Error monitoring refers to the ability to monitor one's own task performance without explicit feedback. This ability is studied typically in two-alternative forced-choice (2AFC) paradigms. Recent research showed that humans can also keep track of the magnitude and direction of errors in different magnitude domains (e.g., numerosity, duration, length). Based on the evidence that suggests a shared mechanism for magnitude representations, we aimed to investigate whether metric error monitoring ability is commonly governed across different magnitude domains. Participants reproduced/estimated temporal, numerical, and spatial magnitudes after which they rated their confidence regarding first order task performance and judged the direction of their reproduction/estimation errors. Participants were also tested in a 2AFC perceptual decision task and provided confidence ratings regarding their decisions. Results showed that variability in reproductions/estimations and metric error monitoring ability, as measured by combining confidence and error direction judgements, were positively related across temporal, spatial, and numerical domains. Metacognitive sensitivity in these metric domains was also positively associated with each other but not with metacognitive sensitivity in the 2AFC perceptual decision task. In conclusion, the current findings point at a general metric error monitoring ability that is shared across different metric domains with limited generalizability to perceptual decision-making.

When we remember a stimulus we rarely maintain a full fidelity representation of the observed item. Our working memory instead maintains a mixture of the observed feature values and categorical/gist information. I will discuss evidence from computational models supporting a mix of categorical and fine-detail information in working memory. Having established the need for two memory formats in working memory, I will discuss whether categorical and fine-detailed information for a stimulus are represented separately or as a single unified representation. Computational models of these two potential cognitive structures make differing predictions about the pattern of responses in visual working memory recall tests. The present study required participants to remember the orientation of stimuli for later reproduction. The pattern of responses are used to test the competing representational structures and to quantify the relative amount of fine-detailed and categorical information maintained. The effects of set size, encoding time, serial order, and response order on memory precision, categorical information, and guessing rates are also explored. (This is a 60 min talk).

For many animals, the sense of olfaction plays a major role in controlling sexual behaviors. Olfaction helps animals to detect mates, discriminate their status, and ultimately, decide on their behavioral output such as courtship behavior or aggression. Specific pheromone cues and receptors have provided a useful model to study how sensory inputs are converted into certain behavioral outputs. With the aid of recent advances in tools to record and manipulate genetically defined neurons, our understanding of the neural basis of sexual and social behavior has expanded substantially. I will discuss the current understanding of the neural processing of sex pheromones and the neural circuitry which controls sexual and social behaviors and ultimately reproduction, by focusing on rodent studies, mainly in mice, and the vomeronasal sensory system.

Animals possess the ability to effortlessly and precisely time their actions even though information received from the world is often ambiguous and is inadvertently transformed as it passes through the nervous system. With such uncertainty pervading through our nervous systems, we could expect that much of human and animal behavior relies on inference that incorporates an important additional source of information, prior knowledge of the environment. These concepts have long been studied under the framework of Bayesian inference with substantial corroboration over the last decade that human time perception is consistent with such models. We, however, know little about the neural mechanisms that enable Bayesian signatures to emerge in temporal perception. I will present our work on three facets of this problem, how Bayesian estimates are encoded in neural populations, how these estimates are used to generate time intervals, and how prior knowledge for these tasks is acquired and optimized by neural circuits. We trained monkeys to perform an interval reproduction task and found their behavior to be consistent with Bayesian inference. Using insights from electrophysiology and in silico models, we propose a mechanism by which cortical populations encode Bayesian estimates and utilize them to generate time intervals. Thereafter, I will present a circuit model for how temporal priors can be acquired by cerebellar machinery leading to estimates consistent with Bayesian theory. Based on electrophysiology and anatomy experiments in rodents, I will provide some support for this model. Overall, these findings attempt to bridge insights from normative frameworks of Bayesian inference with potential neural implementations for the acquisition, estimation, and production of timing behaviors.

According to the theory of predictive processing, expectations modulate neural activity so as to optimize the processing of sensory inputs expected in the current environment. While there is accumulating evidence that the brain indeed operates under this principle, most of the attention has been placed on mechanisms that rely on static coding properties of neurons. The potential contribution of dynamical features, such as those reflected in the evolution of neural population dynamics, has thus far been overlooked. In this talk, I will present evidence for a novel mechanism for predictive processing in the temporal domain which relies on neural population dynamics. I will use recordings from the frontal cortex of macaques trained on a time interval reproduction task and show how neural dynamics can be directly related to animals’ temporal expectations, both in a stationary environment and during learning.

Work in my laboratory is based on the assumptions that we do not know yet how all physiological functions are regulated and that mouse genetics by allowing to identify novel inter-organ communications is the most efficient ways to identify novel regulation of physiological functions. We test these two contention through the study of bone which is the organ my lab has studied since its inception. Based on precise cell biological and clinical reasons that will be presented during the seminar we hypothesized that bone should be a regulator of energy metabolism and reproduction and identified a bone-derived hormone termed osteocalcin that is responsible of these regulatory events. The study of this hormone revealed that in addition to its predicted functions it also regulates brain size, hippocampus development, prevents anxiety and depression and favors spatial learning and memory by signaling through a specific receptor we characterized. As will be presented, we elucidated some of the molecular events accounting for the influence of osteocalcin on brain and showed that maternal osteocalcin is the pool of this hormone that affects brain development. Subsequently and looking at all the physiological functions regulated by osteocalcin, i.e., memory, the ability to exercise, glucose metabolism, the regulation of testosterone biosynthesis, we realized that are all need or regulated in the case of danger. In other words it suggested that osteocalcin is an hormone needed to sense and overcome acute danger. Consonant with this hypothesis we next showed this led us to demonstrate that bone via osteocalcin is needed to mount an acute stress response through molecular and cellular mechanisms that will be presented during the seminar. overall, an evolutionary appraisal of bone biology, this body of work and experiments ongoing in the lab concur to suggest 1] the appearance of bone during evolution has changed how physiological functions as diverse as memory, the acute stress response but also exercise and glucose metabolism are regulated and 2] identified bone and osteocalcin as its molecular vector, as an organ needed to sense and response to danger.