Transcriptomics has revealed that cortical inhibitory neurons exhibit a great diversity of fine molecular subtypes, but it is not known whether these subtypes have correspondingly diverse activity patterns in the living brain. We show that inhibitory subtypes in primary visual cortex (V1) have diverse correlates with brain state, but that this diversity is organized by a single factor: position along their main axis of transcriptomic variation. We combined in vivo 2-photon calcium imaging of mouse V1 with a novel transcriptomic method to identify mRNAs for 72 selected genes in ex vivo slices. We classified inhibitory neurons imaged in layers 1-3 into a three-level hierarchy of 5 Subclasses, 11 Types, and 35 Subtypes using previously-defined transcriptomic clusters. Responses to visual stimuli differed significantly only across Subclasses, suppressing cells in the Sncg Subclass while driving cells in the other Subclasses. Modulation by brain state differed at all hierarchical levels but could be largely predicted from the first transcriptomic principal component, which also predicted correlations with simultaneously recorded cells. Inhibitory Subtypes that fired more in resting, oscillatory brain states have less axon in layer 1, narrower spikes, lower input resistance and weaker adaptation as determined in vitro and express more inhibitory cholinergic receptors. Subtypes firing more during arousal had the opposite properties. Thus, a simple principle may largely explain how diverse inhibitory V1 Subtypes shape state-dependent cortical processing.

SeminarNeuroscience

Neuromodulation of sleep integrity

Luís de Lecea

Stanford University

Apr 12, 2022

The arousal construct underlies a spectrum of behaviors that include sleep, exploration, feeding, sexual activity and adaptive stress. Pathological arousal conditions include stress, anxiety disorders, and addiction. The dynamics between arousal state transitions are modulated by norepinephrine neurons in the locus coeruleus, histaminergic neurons in the hypothalamus, dopaminergic neurons in the mesencephalon and cholinergic neurons in the basal forebrain. The hypocretin/orexin system in the lateral hypothalamus I will also present a new mechanism underlying sleep fragmentation during aging. Hcrt neurons are hyperexcitable in aged mice. We identify a potassium conductance known as the M-current, as a critical player in maintaining excitability of Hcrt neurons. Genetic disruption of KCNQ channels in Hcrt neurons of young animals results in sleep fragmentation. In contrast, treatment of aged animals with a KCNQ channel opener restores sleep/wake architecture. These data point to multiple circuits modulating sleep integrity across lifespan.

SeminarNeuroscienceRecording

Disinhibitory and neuromodulatory regulation of hippocampal synaptic plasticity

Inês Guerreiro

Gutkin lab, Ecole Normale Superieure

Jul 28, 2021

The CA1 pyramidal neurons are embedded in an intricate local circuitry that contains a variety of interneurons. The roles these interneurons play in the regulation of the excitatory synaptic plasticity remains largely understudied. Recent experiments showed that repeated cholinergic activation of 𝛼7 nACh receptors expressed in oriens-lacunosum-moleculare (OLM𝛼2) interneurons could induce LTP in SC-CA1 synapses. We used a biophysically realistic computational model to examine mechanistically how cholinergic activation of OLMa2 interneurons increases SC to CA1 transmission. Our results suggest that, when properly timed, activation of OLMa2 interneurons cancels the feedforward inhibition onto CA1 pyramidal cells by inhibiting fast-spiking interneurons that synapse on the same dendritic compartment as the SC, i.e., by disinhibiting the pyramidal cell dendritic compartment. Our work further describes the pairing of disinhibition with SC stimulation as a general mechanism for the induction of synaptic plasticity. We found that locally-reduced GABA release (disinhibition) paired with SC stimulation could lead to increased NMDAR activation and intracellular calcium concentration sufficient to upregulate AMPAR permeability and potentiate the excitatory synapse. Our work suggests that inhibitory synapses critically modulate excitatory neurotransmission and induction of plasticity at excitatory synapses. Our work also shows how cholinergic action on OLM interneurons, a mechanism whose disruption is associated with memory impairment, can down-regulate the GABAergic signaling into CA1 pyramidal cells and facilitate potentiation of the SC-CA1 synapse.

SeminarNeuroscienceRecording

Cholinergic modulation of the cerebellum

Jasmine Pickford

Apps lab, University of Bristol

Jul 14, 2021

Many studies have investigated the major glutamatergic inputs to the cerebellum, mossy fibres and climbing fibres, however far less is known about its neuromodulatory inputs. In particular, anatomical studies have described cholinergic input to the cerebellum, yet little is known about its role(s). In this talk, I will present our recent findings which demonstrate that manipulating acetylcholine receptors in the cerebellum causes effects at both a cellular and behavioural level. Activating acetylcholine receptors alters the intrinsic properties and synaptic inputs of cerebellar output neurons, and blocking these receptors results in deficits in a range of behavioural tasks.

