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Literature DB >> 32046810

Inhibitory components of retinal bipolar cell receptive fields are differentially modulated by dopamine D1 receptors.

Abstract

During adaptation to an increase in environmental luminance, retinal signaling adjustments are mediated by the neuromodulator dopamine. Retinal dopamine is released with light and can affect center-surround receptive fields, the coupling state between neurons, and inhibitory pathways through inhibitory receptors and neurotransmitter release. While the inhibitory receptive field surround of bipolar cells becomes narrower and weaker during light adaptation, it is unknown how dopamine affects bipolar cell surrounds. If dopamine and light have similar effects, it would suggest that dopamine could be a mechanism for light-adapted changes. We tested the hypothesis that dopamine D1 receptor activation is sufficient to elicit the magnitude of light-adapted reductions in inhibitory bipolar cell surrounds. Surrounds were measured from OFF bipolar cells in dark-adapted mouse retinas while stimulating D1 receptors, which are located on bipolar, horizontal, and inhibitory amacrine cells. The D1 agonist SKF-38393 narrowed and weakened OFF bipolar cell inhibitory receptive fields but not to the same extent as with light adaptation. However, the receptive field surround reductions differed between the glycinergic and GABAergic components of the receptive field. GABAergic inhibitory strength was reduced only at the edges of the surround, while glycinergic inhibitory strength was reduced across the whole receptive field. These results expand the role of retinal dopamine to include modulation of bipolar cell receptive field surrounds. Additionally, our results suggest that D1 receptor pathways may be a mechanism for the light-adapted weakening of glycinergic surround inputs and the furthest wide-field GABAergic inputs to bipolar cells. However, remaining differences between light-adapted and D1 receptor-activated inhibition demonstrate that non-D1 receptor mechanisms are necessary to elicit the full effect of light adaptation on inhibitory surrounds.

Entities: Chemical Disease Gene Species

Keywords: Amacrine cell; Bipolar cell; GABA; Glycine; Luminance

Mesh：

Substances：

Year: 2020 PMID： 32046810 PMCID： PMC7027730 DOI： 10.1017/S0952523819000129

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

80 in total

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Journal: J Neurosci Date: 2002-04-01 Impact factor: 6.167

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Journal: J Neurosci Date: 2001-07-01 Impact factor: 6.167

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Journal: J Neurosci Date: 2007-04-25 Impact factor: 6.167

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Journal: Vis Neurosci Date: 1997 May-Jun Impact factor: 3.241

7. Effects of dopamine antagonists on receptive fields of brisk cells and directionally selective cells in the rabbit retina.

Authors: R J Jensen; N W Daw
Journal: J Neurosci Date: 1984-12 Impact factor: 6.167

8. Eliminating Glutamatergic Input onto Horizontal Cells Changes the Dynamic Range and Receptive Field Organization of Mouse Retinal Ganglion Cells.

Authors: Sebastian Ströh; Christian Puller; Sebastian Swirski; Maj-Britt Hölzel; Lea I S van der Linde; Jasmin Segelken; Konrad Schultz; Christoph Block; Hannah Monyer; Klaus Willecke; Reto Weiler; Martin Greschner; Ulrike Janssen-Bienhold; Karin Dedek
Journal: J Neurosci Date: 2018-01-19 Impact factor: 6.167

Inhibitory components of retinal bipolar cell receptive fields are differentially modulated by dopamine D1 receptors.

1. Functional asymmetries in ON and OFF ganglion cells of primate retina.

2. Synaptic currents generating the inhibitory surround of ganglion cells in the mammalian retina.

3. Ambient light regulates sodium channel activity to dynamically control retinal signaling.

4. Interaction between center and surround in rabbit retinal ganglion cells.

5. Tracer coupling pattern of amacrine and ganglion cells in the rabbit retina.

6. Immunocytochemical localization of dopamine D1 receptors in the retina of mammals.

7. Effects of dopamine antagonists on receptive fields of brisk cells and directionally selective cells in the rabbit retina.

8. Eliminating Glutamatergic Input onto Horizontal Cells Changes the Dynamic Range and Receptive Field Organization of Mouse Retinal Ganglion Cells.

9. Controlling the gain of rod-mediated signals in the Mammalian retina.

10. Interactions of dopamine and the release of [3H]-taurine and [3H]-glycine from the isolated retina of the rat.

1. Dopamine D1 and D4 receptors contribute to light adaptation in ON-sustained retinal ganglion cells.

2. Glycine Release Is Potentiated by cAMP via EPAC2 and Ca²⁺ Stores in a Retinal Interneuron.

3. The effects of reduced ambient lighting on lens compensation in infant rhesus monkeys.

4. Center-surround interactions underlie bipolar cell motion sensitivity in the mouse retina.

5. High glucose treatment promotes extracellular matrix proteome remodeling in Mller glial cells.