Apo state pore opening as functional basis of increased EAAT anion channel activity in episodic ataxia 6

Suslova, Mariia; Kortzak, Daniel; Machtens, Jan‐Philipp; Kovermann, Peter; Fahlke, Christoph

doi:10.3389/fphys.2023.1147216

Cited by 2 publications

References 69 publications

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Allosteric modulation of proton binding confers Cl^-activation and glutamate selectivity to vesicular glutamate transporters

Borghans,

Kortzak,

Longo

et al. 2024

Preprint

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Vesicular glutamate transporters (VGLUTs) fill synaptic vesicles with glutamate and remove luminal Cl-via an additional anion channel mode. Both of these transport functions are stimulated by luminal acidification, luminal-positive membrane potential, and luminal Cl-. We studied VGLUT1 transporter/channel activation using a combination of heterologous expression, cellular electrophysiology, fast solution exchange, and mathematical modeling. Cl-channel gating can be described with a kinetic scheme that includes two protonation sites and distinct opening, closing, and Cl--binding rates for each protonation state. Cl-binding promotes channel opening by modifying the pKa values of the protonation sites and rates of pore opening and closure. VGLUT1 transports glutamate and aspartate at distinct stoichiometries: H+-glutamate exchange at 1:1 stoichiometry and aspartate uniport. Neurotransmitter transport with variable stoichiometry can be described with an alternating access model that assumes that transporters without substrate translocate in the doubly protonated state to the inward-facing conformation and return with the bound amino acid substrate as either singly or doubly protonated. Glutamate, but not aspartate, promotes the release of one proton from inward-facing VGLUT1, resulting in preferential H+-coupled glutamate exchange. Cl-stimulates glutamate transport by making the glutamate-binding site accessible to cytoplasmic glutamate and by facilitating transitions to the inward-facing conformation after outward substrate release. We conclude that allosteric modification of transporter protonation by Cl-is crucial for both VGLUT1 transport functions.

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Allosteric modulation of proton binding confers Cl^-activation and glutamate selectivity to vesicular glutamate transporters

Borghans,

Kortzak,

Longo

et al. 2024

Preprint

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Increased excitatory amino acid transporter 2 levels in basolateral amygdala astrocytes mediate chronic stress–induced anxiety-like behavior

Xu,

Xuan,

Chen

et al. 2024

Neural Regeneration Research

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The conventional perception of astrocytes as mere supportive cells within the brain has recently been called into question by empirical evidence, which has revealed their active involvement in regulating brain function and encoding behaviors associated with emotions. Specifically, astrocytes in the basolateral amygdala (BLA) have been found to play a role in the modulation of anxiety-like behaviors triggered by chronic stress. Nevertheless, the precise molecular mechanisms by which BLA astrocytes regulate chronic stress–induced anxiety-like behaviors remain to be fully elucidated. In this study, we found that in a mouse model of anxiety triggered by unpredictable chronic mild stress (UCMS), the expression of excitatory amino acid transporter 2 (EAAT2) was upregulated in the BLA. Interestingly, our findings indicate that the targeted knockdown of EAAT2 specifically within the BLA astrocytes was able to rescue the anxiety-like behavior in mice subjected to stress. Furthermore, we found that the overexpression of EAAT2 in the BLA, whether achieved through intracranial administration of EAAT2 agonists or through injection of EAAT2-overexpressing viruses with GfaABC1D promoters, evoked anxiety-like behavior in mice. Our single-nucleus RNA sequencing analysis further confirmed that chronic stress induced an upregulation of EAAT2 specifically in astrocytes in the BLA. Moreover, through in vivo calcium signal recordings, we found that the frequency of calcium activity in the BLA of mice subjected to chronic stress was higher compared with normal mice. After knocking down the expression of EAAT2 in the BLA, the frequency of calcium activity was not significantly increased, and anxiety-like behavior was obviously mitigated. Additionally, administration of an EAAT2 inhibitor in the BLA yielded a notable reduction in anxiety level among mice subjected to stress. These results suggest that BLA astrocytic EAAT2 plays a role in in the regulation of UCMS-induced anxiety-like behavior by impacting the activity of local glutamatergic neurons, and targeting EAAT2 in the BLA holds therapeutic promise for addressing anxiety disorders.

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Apo state pore opening as functional basis of increased EAAT anion channel activity in episodic ataxia 6

Cited by 2 publications

References 69 publications

Allosteric modulation of proton binding confers Cl^-activation and glutamate selectivity to vesicular glutamate transporters

Allosteric modulation of proton binding confers Cl^-activation and glutamate selectivity to vesicular glutamate transporters

Increased excitatory amino acid transporter 2 levels in basolateral amygdala astrocytes mediate chronic stress–induced anxiety-like behavior

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Apo state pore opening as functional basis of increased EAAT anion channel activity in episodic ataxia 6

Cited by 2 publications

References 69 publications

Allosteric modulation of proton binding confers Cl-activation and glutamate selectivity to vesicular glutamate transporters

Allosteric modulation of proton binding confers Cl-activation and glutamate selectivity to vesicular glutamate transporters

Increased excitatory amino acid transporter 2 levels in basolateral amygdala astrocytes mediate chronic stress–induced anxiety-like behavior

Contact Info

Product

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Allosteric modulation of proton binding confers Cl^-activation and glutamate selectivity to vesicular glutamate transporters

Allosteric modulation of proton binding confers Cl^-activation and glutamate selectivity to vesicular glutamate transporters