SeminarNeuroscienceRecording

An in-silico framework to study the cholinergic modulation of the neocortex

Cristina Colangelo

EPFL, Blue Brain Project

Jun 30, 2021

Neuromodulators control information processing in cortical microcircuits by regulating the cellular and synaptic physiology of neurons. Computational models and detailed simulations of neocortical microcircuitry offer a unifying framework to analyze the role of neuromodulators on network activity. In the present study, to get a deeper insight in the organization of the cortical neuropil for modeling purposes, we quantify the fiber length per cortical volume and the density of varicosities for catecholaminergic, serotonergic and cholinergic systems using immunocytochemical staining and stereological techniques. The data obtained are integrated into a biologically detailed digital reconstruction of the rodent neocortex (Markram et al, 2015) in order to model the influence of modulatory systems on the activity of the somatosensory cortex neocortical column. Simulations of ascending modulation of network activity in our model predict the effects of increasing levels of neuromodulators on diverse neuron types and synapses and reveal a spectrum of activity states. Low levels of neuromodulation drive microcircuit activity into slow oscillations and network synchrony, whereas high neuromodulator concentrations govern fast oscillations and network asynchrony. The models and simulations thus provide a unifying in silico framework to study the role of neuromodulators in reconfiguring network activity.

SeminarNeuroscienceRecording

Effects of Vagus Nerve Stimulation on Arousal State and Cortical Excitation

Lindsay Collins

McCormick Lab, University of Oregon

Jun 30, 2021

The vagus nerve is a major pathway by which the brain and the body communicate. Electrical stimulation of the vagus nerve (VNS) is widely used as a therapeutic intervention for epilepsy and there is compelling evidence that it can enhance recovery following stroke. Our work demonstrates that VNS exerts a robust excitatory effect on the brain. First, we establish that VNS triggers an increase in arousal state as measured by behavioral state change. This behavioral state change is linked to an increase in excitatory activity within the cortex. We also show that cholinergic and noradrenergic neuromodulatory pathways are activated by VNS, providing a potential mechanism by which VNS may trigger cortical activation. Importantly, the effect of VNS on neuromodulation and cortical excitation persists in anesthetized mice, demonstrating that VNS-induced cortical activation cannot be fully explained by associated behavioral changes.

SeminarNeuroscience

State-dependent cortical circuits

Jess Cardin

Yale School of Medicine

May 14, 2021

Spontaneous and sensory-evoked cortical activity is highly state-dependent, promoting the functional flexibility of cortical circuits underlying perception and cognition. Using neural recordings in combination with behavioral state monitoring, we find that arousal and motor activity have complementary roles in regulating local cortical operations, providing dynamic control of sensory encoding. These changes in encoding are linked to altered performance on perceptual tasks. Neuromodulators, such as acetylcholine, may regulate this state-dependent flexibility of cortical network function. We therefore recently developed an approach for dual mesoscopic imaging of acetylcholine release and neural activity across the entire cortical mantle in behaving mice. We find spatiotemporally heterogeneous patterns of cholinergic signaling across the cortex. Transitions between distinct behavioral states reorganize the structure of large-scale cortico-cortical networks and differentially regulate the relationship between cholinergic signals and neural activity. Together, our findings suggest dynamic state-dependent regulation of cortical network operations at the levels of both local and large-scale circuits. Zoom Meeting ID: 964 8138 3003 Contact host if you cannot connect.

SeminarNeuroscience

State-dependent cortical circuits

Jessica Cardin

Yale School of Medicine

Jan 18, 2021

SeminarNeuroscienceRecording

Synapse-specific direction selectivity in retinal bipolar cell axon terminals

Keisuke Yonehara

Aarhus University

Nov 16, 2020

The ability to encode the direction of image motion is fundamental to our sense of vision. Direction selectivity along the four cardinal directions is thought to originate in direction-selective ganglion cells (DSGCs), due to directionally-tuned GABAergic suppression by starburst cells. Here, by utilizing two-photon glutamate imaging to measure synaptic release, we reveal that direction selectivity along all four directions arises earlier than expected, at bipolar cell outputs. Thus, DSGCs receive directionally-aligned glutamatergic inputs from bipolar cell boutons. We further show that this bouton-specific tuning relies on cholinergic excitation and GABAergic inhibition from starburst cells. In this way, starburst cells are able to refine directional tuning in the excitatory visual pathway by modulating the activity of DSGC dendrites and their axonal inputs using two different neurotransmitters.

