Cortical variations in cytoarchitecture form a sensory-fugal axis that shapes regional profiles of extrinsic connectivity and is thought to guide signal propagation and integration across the cortical hierarchy. While neuroimaging work has shown that this axis constrains local properties of the human connectome, it remains unclear whether it also shapes the asymmetric signaling that arises from higher-order topology. Here, we used network control theory to examine the amount of energy required to propagate dynamics across the sensory-fugal axis. Our results revealed an asymmetry in this energy, indicating that bottom-up transitions were easier to complete compared to top-down. Supporting analyses demonstrated that asymmetries were underpinned by a connectome topology that is wired to support efficient bottom-up signaling. Lastly, we found that asymmetries correlated with differences in communicability and intrinsic neuronal time scales and lessened throughout youth. Our results show that cortical variation in cytoarchitecture may guide the formation of macroscopic connectome topology.

The medial entorhinal cortex (MEC) hosts many of the brain’s circuit elements for spatial navigation and episodic memory, operations that require neural activity to be organized across long durations of experience. While location is known to be encoded by a plethora of spatially tuned cell types in this brain region, little is known about how the activity of entorhinal cells is tied together over time. Among the brain’s most powerful mechanisms for neural coordination are network oscillations, which dynamically synchronize neural activity across circuit elements. In MEC, theta and gamma oscillations provide temporal structure to the neural population activity at subsecond time scales. It remains an open question, however, whether similarly coordination occurs in MEC at behavioural time scales, in the second-to-minute regime. In this talk I will show that MEC activity can be organized into a minute-scale oscillation that entrains nearly the entire cell population, with periods ranging from 10 to 100 seconds. Throughout this ultraslow oscillation, neural activity progresses in periodic and stereotyped sequences. The oscillation sometimes advances uninterruptedly for tens of minutes, transcending epochs of locomotion and immobility. Similar oscillatory sequences were not observed in neighboring parasubiculum or in visual cortex. The ultraslow periodic sequences in MEC may have the potential to couple its neurons and circuits across extended time scales and to serve as a scaffold for processes that unfold at behavioural time scales.

Dopamine is a neuromodulator that codes information on various time scales. I will discuss recent progress on the identification of fast release mechanisms for dopamine in the mouse striatum. I will present data on triggering mechanisms of dopamine release and evaluate its roles in striatal regulation. In the long-term, our work will allow for a better understanding of the mechanisms and time scales of dopamine coding in health and disease.

Neurons in the brain communicate through action potentials (spikes) that are transmitted through chemical synapses. Throughout the last decades, the question how networks of spiking neurons represent and process information has remained an important challenge. Some progress has resulted from a recent family of supervised learning rules (tempotrons) for models of spiking neurons. However, these studies have viewed synaptic transmission as static and characterized synaptic efficacies as scalar quantities that change only on slow time scales of learning across trials but remain fixed on the fast time scales of information processing within a trial. By contrast, signal transduction at chemical synapses in the brain results from complex molecular interactions between multiple biochemical processes whose dynamics result in substantial short-term plasticity of most connections. Here we study the computational capabilities of spiking neurons whose synapses are dynamic and plastic, such that each individual synapse can learn its own dynamics. We derive tempotron learning rules for current-based leaky-integrate-and-fire neurons with different types of dynamic synapses. Introducing ordinal synapses whose efficacies depend only on the order of input spikes, we establish an upper capacity bound for spiking neurons with dynamic synapses. We compare this bound to independent synapses, static synapses and to the well established phenomenological Tsodyks-Markram model. We show that synaptic dynamics in principle allow the storage capacity of spiking neurons to scale with the number of input spikes and that this increase in capacity can be traded for greater robustness to input noise, such as spike time jitter. Our work highlights the feasibility of a novel computational paradigm for spiking neural circuits with plastic synaptic dynamics: Rather than being determined by the fixed number of afferents, the dimensionality of a neuron's decision space can be scaled flexibly through the number of input spikes emitted by its input layer.

Recent chronic imaging experiments in mice have revealed that the hippocampal code exhibits non-trivial turnover dynamics over long time scales. Specifically, the subset of cells which are active on any given session in a familiar environment changes over the course of days and weeks. While some cells transition into or out of the code after a few sessions, others are stable over the entire experiment. The mechanisms underlying this turnover are unknown. Here we show that the statistics of turnover are consistent with a model in which non-spatial inputs to CA1 pyramidal cells readily undergo plasticity, while spatially tuned inputs are largely stable over time. The heterogeneity in stability across the cell assembly, as well as the decrease in correlation of the population vector of activity over time, are both quantitatively fit by a simple model with Gaussian input statistics. In fact, such input statistics emerge naturally in a network of spiking neurons operating in the fluctuation-driven regime. This correspondence allows one to map the parameters of a large-scale spiking network model of CA1 onto the simple statistical model, and thereby fit the experimental data quantitatively. Importantly, we show that the observed drift is entirely consistent with random, ongoing synaptic turnover. This synaptic turnover is, in turn, consistent with Hebbian plasticity related to continuous learning in a fast memory system.

The neurobiology of decision-making is informed by neurons capable of representing information over time scales of seconds. Such neurons were initially characterized in studies of spatial working memory, motor planning (e.g., Richard Andersen lab) and spatial attention. For decision-making, such neurons emit graded spike rates, that represent the accumulated evidence for or against a choice. They establish the conduit between the formation of the decision and its completion, usually in the form of a commitment to an action, even if provisional. Indeed, many decisions appear to arise through an accumulation of noisy samples of evidence to a terminating threshold, or bound. Previous studies show that single neurons in the lateral intraparietal area (LIP) represent the accumulation of evidence when monkeys make decisions about the direction of random dot motion (RDM) and express their decision with a saccade to the neuron’s preferred target. The mechanism of termination (the bound) is elusive. LIP is interconnected with other brain regions that also display decision-related activity. Whether these areas play roles in the decision process that are similar to or fundamentally different from that of LIP is unclear. I will present new unpublished experiments that begin to resolve these issues by recording from populations of neurons simultaneously in LIP and one of its primary targets, the superior colliculus (SC), while monkeys make difficult perceptual decisions.

How can neural networks exhibit persistent activity on time scales much larger than allowed by cellular properties? We address this question in the context of larval zebrafish, a model vertebrate that is accessible to brain-scale neuronal recording and high-throughput behavioral studies. We study in particular the dynamics of a bilaterally distributed circuit, the so-called ARTR, including hundreds neurons. ARTR exhibits slow antiphasic alternations between its left and right subpopulations, which can be modulated by the water temperature, and drive the coordinated orientation of swim bouts, thus organizing the fish spatial exploration. To elucidate the mechanism leading to the slow self-oscillation, we train a network graphical model (Ising) on neural recordings. Sampling the inferred model allows us to generate synthetic oscillatory activity, whose features correctly capture the observed dynamics. A mean-field analysis of the inferred model reveals the existence several phases; activated crossing of the barriers in between those phases controls the long time scales present in the network oscillations. We show in particular how the barrier heights and the nature of the phases vary with the water temperature.