Mineralocorticoid receptor is involved in rat and human ocular chorioretinopathy
Min Zhao, … , Frédéric Jaisser, Francine Behar-Cohen
Min Zhao, … , Frédéric Jaisser, Francine Behar-Cohen
Published June 11, 2012
Citation Information: J Clin Invest. 2012;122(7):2672-2679. https://doi.org/10.1172/JCI61427.
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Research Article Ophthalmology

Mineralocorticoid receptor is involved in rat and human ocular chorioretinopathy

Abstract

Central serous chorioretinopathy (CSCR) is a vision-threatening eye disease with no validated treatment and unknown pathogeny. In CSCR, dilation and leakage of choroid vessels underneath the retina cause subretinal fluid accumulation and retinal detachment. Because glucocorticoids induce and aggravate CSCR and are known to bind to the mineralocorticoid receptor (MR), CSCR may be related to inappropriate MR activation. Our aim was to assess the effect of MR activation on rat choroidal vasculature and translate the results to CSCR patients. Intravitreous injection of the glucocorticoid corticosterone in rat eyes induced choroidal enlargement. Aldosterone, a specific MR activator, elicited the same effect, producing choroid vessel dilation -and leakage. We identified an underlying mechanism of this effect: aldosterone upregulated the endothelial vasodilatory K channel KCa2.3. Its blockade prevented aldosterone-induced thickening. To translate these findings, we treated 2 patients with chronic nonresolved CSCR with oral eplerenone, a specific MR antagonist, for 5 weeks, and observed impressive and rapid resolution of retinal detachment and choroidal vasodilation as well as improved visual acuity. The benefit was maintained 5 months after eplerenone withdrawal. Our results identify MR signaling as a pathway controlling choroidal vascular bed relaxation and provide a pathogenic link with human CSCR, which suggests that blockade of MR could be used therapeutically to reverse choroid vasculopathy.

Authors

Min Zhao, Isabelle Célérier, Elodie Bousquet, Jean-Claude Jeanny, Laurent Jonet, Michèle Savoldelli, Olivier Offret, Antoine Curan, Nicolette Farman, Frédéric Jaisser, Francine Behar-Cohen

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Figure 2

Expression and aldosterone regulation of KCa2.3 in rat eyes.

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Expression and aldosterone regulation of KCa2.3 in rat eyes. (A) Immunof...
(A) Immunofluorescence localization of KCa2.3 and CD31 in the retina. KCa2.3 labeling was restricted to the choroid vessels, CD31 labeled both choroid and retinal vessels (arrowhead). Higher magnification of KCa2.3 labeling of choroid vessels (arrowheads) and nuclei (blue) is shown below. Scale bars: 100 μm (top); 25 μm (bottom). (B) KCa2.3 and CD31 were colocalized (arrowhead) in choroid vessel endothelial cells. Scale bar: 25 μm. (C) Colocalization of KCa2.3 and CD31 (arrowhead) in a choroid vessel. Scale bar: 25 μm. See Supplemental Figure 4 for lower magnification and separate signals of individual markers. (D) KCa2.3 expression was increased in aldosterone-injected eyes compared with vehicle injection, an effect prevented by coinjection with the MR antagonist canreonate (Canre) in 500-fold excess. Shown are Western blot on choroid samples and quantification of KCa2.3/β-actin, relative to vehicle-injected eyes (n = 8 per condition). **P < 0.01, ***P < 0.001.