2021
DOI: 10.1016/j.neuint.2021.105142
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Pharmacological evidence for the concept of spare glutamate transporters

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Cited by 3 publications
(3 citation statements)
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“…One notable feature of our iGluSnFR decay measures was that genotype differences were typically only detected after a longer train of neural activity was evoked with 100 pulses, and not with 5 pulses. A possible explanation for this finding is suggested by the concept of spare glutamate transporters [ 70 ], and that the glutamate released by 5 pulses is insufficient to overwhelm the glutamate uptake system. In other words, 3xTg mice still have sufficient GLT-1 protein to efficiently clear glutamate released by short bursts of activity.…”
Section: Discussionmentioning
confidence: 99%
“…One notable feature of our iGluSnFR decay measures was that genotype differences were typically only detected after a longer train of neural activity was evoked with 100 pulses, and not with 5 pulses. A possible explanation for this finding is suggested by the concept of spare glutamate transporters [ 70 ], and that the glutamate released by 5 pulses is insufficient to overwhelm the glutamate uptake system. In other words, 3xTg mice still have sufficient GLT-1 protein to efficiently clear glutamate released by short bursts of activity.…”
Section: Discussionmentioning
confidence: 99%
“…Although these assays use different readouts, one explanation for this discrepancy might be the high competing concentrations of substrate in the cell swelling assay, which are 100–10,000 times higher than in radioligand uptake assays ( Fontana, 2018 ). Alternatively, dox-induced overexpression of EAATs could create a pool of “spare” transporters on the plasma membrane that effectively buffers the extracellular concentration of inhibitor, resulting in a rightward shift of the concentration-inhibition curve and a lower apparent inhibitory potency ( Belo do Nascimento et al, 2021 ). Although the transporter expression levels and substrate concentrations should be thoroughly considered in further assay development, our impedance-based assay showed a robust window for the detection of transporter inhibitors.…”
Section: Discussionmentioning
confidence: 99%
“…One notable feature of our iGluSnFR decay measures was that genotype differences were typically only detected after a longer train of neural activity was evoked with 100 pulses, and not with 5 pulses. The most likely explanation for this finding is suggested by the concept of spare glutamate transporters (Belo do Nascimento et al, 2021), and that the glutamate released by 5 pulses is insufficient to overwhelm the glutamate uptake system. In other words, 3xTg still have sufficient GLT-1 protein to efficiently clear glutamate released by short bursts of activity.…”
Section: Activity-dependent Slowing Of Glutamate Clearancementioning
confidence: 99%