172/JCI39680.
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Research Article Nephrology

A selective EP4 PGE2 receptor agonist alleviates disease in a new mouse model of X-linked nephrogenic diabetes insipidus

Abstract

X-linked nephrogenic diabetes insipidus (XNDI) is a severe kidney disease caused by inactivating mutations in the V2 vasopressin receptor (V2R) gene that result in the loss of renal urine-concentrating ability. At present, no specific pharmacological therapy has been developed for XNDI, primarily due to the lack of suitable animal models. To develop what we believe to be the first viable animal model of XNDI, we generated mice in which the V2R gene could be conditionally deleted during adulthood by administration of 4-OH-tamoxifen. Radioligand-binding studies confirmed the lack of V2R-binding sites in kidneys following 4-OH-tamoxifen treatment, and further analysis indicated that upon V2R deletion, adult mice displayed all characteristic symptoms of XNDI, including polyuria, polydipsia, and resistance to the antidiuretic actions of vasopressin. Gene expression analysis suggested that activation of renal EP4 PGE2 receptors might compensate for the lack of renal V2R activity in XNDI mice. Strikingly, both acute and chronic treatment of the mutant mice with a selective EP4 receptor agonist greatly reduced all major manifestations of XNDI, including changes in renal morphology. These physiological improvements were most likely due to a direct action on EP4 receptors expressed on collecting duct cells. These findings illustrate the usefulness of the newly generated V2R mutant mice for elucidating and testing new strategies for the potential treatment of humans with XNDI.

Authors

Jian Hua Li, Chung-Lin Chou, Bo Li, Oksana Gavrilova, Christoph Eisner, Jürgen Schnermann, Stasia A. Anderson, Chu-Xia Deng, Mark A. Knepper, Jürgen Wess

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Figure 5

Effects of prolonged treatment of V2R-KO mice with ONO on urine output, water intake, urine osmolality, and kidney morphology.

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Effects of prolonged treatment of V2R-KO mice with ONO on urine output, ...
(A and B) Urine output and water intake measurements. One day after the end of the TMX-injection period, V2R-KO mice received either vehicle or ONO (55 μg daily per mouse) via s.c. infusion for 9 days, followed by urine output (A) and water consumption (B) measurements (n = 4 or 5). (C) Urine osmolality measurements. Urine samples collected during the experiments shown in A and B were used for these measurements (n = 4 or 5). (D) Urine osmolality of vehicle- or ONO-treated V2R-KO mice over a 6-day period. Five days after the end of the TMX-injection period, V2R-KO mice received either vehicle or ONO (55 μg daily per mouse) via s.c. infusion (n = 4-6). (E) MRI images of kidneys from V2Rfl/yEsr1-Cre mice. Five days after the end of the TMX-injection period, V2R-KO mice received either vehicle or ONO (55 μg daily per mouse) via s.c. infusion for 2 weeks. Cavities where the contrast agent (Magnevist) accumulates in fluid appear white on the MRI (see Methods for experimental details). Representative images are shown (n = 4 per group). (F) Quantification of MRI images shown in E. Data are presented as mean ± SEM. *P < 0.05; ***P < 0.001. Veh, vehicle.