SeminarNeuroscienceRecording

State-dependent regulation of cortical circuits

Jessica Cardin

Yale School of Medicine

Nov 11, 2020

SeminarNeuroscienceRecording

When spontaneous waves meet angiogenesis: a case study from the neonatal retina

Evelyne Sernagor

Newcastle University

Oct 12, 2020

By continuously producing electrical signals, neurones are amongst the most energy-demanding cells in the organism. Resting ionic levels are restored via metabolic pumps that receive the necessary energy from oxygen supplied by blood vessels. Intense spontaneous neural activity is omnipresent in the developing CNS. It occurs during short, well-defined periods that coincide precisely with the timing of angiogenesis. Such coincidence cannot be random; there must be a universal mechanism triggering spontaneous activity concurrently with blood vessels invading neural territories for the first time. However, surprisingly little is known about the role of neural activity per se in guiding angiogenesis. Part of the reason is that it is challenging to study developing neurovascular networks in tri-dimensional space in the brain. We investigate these questions in the neonatal mouse retina, where blood vessels are much easier to visualise because they initially grow in a plane, while waves of spontaneous neural activity (spreading via cholinergic starburst amacrine cells) sweep across the retinal ganglion cell layer, in close juxtaposition with the growing vasculature. Blood vessels reach the periphery by postnatal day (P) 7-8, shortly before the cholinergic waves disappear (at P10). We discovered transient clusters of auto-fluorescent cells that form an annulus around the optic disc, gradually expanding to the periphery, which they reach at the same time as the growing blood vessels. Remarkably, these cells appear locked to the frontline of the growing vasculature. Moreover, by recording waves with a large-scale multielectrode array that enables us to visualise them at pan-retinal level, we found that their initiation points are not random; they follow a developmental centre-to-periphery pattern similar to the clusters and blood vessels. The density of growing blood vessels is higher in cluster areas than in-between clusters at matching eccentricity. The cluster cells appear to be phagocytosed by microglia. Blocking Pannexin1 (PANX1) hemichannels activity with probenecid completely blocks the spontaneous waves and results in the disappearance of the fluorescent cell clusters. We suggest that these transient cells are specialised, hyperactive neurones that form spontaneous activity hotspots, thereby triggering retinal waves through the release of ATP via PANX1 hemichannels. These activity hotspots attract new blood vessels to enhance local oxygen supply. Signalling through PANX1 attracts microglia that establish contact with these cells, eventually eliminating them once blood vessels have reached their vicinity. The auto-fluorescence that characterises the cell clusters may develop only once the process of microglial phagocytosis is initiated.

SeminarNeuroscience

Rapid State Changes Account for Apparent Brain and Behavior Variability

David McCormick

University of Oregon

Sep 17, 2020

Neural and behavioral responses to sensory stimuli are notoriously variable from trial to trial. Does this mean the brain is inherently noisy or that we don’t completely understand the nature of the brain and behavior? Here we monitor the state of activity of the animal through videography of the face, including pupil and whisker movements, as well as walking, while also monitoring the ability of the animal to perform a difficult auditory or visual task. We find that the state of the animal is continuously changing and is never stable. The animal is constantly becoming more or less activated (aroused) on a second and subsecond scale. These changes in state are reflected in all of the neural systems we have measured, including cortical, thalamic, and neuromodulatory activity. Rapid changes in cortical activity are highly correlated with changes in neural responses to sensory stimuli and the ability of the animal to perform auditory or visual detection tasks. On the intracellular level, these changes in forebrain activity are associated with large changes in neuronal membrane potential and the nature of network activity (e.g. from slow rhythm generation to sustained activation and depolarization). Monitoring cholinergic and noradrenergic axonal activity reveals widespread correlations across the cortex. However, we suggest that a significant component of these rapid state changes arise from glutamatergic pathways (e.g. corticocortical or thalamocortical), owing to their rapidity. Understanding the neural mechanisms of state-dependent variations in brain and behavior promises to significantly “denoise” our understanding of the brain.

