During the first reporting period we have established most of the new experimental systems outlined in the proposal, and they are all now being routinely used in our lab. First, we have established of a behavioural assay to evaluate taste-independent post-ingestive reinforcing effects of nutrients. Second, we have developed novel assays for non-invasive artificial stimulation of specific gut signals using optogenetics. Third, we examined the role of insular cortex activity in anticipatory physiological regulation. Fourth, we established two-photon holography for optogenetic activation of precise insular cortex activity patterns via a microprism.
In addition to these achievements, we sought to create a comprehensive analytical pipeline for detailed analyses of neuronal population activity patterns in insular cortex. To do so, we leveraged recent advances in unsupervised machine learning to study insular cortex population activity patterns (a.k.a. neuronal manifold) in mice performing goal-directed behaviours aimed to fulfil physiological needs. We found that the insular cortex activity manifold is remarkably consistent across different animals and under different physiological need states. Activity dynamics within the neuronal manifold were highly stereotyped during food or water rewards, enabling robust prediction of single-trial outcomes across different mice, and across various natural and artificial physiological needs. Comparing goal-directed behaviour with self-paced free consumption, we found that the stereotyped activity patterns reflect task-dependent goal-directed reward anticipation, and not licking, taste, or positive valence. These findings revealed a core computation in insular cortex that could explain its involvement in pathologies involving aberrant motivations. This work was recently published (Talpir and Livneh, Cell Reports, 2024).
