Neuronal Excitability in Memory Allocation: Mechanisms and Consequences

Throughout the brain, sparse ensembles of neurons, termed “engrams,” are responsible for representing events. Engrams are composed of neurons active at the time of an event, and recent research has revealed how these active neurons compete to gain inclusion into a subsequently formed engram. This competitive selection mechanism, called “memory allocation,” is the process by which individual neurons become components of the engram. Memory allocation is crucially influenced by neuronal excitability, with more highly excitable neurons outcompeting their neighbors for inclusion into the engram. The dynamics of this excitability-dependent memory allocation process have important consequences for the function of the memory circuit, including effects on memory generalization and linking of events experienced closely in time. Memory allocation arises from cellular mechanisms of excitability, governs circuit-level dynamics of the engram, and has higher-order consequences for memory system function.

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CCR5 closes the temporal window for memory linking

10.1101/2021.10.07.463602 ◽

2021 ◽

Author(s):

Yang Shen ◽

Miou Zhou ◽

Denise Cai ◽

Daniel Almeida Filho ◽

Giselle Fernandes ◽

...

Keyword(s):

Neuronal Excitability ◽

Memory Allocation ◽

Clinical Implications ◽

Ccr5 Expression ◽

Cellular Mechanisms ◽

Temporal Window ◽

Contextual Memory ◽

Age Related ◽

The Brain ◽

Related Increase

Real world memories are formed in a particular context and are not acquired or recalled in isolation. Time is a key variable in the organization of memories, since events experienced close in time are more likely to be meaningfully associated, while those experienced with a longer interval are not. How does the brain segregate events that are temporally distinct? Here, we report that a delayed (12-24h) increase in the expression of the C-C chemokine receptor type 5 (CCR5), an immune receptor well known as a co-receptor for HIV infection, following the formation of a contextual memory, determines the duration of the temporal window for associating or linking that memory with subsequent memories. This delayed CCR5 expression in mouse dorsal CA1 (dCA1) neurons results in a decrease in neuronal excitability, which in turn negatively regulates neuronal memory allocation, thus reducing the overlap between dCA1 memory ensembles. Lowering this overlap affects the ability of one memory to trigger the recall of the other, thus closing the temporal window for memory linking. Remarkably, our findings also show that an age-related increase in CCL5/CCR5 expression leads to impairments in memory linking in aged mice, which could be reversed with a CCR5 knockout and an FDA approved drug that inhibits this receptor, a result with significant clinical implications. All together the findings reported here provide the first insights into the molecular and cellular mechanisms that shape the temporal window for memory linking.

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Memory Allocation: Mechanisms and Function

Annual Review of Neuroscience ◽

10.1146/annurev-neuro-080317-061956 ◽

2018 ◽

Vol 41 (1) ◽

pp. 389-413 ◽

Cited By ~ 48

Author(s):

Sheena A. Josselyn ◽

Paul W. Frankland

Keyword(s):

Neuronal Excitability ◽

Memory Allocation ◽

Integration Process ◽

Neuronal Ensembles ◽

Memory Integration ◽

And Function ◽

The Brain

Memories for events are thought to be represented in sparse, distributed neuronal ensembles (or engrams). In this article, we review how neurons are chosen to become part of a particular engram, via a process of neuronal allocation. Experiments in rodents indicate that eligible neurons compete for allocation to a given engram, with more excitable neurons winning this competition. Moreover, fluctuations in neuronal excitability determine how engrams interact, promoting either memory integration (via coallocation to overlapping engrams) or separation (via disallocation to nonoverlapping engrams). In parallel with rodent studies, recent findings in humans verify the importance of this memory integration process for linking memories that occur close in time or share related content. A deeper understanding of allocation promises to provide insights into the logic underlying how knowledge is normally organized in the brain and the disorders in which this process has gone awry.

