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Active NON-SBIR/STTR RPGS NIH (US)

Astrocyte-neuron mechanisms of glutamatergic modulation in social novelty recognition

$3.85M USD

Funder NATIONAL INSTITUTE OF MENTAL HEALTH
Recipient Organization Augusta University
Country United States
Start Date Jul 25, 2024
End Date Feb 28, 2029
Duration 1,679 days
Number of Grantees 1
Roles Principal Investigator
Data Source NIH (US)
Grant ID 10943091
Grant Description

Project Summary Social behavior is a fundamental component of complex behaviors for animals to sustain healthy living patterns. Consequently, deficits or dysfunctional social behaviors are found in multiple psychiatric and neurological disorders, such as autism spectrum disorder (ASD). Recently, a growing body of research demonstrates a

significant adaptation of astrocytes, non-neuronal glial cells in the brain, in the etiology of ASD. However, the detailed mechanisms underlying how astrocyte dysfunction represents social behavioral deficiency remain poorly understood. Particularly, the challenge is exaggerated by the lack of knowledge about whether and how

the local astrocytes affect the ASD-phenotype brain in cell-type, circuit, and network levels. Abnormal glutamatergic transmission contributes to aberrant hyperexcitability in brain regions critical for controlling social behaviors by shifting the excitation-to-inhibition ratio. Excess glutamate is typically cleared from

the synaptic cleft into astrocytes via glutamate transporters. Our recent studies revealed that astrocyte activation in the paraventricular nucleus of the thalamus (PVT), a hub of communications in thalamo-cortical circuits where processes the sensitivity to external social environmental stimuli, impairs social novelty recognition while

parallelly downregulating functional astrocyte dominant glutamate transporter type 1 (GLT1; EAAT2 in humans). Interestingly, astrocyte-specific conditional knock-out of GLT1 in the PVT mimics the impairment of social novelty recognition, reinforcing the importance of the glutamatergic system in astrocyte-based social behavioral

modulation. Thus, based on our findings, we hypothesize that astrocytic modulation of glutamatergic signaling has an important role in the regulation of social novelty recognition. Chemogenetic activation of astrocytes, mimicking reactive calcium-increased astrocytes and sequentially reducing GLT1 function, impairs the normal

response of astrocytes in the PVT to neuronal activity and this, in turn, contributes to abnormal social recognition. In contrast, GLT1 overexpression facilitates the maintenance of normal social recognition behaviors. To investigate this hypothesis, first we will investigate the spatiotemporal glutamate and calcium signals

synchronized to social behaviors in the astrocytes and neurons and their adaptation by GLT1 modulation. Second, we will examine the contribution of PVT GLT1 null and overexpression in synaptic events and metabolism in the PVT circuits, and consequent social novelty recognition behaviors. Finally, we will determine

whether astrocytic glutamate modulation via GLT1 affects the brain-wide spatiotemporal signature, and the brain network coherence provides any distinguishable profiles that represent social behavioral outcomes. Our study will elucidate the detailed mechanisms of astrocyte-neuron interaction via the glutamate

system encoding social novelty recognition. We will provide a rational path for the development of new therapeutic methods for the treatment of social behavioral deficits.

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Augusta University

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