SeminarNeuroscienceRecording

On the purpose and origin of spontaneous neural activity

Tim Vogels

IST Austria

Sep 4, 2020

Spontaneous firing, observed in many neurons, is often attributed to ion channel or network level noise. Cortical cells during slow wave sleep exhibit transitions between so called Up and Down states. In this sleep state, with limited sensory stimuli, neurons fire in the Up state. Spontaneous firing is also observed in slices of cholinergic interneurons, cerebellar Purkinje cells and even brainstem inspiratory neurons. In such in vitro preparations, where the functional relevance is long lost, neurons continue to display a rich repertoire of firing properties. It is perplexing that these neurons, instead of saving their energy during information downtime and functional irrelevance, are eager to fire. We propose that spontaneous firing is not a chance event but instead, a vital activity for the well-being of a neuron. We postulate that neurons, in anticipation of synaptic inputs, keep their ATP levels at maximum. As recovery from inputs requires most of the energy resources, neurons are ATP surplus and ADP scarce during synaptic quiescence. With ADP as the rate-limiting step, ATP production stalls in the mitochondria when ADP is low. This leads to toxic Reactive Oxygen Species (ROS) formation, which are known to disrupt many cellular processes. We hypothesize that spontaneous firing occurs at these conditions - as a release valve to spend energy and to restore ATP production, shielding the neuron against ROS. By linking a mitochondrial metabolism model to a conductance-based neuron model, we show that spontaneous firing depends on baseline ATP usage and on ATP-cost-per-spike. From our model, emerges a mitochondrial mediated homeostatic mechanism that provides a recipe for different firing patterns. Our findings, though mostly affecting intracellular dynamics, may have large knock-on effects on the nature of neural coding. Hitherto it has been thought that the neural code is optimised for energy minimisation, but this may be true only when neurons do not experience synaptic quiescence.

SeminarNeuroscience

Cholinergic regulation of learning in the olfactory system

Christiane Linster

Cornell University

Jul 9, 2020

In the olfactory system, cholinergic modulation has been associated with contrast modulation and changes in receptive fields in the olfactory bulb, as well the learning of odor associations in the olfactory cortex. Computational modeling and behavioral studies suggest that cholinergic modulation could improve sensory processing and learning while preventing pro-active interference when task demands are high. However, how sensory inputs and/or learning regulate incoming modulation has not yet been elucidated. We here use a computational model of the olfactory bulb, piriform cortex (PC) and horizontal limb of the diagonal band of Broca (HDB) to explore how olfactory learning could regulate cholinergic inputs to the system in a closed feedback loop. In our model, the novelty of an odor is reflected in firing rates and sparseness of cortical neurons in response to that odor and these firing rates can directly regulate learning in the system by modifying cholinergic inputs to the system.

cholinergic

Latest

Cholinergic Interneurons

Immature brain insults and possible effects on cholinergic system neuroplasticity

A transcriptomic axis predicts state modulation of cortical interneurons

Neuromodulation of sleep integrity

Disinhibitory and neuromodulatory regulation of hippocampal synaptic plasticity

Cholinergic modulation of the cerebellum

An in-silico framework to study the cholinergic modulation of the neocortex

Effects of Vagus Nerve Stimulation on Arousal State and Cortical Excitation

State-dependent cortical circuits

State-dependent cortical circuits

Synapse-specific direction selectivity in retinal bipolar cell axon terminals

State-dependent regulation of cortical circuits

When spontaneous waves meet angiogenesis: a case study from the neonatal retina

Rapid State Changes Account for Apparent Brain and Behavior Variability

On the purpose and origin of spontaneous neural activity

Cholinergic regulation of learning in the olfactory system

CHOLINERGIC MUSCARINIC MODULATION OF DOPAMINE RELEASE DYNAMICS IN DRUG-SENSITIZED MICE

SYNERGY AND ANTAGONISM OF THE CHOLINERGIC AND DOPAMINERGIC SYSTEMS DURING ASSOCIATIVE LEARNING

VITAMIN A STATUS MODULATES NEURODEVELOPMENTAL, OXIDATIVE, AND CHOLINERGIC ALTERATIONS IN A VALPROIC ACID–INDUCED RAT MODEL OF AUTISM

CONSTRUCTION OF HUMAN CHOLINERGIC PROJECTIONS IN NBM-CORTICAL ASSEMBLOIDS REVEAL PROJECTIVE DEFECTS IN DOWN SYNDROME

SEROTONIN AND SEROTONERGIC INPUTS MODULATE CHOLINERGIC INTERNEURONS IN THE STRIATUM ON DIFFERENT TIMESCALES

CHOLINERGIC MODULATION OF DENTATE GYRUS CIRCUITS SUPPORTS LEARNING AND SYNAPTIC PLASTICITY

ACTIVATION OF PROTEIN KINASE CΑ IN STRIATAL CHOLINERGIC INTERNEURONS DURING EARLY PHASES OF REVERSAL LEARNING

THE CHOLINERGIC TAN SYSTEM IN DISTINCT REGIONS OF THE PRIMATE DORSAL STRIATUM MAKES DIFFERENT CONTRIBUTIONS TO FLEXIBLE SWITCHING BETWEEN TWO STIMULUS–RESPONSE RULES