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Modeling temperature- and Cav3 subtype-dependent alterations in T-type calcium channel mediated burst firing

Molecular Brain ◽

10.1186/s13041-021-00813-7 ◽

2021 ◽

Vol 14 (1) ◽

Author(s):

Fernando R. Fernandez ◽

Mircea C. Iftinca ◽

Gerald W. Zamponi ◽

Ray W. Turner

Keyword(s):

Calcium Channel ◽

Neuronal Excitability ◽

Neuronal Firing ◽

Mammalian Brain ◽

Peripheral Tissues ◽

Window Current ◽

Modeling Data ◽

The Brain ◽

Firing Neuron ◽

Cav3 Channel

AbstractT-type calcium channels are important regulators of neuronal excitability. The mammalian brain expresses three T-type channel isoforms (Cav3.1, Cav3.2 and Cav3.3) with distinct biophysical properties that are critically regulated by temperature. Here, we test the effects of how temperature affects spike output in a reduced firing neuron model expressing specific Cav3 channel isoforms. The modeling data revealed only a minimal effect on baseline spontaneous firing near rest, but a dramatic increase in rebound burst discharge frequency for Cav3.1 compared to Cav3.2 or Cav3.3 due to differences in window current or activation/recovery time constants. The reduced response by Cav3.2 could optimize its activity where it is expressed in peripheral tissues more subject to temperature variations than Cav3.1 or Cav3.3 channels expressed prominently in the brain. These tests thus reveal that aspects of neuronal firing behavior are critically dependent on both temperature and T-type calcium channel subtype.

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A Destruction Model of the Vascular and Lymphatic Systems in the Emergence of Psychiatric Symptoms

Biology ◽

10.3390/biology10010034 ◽

2021 ◽

Vol 10 (1) ◽

pp. 34

Author(s):

Kohei Segawa ◽

Yukari Blumenthal ◽

Yuki Yamawaki ◽

Gen Ohtsuki

Keyword(s):

Neurodegenerative Diseases ◽

Lymphatic System ◽

Psychiatric Symptoms ◽

Neurological Diseases ◽

Immune Surveillance ◽

Brain Network ◽

Cellular Mechanisms ◽

Postmortem Brains ◽

New Interpretation ◽

The Brain

The lymphatic system is important for antigen presentation and immune surveillance. The lymphatic system in the brain was originally introduced by Giovanni Mascagni in 1787, while the rediscovery of it by Jonathan Kipnis and Kari Kustaa Alitalo now opens the door for a new interpretation of neurological diseases and therapeutic applications. The glymphatic system for the exchanges of cerebrospinal fluid (CSF) and interstitial fluid (ISF) is associated with the blood-brain barrier (BBB), which is involved in the maintenance of immune privilege and homeostasis in the brain. Recent notions from studies of postmortem brains and clinical studies of neurodegenerative diseases, infection, and cerebral hemorrhage, implied that the breakdown of those barrier systems and infiltration of activated immune cells disrupt the function of both neurons and glia in the parenchyma (e.g., modulation of neurophysiological properties and maturation of myelination), which causes the abnormality in the functional connectivity of the entire brain network. Due to the vulnerability, such dysfunction may occur in developing brains as well as in senile or neurodegenerative diseases and may raise the risk of emergence of psychosis symptoms. Here, we introduce this hypothesis with a series of studies and cellular mechanisms.

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The Memory System of the Brain

The Computer Journal ◽

10.1093/comjnl/10.2.187 ◽

1967 ◽

Vol 10 (2) ◽

pp. 187-187

Keyword(s):

Memory System ◽

The Brain

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The novel guanylyl cyclase MsGC-I is strongly expressed in higher-order neuropils in the brain of Manduca sexta

Journal of Experimental Biology ◽

10.1242/jeb.204.2.305 ◽

2001 ◽

Vol 204 (2) ◽

pp. 305-314 ◽

Cited By ~ 1

Author(s):

A. Nighorn ◽

P.J. Simpson ◽

D.B. Morton

Keyword(s):

