PubMed 19809515
Referenced in: none
Automatically associated channels: Kir4.1 , Slo1
Title: Functional implication of Dp71 in osmoregulation and vascular permeability of the retina.
Authors: Abdoulaye Sene, Ramin Tadayoni, Thomas Pannicke, Antje Wurm, Brahim El Mathari, Romain Benard, Michel Joseph Roux, David Yaffe, Dominique Mornet, Andreas Reichenbach, José-Alain Sahel, Alvaro Rendon
Journal, date & volume: PLoS ONE, 2009 , 4, e7329
PubMed link: http://www.ncbi.nlm.nih.gov/pubmed/19809515
Abstract
Functional alterations of Müller cells, the principal glia of the retina, are an early hallmark of most retina diseases and contribute to their further progression. The molecular mechanisms of these reactive Müller cell alterations, resulting in disturbed retinal homeostasis, remain largely unknown. Here we show that experimental detachment of mouse retina induces mislocation of the inwardly rectifying potassium channels (Kir4.1) and a downregulation of the water channel protein (AQP4) in Müller cells. These alterations are associated with a strong decrease of Dp71, a cytoskeleton protein responsible for the localization and the clustering of Kir4.1 and AQP4. Partial (in detached retinas) or total depletion of Dp71 in Müller cells (in Dp71-null mice) impairs the capability of volume regulation of Müller cells under osmotic stress. The abnormal swelling of Müller cells In Dp71-null mice involves the action of inflammatory mediators. Moreover, we investigated whether the alterations in Müller cells of Dp71-null mice may interfere with their regulatory effect on the blood-retina barrier. In the absence of Dp71, the retinal vascular permeability was increased as compared to the controls. Our results reveal that Dp71 is crucially implicated in the maintenance of potassium homeostasis, in transmembraneous water transport, and in the Müller cell-mediated regulation of retinal vascular permeability. Furthermore, our data provide novel insights into the mechanisms of retinal homeostasis provided by Müller cells under normal and pathological conditions.