CELL-TYPE-SPECIFIC ALTERATIONS IN HIPPOCAMPAL CHOLINERGIC SIGNALING IN APOE4 MICE

IDENTIFICATION OF MOLECULAR PARTNERS INVOLVED IN ACETYLCHOLINE/GLUTAMATE COTRANSMISSION WITHIN SYNAPTIC VESICLES OF STRIATAL CHOLINERGIC INTERNEURONS

UNVEILING AN ENDOGENOUS SOURCE OF CHOLINERGIC TRANSMISSION IN THE LATERAL HABENULA

EFFECTS OF SELECTIVE STIMULATION OF MEDIAL SEPTAL CHOLINERGIC NEURONS ON ALZHEIMER’S DISEASE PATHOLOGY IN A TRANSGENIC MOUSE MODEL

SPATIOTEMPORAL ORGANIZATION OF CHOLINERGIC INPUT IN THE SOMATOSENSORY CORTEX DURING TACTILE DETECTION

MODULATION OF CHOLINERGIC SIGNAL TRANSMISSION BY REELIN: NOVEL APPROACHES TO NEURODEGENERATIVE DISEASES

CHOLINERGIC AND OXYTOCINERGIC NEUROMODULATION IN THE DEVELOPING HIPPOCAMPUS

LATERAL SEPTAL CHOLINERGIC NEURONS REPRESENT AVERSIVE STIMULI AND MEDIATE AVOIDANCE BEHAVIOR

LATE-ONSET CHRONIC ALCOHOL CONSUMPTION EFFECTS ON THE TOTAL NUMBER OF CHOLINERGIC NEURONS OF THE LATERODORSAL TEGMENTAL NUCLEUS OF THE RAT: AN UNBIASED STEREOLOGICAL STUDY

CHOLINERGIC MODULATION OF NETWORK DYNAMICS MEDIATES SWITCHING BETWEEN MEMORY ACTIVATION AND REACTIVATION MODES DURING DIFFERENT VIGILANCE STATES AND SUPPORTS FORMATION OF COMPLEX MEMORY REPRESENTATIONS

DOMAIN-SPECIFIC CHOLINERGIC MODULATION OF COGNITIVE FUNCTIONS IN A PRIMATE TEST BATTERY

CHOLINERGIC MODULATION PRESERVES PERINEURONAL NET ORGANIZATION IN THE ADULT MOUSE VISUAL CORTEX AFTER RETINAL INJURY

Rapid Modulation of Cholinergic Interneurons and Dopamine Release by Satellite Astrocytes

Social deficiency and alterations of cholinergic activity in the medial prefrontal cortex in adult rat prenatally exposed to valproic acid

Striatal cholinergic interneurons control nicotine withdrawal via muscarinic signaling

Striatal cholinergic interneurons dysfunction as a substrate for stereotypies in autism spectrum disorder

Targeting cholinergic basal forebrain neurons to modulate inflammatory pain in mice

Target-specific control of olfactory bulb periglomerular cells by GABAergic and cholinergic basal forebrain inputs

In vivo examination of age-dependent changes in the activity of basal forebrain cholinergic neurons during a Pavlovian conditioning task

Anatomical, electrophysiological, and functional characterization of lateral septal cholinergic neurons

The basal forebrain cholinergic system linking olfaction and cognitive function: From basic studies to clinical application

Caffeic acid attenuates neuroinflammation and cognitive impairment in streptozotocin-induced diabetic rats: Pivotal role of the cholinergic and purinergic signaling pathways

Changes in striatal spiny projection neurons’ properties and circuitry in a mouse model of autism spectrum disorder with cholinergic interneuron dysfunction

Cholinergic-dependent slow-wave oscillations in the claustro-cortical networks in vitro

Cholinergic heterogeneity in synchronous and asynchronous states in a whole brain model

LDT cholinergic inputs to the nucleus accumbens neurons facilitate cocaine reinforcing properties

Cholinergic modulation of anti-correlated activity in the aversive brain

Cholinergic modulation of attentional performance on a signal detection task: Pharmacological modulation of nicotinic and muscarinic receptors

Cholinergic neuromodulation of processing sensory and reinforcement signals

Cholinergic regulation of dendritic Ca2+ spikes controls firing mode of hippocampal CA3 pyramidal neurons

Cholinergic regulation of heart employs two cholinesterases with distinct localization and functions

Cholinergic system and amyloid beta (Aβ) interplay at tripartite glutamatergic synapses in an alternative mouse model of Alzheimer’s disease