Nervous System ◽

Manduca Sexta ◽

Guanylyl Cyclase ◽

Higher Order ◽

Adult Brain ◽

Central Complex ◽

Amino Acid Residues ◽

Order Processing ◽

Guanylyl Cyclases ◽

The Brain

Guanylyl cyclases are usually characterized as being either soluble (sGCs) or receptor (rGCs). We have recently cloned a novel guanylyl cyclase, MsGC-I, from the developing nervous system of the hawkmoth Manduca sexta that cannot be classified as either an sGC or an rGC. MsGC-I shows highest sequence identity with receptor guanylyl cyclases throughout its catalytic and dimerization domains, but does not contain the ligand-binding, transmembrane or kinase-like domains characteristic of receptor guanylyl cyclases. In addition, MsGC-I contains a C-terminal extension of 149 amino acid residues. In this paper, we report the expression of MsGC-I in the adult. Northern blots show that it is expressed preferentially in the nervous system, with high levels in the pharate adult brain and antennae. In the antennae, immunohistochemical analyses show that it is expressed in the cell bodies and dendrites, but not axons, of olfactory receptor neurons. In the brain, it is expressed in a variety of sensory neuropils including the antennal and optic lobes. It is also expressed in structures involved in higher-order processing including the mushroom bodies and central complex. This complicated expression pattern suggests that this novel guanylyl cyclase plays an important role in mediating cyclic GMP levels in the nervous system of Manduca sexta.

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Defective actin dynamics in dendritic spines: cause or consequence of age-induced cognitive decline?

Biological Chemistry ◽

10.1515/hsz-2015-0185 ◽

2016 ◽

Vol 397 (3) ◽

pp. 223-229 ◽

Cited By ~ 3

Author(s):

Till Georg Alexander Mack ◽

Patricia Kreis ◽

Britta Johanna Eickholt

Keyword(s):

Dendritic Spines ◽

Neuronal Excitability ◽

Replicative Senescence ◽

Morphological Changes ◽

Actin Dynamics ◽

Cellular Processes ◽

Filament Dynamics ◽

Neuronal Soma ◽

Deteriorating Process ◽

The Brain

Abstract Ageing is a complex deteriorating process that coincides with changes in metabolism, replicative senescence, increased resistance to apoptosis, as well as progressive mitochondria dysfunction that lead to an increase production and accumulation of reactive oxygen species (ROS). Although controversy on the paradigm of the oxidative damage theory of ageing exists, persuasive studies in Caenorhabditis elegans and yeast have demonstrated that manipulation of ROS can modify the process of ageing and influences the damage of proteins, lipids and DNA. In neurons, ageing impacts on the intrinsic neuronal excitability, it decreases the size of neuronal soma and induces the loss of dendrites and dendritic spines. The actin cytoskeleton is an abundant and broadly expressed system that plays critical functions in many cellular processes ranging from cell motility to controlling cell shape and polarity. It is thus hardly surprising that the expression and the function of actin in neurons is crucial for the morphological changes that occur in the brain throughout life. We propose that alterations in actin filament dynamics in dendritic spines may be one of the key events contributing to the initial phases of ageing in the brain.

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Evolutionary modifications in human brain connectivity associated with schizophrenia

Brain ◽

10.1093/brain/awz330 ◽

2019 ◽

Vol 142 (12) ◽

pp. 3991-4002 ◽

Cited By ~ 13

Author(s):

Martijn P van den Heuvel ◽

Lianne H Scholtens ◽

Siemon C de Lange ◽

Rory Pijnenburg ◽

Wiepke Cahn ◽

...

Keyword(s):

Human Brain ◽

Brain Connectivity ◽

Brain Evolution ◽

Higher Order ◽

Brain Functions ◽

Human Brain Evolution ◽

The Brain

See Vértes and Seidlitz (doi:10.1093/brain/awz353) for a scientific commentary on this article. Is schizophrenia a by-product of human brain evolution? By comparing the human and chimpanzee connectomes, van den Heuvel et al. demonstrate that connections unique to the human brain show greater involvement in schizophrenia pathology. Modifications in service of higher-order brain functions may have rendered the brain more vulnerable to dysfunction.

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Entry of antiepileptic drugs (valproate and lamotrigine) into the developing rat brain

F1000Research ◽

10.12688/f1000research.52607.1 ◽

2021 ◽

Vol 10 ◽

pp. 384

Author(s):

Samuel J. Toll ◽

Fiona Qiu ◽

Yifan Huang ◽

Mark D. Habgood ◽

Katarzyna M. Dziegielewska ◽

...

