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Publication : Müller cell-mediated neurite outgrowth of the retinal ganglion cells via P2Y<sub>6</sub> receptor signals.

First Author  Taguchi M Year  2015
Journal  J Neurochem PubMed ID  26560804
Mgi Jnum  J:231101 Mgi Id  MGI:5766854
Doi  10.1111/jnc.13427 Citation  Taguchi M, et al. (2015) Muller cell-mediated neurite outgrowth of the retinal ganglion cells via P2Y6 receptor signals. J Neurochem
abstractText  Muller cells, the primary macroglia of the retina, support various functions of retinal ganglion cells (RGCs). Here, we demonstrate a nucleotide-mediated communication between these two types of cells, by which Muller cells control neurite outgrowth of RGCs by activation of P2 receptors such as P2Y6 . Cultured mouse RGCs had significantly enhanced neurite outgrowth when cultured with either cultured mouse Muller cells or conditioned medium derived from Muller cells, and this was completely inhibited by the nucleotide-degrading enzyme, apyrase. This increase in outgrowth was mimicked by exogenously applied nucleotides such as ATP, UTP and UDP. Pharmacological and genetic analysis revealed that P2Y6 receptor in RGCs was responsible for the increased neurite outgrowth. P2Y6 receptor was expressed in the ganglion cell layer of the retina and in RGC primary cultures. High performance liquid chromatography has revealed that Muller cells constitutively release UTP, which is immediately metabolized into UDP, an endogenous agonist for P2Y6 receptor. In the in vitro ocular hypertension model (i.e. glaucoma model), neurite outgrowth in RGCs was significantly reduced, which was associated with a decrease in P2Y6 receptors. Taken together, Muller cells control neurite outgrowth of RGCs by activating P2 receptors such as P2Y6 receptor, and the receptor expression level might be down-regulated in glaucoma. This article is protected by copyright. All rights reserved.
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