Electrogenic uptake of glutamate and aspartate into glial cells isolated from the salamander (Ambystoma) retina.

Barbour, Boris; Brew, Helen M.; Attwell, David

doi:10.1113/jphysiol.1991.sp018545

Cited by 186 publications

(182 citation statements)

References 40 publications

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“…The inclusion of 0.25 mM glutamate (or glutamine) in the media fulfilled this need. Since the amplitude of the b-wave was maintained in the rat retinas incubated in media containing 0.25 mM glutamate, we believe that the level of glutamate in the synaptic regions in the outer plexiform layer is at a physiological concentration, perhaps in the range of 1-10 μM (Brew & Attwell, 1987;Barbour et al, 1991), though its concentration at this site has not been measured in this tissue. An unphysiologically high level of glutamate in the synaptic zones between photoreceptor cells and ON-bipolars would be expected to saturate the glutamate receptors on the bipolar cells in darkness and in light, thereby resulting in a decline in the amplitude of the b-wave, as is observed when the bath concentration of glutamate is raised to 2-5 mM (data not shown).…”

Section: Discussionmentioning

confidence: 99%

“…Given the high release in the dark, for continued normal function of excitatory glutamatergic synapses in the retina, it is important that the extracellular concentration of glutamate be controlled so that the receptors are not saturated. This is usually accomplished by uptake of the released glutamate into cells within the localized region bordering the synaptic region, rather than by extracellular enzymatic degradation (Hertz, 1979;Brew & Attwell, 1987;Barbour et al, 1991;Kanai et al, 1993;Eliasoff & Werblin, 1993;Rauen & Kanner, 1994;Derouiche & Rauen, 1995;Sontheimer, 1995;Yang & Wu, 1997). The cells which could participate in the uptake of synaptically released glutamate include the photoreceptor cells themselves, the horizontal cells, the bipolar cells, and the glial (Müller) cells.…”

Section: Introductionmentioning

confidence: 99%

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Effects of inhibiting glutamine synthetase and blocking glutamate uptake on b-wave generation in the isolated rat retina

et al. 1999

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The purpose of the present experiments was to evaluate the contribution of the glutamate-glutamine cycle in retinal glial (Müller) cells to photoreceptor cell synaptic transmission. Dark-adapted isolated rat retinas were superfused with oxygenated bicarbonate-buffered media. Recordings were made of the b-wave of the electroretinogram as a measure of light-induced photoreceptor to ON-bipolar neuron transmission. L-methionine sulfoximine (1-10 mM) was added to superfusion media to inhibit glutamine synthetase, a Müller cell specific enzyme, by more than 99% within 5-10 min, thereby disrupting the conversion of glutamate to glutamine in the Müller cells. Threohydroxyaspartic acid and D-aspartate were used to block glutamate transporters. The amplitude of the b-wave was well maintained for 1-2 h provided 0.25 mM glutamate or 0.25 mM glutamine was included in the media. Without exogenous glutamate or glutamine the amplitude of the b-wave declined by about 70% within 1 h. Inhibition of glutamate transporters led to a rapid (2-5 min) reversible loss of the b-wave in the presence and absence of the amino acids. In contrast, inhibition of glutamine synthetase did not alter significantly either the amplitude of the b-wave in the presence of glutamate or glutamine or the rate of decline of the b-wave found in the absence of these amino acids. Excellent recovery of the b-wave was found when 0.25 mM glutamate was resupplied to Lmethionine sulfoximine-treated retinas. The results suggest that in the isolated rat retina uptake of released glutamate into photoreceptors plays a more important role in transmitter recycling than does uptake of glutamate into Müller cells and its subsequent conversion to glutamine.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Effects of inhibiting glutamine synthetase and blocking glutamate uptake on b-wave generation in the isolated rat retina

et al. 1999

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“…3C). This probably indicated intracellular accumulation of Na ϩ or glutamate, or both, and a breakdown of the respective concentration gradients over the plasma membrane (Barbour et al, 1991). In another subgroup of green fluorescent cells, morphologically resembling GluR cells, glutamate evoked neither GluR responses nor uptake currents ("silent cells"; 16% of the weakly fluorescent cells with few processes).…”

Section: Brightly Fluorescent Cells Express Glutamate Transporter Butmentioning

confidence: 99%

Segregated Expression of AMPA-Type Glutamate Receptors and Glutamate Transporters Defines Distinct Astrocyte Populations in the Mouse Hippocampus

et al. 2003

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“…GluTPs are pharmacologically distinct from both iGluRs and mGluRs and L-Glu, L-Asp, and D-Asp are s u b s t r a t e s f o r t h e t r a n s p o r t e r s 1 2 9 , 1 3 0 , 1 7 5 ; G l u R agonists 129,130,175,176 and antagonists 130,177 are not. Glu uptake can be blocked by the transporter blockers dihydrokainate (DHKA) and DL-threo-β-hydroxyaspartate (HA) 130,177 .…”

Section: ) Glutamatementioning

confidence: 99%

“…Glu uptake can be blocked by the transporter blockers dihydrokainate (DHKA) and DL-threo-β-hydroxyaspartate (HA) 130,177 .…”

Section: ) Glutamatementioning

confidence: 99%

A Review of Glutamate Receptors I: Current Understanding of Their Biology

Rousseaux

2008

J Toxicol Pathol

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Seventy years ago it was discovered that glutamate is abundant in the brain and that it plays a central role in brain metabolism. However, it took the scientific community a long time to realize that glutamate also acts as a neurotransmitter. Glutamate is an amino acid and brain tissue contains as much as 5 -15 mM glutamate per kg depending on the region, which is more than of any other amino acid. The main motivation for the ongoing research on glutamate is due to the role of glutamate in the signal transduction in the nervous systems of apparently all complex living organisms, including man. Glutamate is considered to be the major mediator of excitatory signals in the mammalian central nervous system and is involved in most aspects of normal brain function including cognition, memory and learning. In this review, the basic biology of the excitatory amino acids glutamate, glutamate receptors, GABA, and glycine will first be explored. In the second part of this review, the known pathophysiology and pathology will be described. (J Toxicol Pathol 2008; 21: 25-51)

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Electrogenic uptake of glutamate and aspartate into glial cells isolated from the salamander (Ambystoma) retina.

Cited by 186 publications

References 40 publications

Effects of inhibiting glutamine synthetase and blocking glutamate uptake on b-wave generation in the isolated rat retina

Effects of inhibiting glutamine synthetase and blocking glutamate uptake on b-wave generation in the isolated rat retina

Segregated Expression of AMPA-Type Glutamate Receptors and Glutamate Transporters Defines Distinct Astrocyte Populations in the Mouse Hippocampus

A Review of Glutamate Receptors I: Current Understanding of Their Biology

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