Keyword(s):

Antiepileptic Drug ◽

Placental Transfer ◽

Rat Plasma ◽

Developing Brain ◽

Adult Brain ◽

Cellular Mechanisms ◽

Antiepileptic Drug Treatment ◽

Dose Dependent ◽

The Brain ◽

Drug Entry

Background: Women with epilepsy face difficult choices whether to continue antiepileptic drug treatment during pregnancy, as uncontrolled seizures carry great risk to mother and fetus but continuing treatment may have adverse effects on baby’s development. This study aimed at evaluating antiepileptic drug entry into developing brain. Methods: Anaesthetised pregnant, non-pregnant adult females, postnatal and fetal rats were injected intraperitoneally with different doses, single or in combinations, of valproate and lamotrigine, all within clinical range. Injectate included 3H-labelled drug. After 30min, CSF, blood and brain samples were obtained; radioactivity was measured using liquid scintillation counting. Some animals were also exposed to valproate in feed throughout pregnancy and into neonatal period. Drug levels were measured by liquid chromatography coupled to mass spectrometry (LC-MS). Results are given as CSF or tissue/plasma% as index of drug entry. Results: Entry of valproate into brain and CSF was higher at E19 and P4 compared to adult but was not dose-dependent; placental transfer increased significantly at highest dose of 100mg/Kg. Lamotrigine entry into the brain was dose dependent only at E19. Chronic valproate treatment, or combination of valproate and lamotrigine had little effect on either drug entry, except for reduced valproate brain entry in adult brain with chronic treatment. Placental transfer decreased significantly after chronic valproate treatment. LC-MS measurement of valproate in adults confirmed that rat plasma values were within the clinical range and CSF/plasma and brain/plasma ratios for LC-MS and 3H-valproate were similar. Conclusion: Results suggest that entry of valproate may be higher in developing brain, the capacity of barrier mechanism is mostly unaffected by doses within the clinical range, with or without addition of lamotrigine. Chronic valproate exposure may result in upregulation in cellular mechanisms restricting its entry into the brain. Entry of lamotrigine was little different at different ages and was not dose dependent.

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The role of thickness inhomogeneities in hierarchical cortical folding

10.1101/2020.04.01.020172 ◽

2020 ◽

Cited By ~ 1

Author(s):

Lucas da Costa Campos ◽

Raphael Hornung ◽

Gerhard Gompper ◽

Jens Elgeti ◽

Svenja Caspers

Keyword(s):

Fetal Brain ◽

Epileptic Seizures ◽

Quantitative Model ◽

Higher Order ◽

Mammalian Brain ◽

Cortical Folding ◽

Differential Growth ◽

The Brain ◽

Short Life Expectancy

AbstractThe morphology of the mammalian brain cortex is highly folded. For long it has been known that specific patterns of folding are necessary for an optimally functioning brain. On the extremes, lissencephaly, a lack of folds in humans, and polymicrogyria, an overly folded brain, can lead to severe mental retardation, short life expectancy, epileptic seizures, and tetraplegia. The construction of a quantitative model on how and why these folds appear during the development of the brain is the first step in understanding the cause of these conditions. In recent years, there have been various attempts to understand and model the mechanisms of brain folding. Previous works have shown that mechanical instabilities play a crucial role in the formation of brain folds, and that the geometry of the fetal brain is one of the main factors in dictating the folding characteristics. However, modeling higher-order folding, one of the main characteristics of the highly gyrencephalic brain, has not been fully tackled. The effects of thickness inhomogeneity in the gyrogenesis of the mammalian brain are studied in silico. Finite-element simulations of rectangular slabs are performed. The slabs are divided into two distinct regions, where the outer layer mimics the gray matter, and the inner layer the underlying white matter. Differential growth is introduced by growing the top layer tangentially, while keeping the underlying layer untouched. The brain tissue is modeled as a neo-Hookean hyperelastic material. Simulations are performed with both, homogeneous and inhomogeneous cortical thickness. The homogeneous cortex is shown to fold into a single wavelength, as is common for bilayered materials, while the inhomogeneous cortex folds into more complex conformations. In the early stages of development of the inhomogeneous cortex, structures reminiscent of the deep sulci in the brain are obtained. As the cortex continues to develop, secondary undulations, which are shallower and more variable than the structures obtained in earlier gyrification stage emerge, reproducing well-known characteristics of higher-order folding in the mammalian, and particularly the human, brain.

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