Gabaa Receptor
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Synchrony and Synaptic Signaling in Cerebellar Circuits
The cerebellum permits a wide range of behaviors that involve sensorimotor integration. We have been investigating how specific cellular and synaptic specializations of cerebellar neurons measured in vitro, give rise to circuit activity in vivo. We have investigated these issues by studying Purkinje neurons as well as the large neurons of the mouse cerebellar nuclei, which form the major excitatory premotor projection from the cerebellum. Large CbN cells have ion channels that favor spontaneous action potential firing and GABAA receptors that generate ultra-fast inhibitory synaptic currents, raising the possibility that these biophysical attributes may permit CbN cells to respond differently to the degree of temporal coherence of their Purkinje cell inputs. In vivo, self-initiated motor programs associated with whisking correlates with asynchronous changes in Purkinje cell simple spiking that are asynchronous across the population. The resulting inhibition converges with mossy fiber excitation to yield little change in CbN cell firing, such that cerebellar output is low or cancelled. In contrast, externally applied sensory stimuli elicits a transient, synchronous inhibition of Purkinje cell simple spiking. During the resulting strong disinhibition of CbN cells, sensory-induced excitation from mossy fibers effectively drives cerebellar outputs that increase the magnitude of reflexive whisking. Purkinje cell synchrony, therefore, may be a key variable contributing to the “positive effort” hypothesized by David Marr in 1969 to be necessary for cerebellar control of movement.
Downregulation of extra-synaptic delta GABAA receptors is correlated with disrupted tonic inhibition in an APP knock-in mouse model of Alzheimer’s disease
Comparing the efficacy of selective negative allosteric modulators of α5‐containing GABAA receptors on synaptic inhibition and cognitive deficits in a mouse model of Down syndrome
A conserved region at the end of the N-terminal extracellular domain of GABAA receptor subunits is crucial for the receptor forward trafficking
Golexanolone, a GABAA receptor modulating steroid antagonist, reverses neuroinflammation in cerebellum and hippocampus and restores motor coordination and cognitive function in hyperammonemic rats
Modulation by neurosteroids of the GABAA receptors and Kir channels expressed in oligodendroglia
Pharmacology and desensitization properties of α4-containg GABAA receptors
GABAA receptors and neuroligin 2 synergize to promote synaptic adhesion and inhibitory synaptogenesis
FENS Forum 2024
Golexanolone, a GABAA receptor-modulating steroid antagonist, improves neuroinflammation, fatigue, anxiety, depression, and some cognitive and motor alterations in a rat model of Parkinson's disease
FENS Forum 2024
GABAA receptors modulate anxiety-like behavior through the central amygdala area in rats with higher physical activity
FENS Forum 2024
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