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Active NON-SBIR/STTR RPGS NIH (US)

Basal Forebrain Non-cholinergic Circuit Mechanisms of Sustained Attention

$5.82M USD

Funder NATIONAL INSTITUTE OF MENTAL HEALTH
Recipient Organization Washington University
Country United States
Start Date Sep 01, 2024
End Date May 31, 2029
Duration 1,733 days
Number of Grantees 1
Roles Principal Investigator
Data Source NIH (US)
Grant ID 10946455
Grant Description

ABSTRACT The long-term goal is to understand how basal forebrain (BF) circuits underlie cognitive functions like sustained attention. Traditionally, BF was thought to mediate attention through its cholinergic neurons and cortical acetylcholine release. However, recent recordings suggest that cholinergic signaling

reflects arousal and reinforcement learning instead. If not cholinergic neurons, what alternative BF circuits support attention? The objective of this proposal is to determine the circuit and behavioral roles of an understudied BF population: parvalbumin-expressing GABAergic neurons (BF-PV) that project to the cortex. Our

previous work using a sustained attention-demanding auditory detection task revealed that BF cholinergic neurons respond to reinforcement surprises, independent of temporal fluctuations of attention. This discovery prompted an investigation into alternative BF neuron types. Our preliminary studies suggest that BF-PV neurons have key attributes relevant for sustained attention: their activity

predicts detection accuracy and reaction time on a trial-by-trial basis, and their optogenetic stimulation enhances performance. Using quantitative behavior, cell-type-specific recordings and manipulations, viral tracing, and computational modeling, we aim to explore the link between BF-PV neurons and sustained attention.

Aim 1 will map BF-PV cortical projections and investigate whether they produce cortical gain control through disinhibition. Aim 2 will record BF-PV neuron activity to assess how its dynamics predict momentary attention levels during sustained attention tasks and use optogenetics to evaluate their necessity and sufficiency. Aim 3 seeks to determine if BF-PV neurons convey motivational salience

signals that guide attention allocation. This work will elucidate how long-range, cortex-projecting BF-PV neurons support sustained attention, distinguishing their contributions from known cholinergic effects. Defining the computations and connectivity underlying sustained attention will provide fundamental insights into basal forebrain circuits

for normal cognition. Illuminating this poorly understood pathway may also reveal new therapeutic targets for attention disorders and BF-related dementias like Alzheimer's and Parkinson's disease.

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Washington University

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