Abstract

Sensory perception underlies how we internalize and interact with the external world. In order to adapt to changing circumstances and interpret signals in a variety of contexts, sensation needs to be reliable, but perception of sensory input needs to be flexible. An important mediator of this flexibility is top-down regulation from the cholinergic basal forebrain. Basal forebrain projection neurons serve as pacemakers and gatekeepers for downstream neural networks, modulating circuit activity across diverse neuronal populations. This top-down control is necessary for sensory cue detection, learning, and memory, and is disproportionately disrupted in neurodegenerative diseases associated with cognitive decline. Intriguingly, cholinergic signaling acts locally within the basal forebrain to sculpt the activity of basal forebrain output neurons. To determine how local cholinergic signaling impacts basal forebrain output pathways that participate in top-down regulation, we sought to define the dynamics of cholinergic signaling within the basal forebrain during motivated behavior and learning. Toward this, we utilized fiber photometry and the genetically encoded acetylcholine indicator GAChR2.0 to define temporal patterns of cholinergic signaling in the basal forebrain during olfactory-guided, motivated behaviors and learning. We show that cholinergic signaling reliably increased during reward seeking behaviors, but was strongly suppressed by reward delivery in a go/no-go olfactory-cued discrimination task. The observed transient reduction in cholinergic tone was mirrored by a suppression in basal forebrain GABAergic neuronal activity. Together, these findings suggest that cholinergic tone in the basal forebrain changes rapidly to reflect reward-seeking behavior and positive reinforcement and may impact downstream circuitry that modulates olfaction.

Highlights

  • Rapid and precise sensory processing is critical for properly interpreting the external world

  • In contrast to the cholinergic signal, aligning False Alarm and Hit trials to reward port entries revealed no initial decrease in False Alarm trials, but a large and sustained suppression in Hit trials (Figure 5H). Together these data raise the intriguing possibility that HDB acetylcholine levels decrease in anticipation of a reward, while HDB GABAergic neuronal activity is suppressed by the reinforcement itself

  • Having revealed dynamic cholinergic signaling in the HDB during olfactory-guided behavior, we examined a potential target of local cholinergic signaling

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Summary

INTRODUCTION

Rapid and precise sensory processing is critical for properly interpreting the external world. The cholinergic and GABAergic projections control gain, signal-to-noise ratio, habituation, oscillatory activity, and odor discrimination (Ma and Luo, 2012; Nunez-Parra et al, 2013; Rothermel et al, 2014; Ogg et al, 2018; Villar et al, 2020) Though both types of basal forebrain projections are important modulators of olfactory bulb odor and sniff responses, the upstream mechanisms that control basal forebrain output remain largely unknown. Reward seeking behavior reliably evoked rapid increases in HDB acetylcholine, while positive feedback transiently suppressed cholinergic tone These dynamics suggest that local cholinergic signaling is rapidly modulated in the HDB circuitry and may impact basal forebrain output pathways important for regulating olfaction

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