Literature DB >> 12507334

Localization of kainate receptors to the presynaptic active zone of the rod photoreceptor in primate retina.

D M Harvey1, D J Calkins.   

Abstract

Visual information is encoded at the photoreceptor synapse by modulation of the tonic release of glutamate from one or more electron-dense ribbons. This release is highest in the dark, when photoreceptors are depolarized, and decreases in grades when photoreceptors hyperpolarize with increasing light. Functional diversity between neurons postsynaptic at the synaptic ribbon arises in part from differential expression of both metabotropic (G-protein-gated) and ionotropic (ligand-gated) glutamate receptor. In the brain, different subunits also modulate the presynaptic active zone. In hippocampus, ionotropic kainate receptors localize to the presynaptic membrane of glutamatergic axon terminals and facilitate depolarization of the synapse (e.g. Lauri et al., 2001). Such facilitation may be helpful in the retina, where consistent depolarization of the photoreceptor axon terminal is necessary to maintain glutamate release in the dark. We investigated whether such a mechanism could be present in primate retina by using electron microscopy to examine the localization of the kainate subunits GluR6/7 at the rod axon terminal, where only a single ribbon synapse mediates glutamate release. We scored 54 rod axon terminals whose postsynaptic space contained one or more GluR6/7-labeled processes and traced these processes through serial sections to determine their identity. Of 68 labeled processes, 63% originated from narrow "fingers" of cytoplasm extending from the presynaptic axon terminal into the postsynaptic cleft. Each rod terminal typically inserts 4-6 presynaptic fingers, and we scored several instances where multiple fingers contained label. Such consistency suggests that each presynaptic finger expresses GluR6/7. The physiological properties of kainate receptors and the geometry of the rod axon terminal suggest that presynaptic GluR6/7 could provide a steady inward current to maintain consistent depolarization of the rod synapse in the long intervals between photons in the dark.

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Year:  2002        PMID: 12507334     DOI: 10.1017/s0952523802195137

Source DB:  PubMed          Journal:  Vis Neurosci        ISSN: 0952-5238            Impact factor:   3.241


  11 in total

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4.  Clustered mutations in the GRIK2 kainate receptor subunit gene underlie diverse neurodevelopmental disorders.

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5.  TRPV1: contribution to retinal ganglion cell apoptosis and increased intracellular Ca2+ with exposure to hydrostatic pressure.

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6.  Effects of the AMPA antagonist ZK 200775 on visual function: a randomized controlled trial.

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Journal:  PLoS One       Date:  2010-08-12       Impact factor: 3.240

7.  Contribution of TRPV1 to microglia-derived IL-6 and NFkappaB translocation with elevated hydrostatic pressure.

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8.  Induced autoimmunity to heat shock proteins elicits glaucomatous loss of retinal ganglion cell neurons via activated T-cell-derived fas-ligand.

Authors:  Martin B Wax; Gülgün Tezel; Junjie Yang; Guanghua Peng; Rajkumar V Patil; Neeraj Agarwal; Rebecca M Sappington; David J Calkins
Journal:  J Neurosci       Date:  2008-11-12       Impact factor: 6.167

9.  AMPA and kainate receptors in turtle retina: an immunocytochemical study.

Authors:  Lily Vitanova
Journal:  Cell Mol Neurobiol       Date:  2007-01-19       Impact factor: 4.231

10.  Expression of mRNA for glutamate receptor subunits distinguishes the major classes of retinal neurons, but is less specific for individual cell types.

Authors:  Tatjana C Jakobs; Yixin Ben; Richard H Masland
Journal:  Mol Vis       Date:  2007-06-18       Impact factor: 2.367

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