Computing and Stability in Cortical Networks

Cortical neurons are predominantly excitatory and highly interconnected. In spite of this, the cortex is remarkably stable: normal brains do not exhibit the kind of runaway excitation one might expect of such a system. How does the cortex maintain stability in the face of this massive excitatory feedback? More importantly, how does it do so during computations, which necessarily involve elevated firing rates? Here we address these questions in the context of attractor networks—networks that exhibit multiple stable states, or memories. We find that such networks can be stabilized at the relatively low firing rates observed in vivo if two conditions are met: (1) the background state, where all neurons are firing at low rates, is inhibition dominated, and (2) the fraction of neurons involved in a memory is above some threshold, so that there is sufficient coupling between the memory neurons and the background. This allows “dynamical stabilization” of the attractors, meaning feedback from the pool of background neurons stabilizes what would otherwise be an unstable state. We suggest that dynamical stabilization may be a strategy used for a broad range of computations, not just those involving attractors.

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Does actin produce the force that moves a chromosome to the pole during anaphase?

Canadian Journal of Biochemistry and Cell Biology ◽

10.1139/o85-077 ◽

1985 ◽

Vol 63 (6) ◽

pp. 585-598 ◽

Cited By ~ 20

Author(s):

Arthur Forer

Keyword(s):

Spindle Fibre ◽

Apparent Contradiction ◽

Spindle Poles ◽

Ultraviolet Microbeam ◽

The Face ◽

Spindle Fibres ◽

Rule Out ◽

Do So

Chromosomes move towards spindle poles because of force produced by chromosomal spindle fibres. I argue that actin is involved in producing this force. Actin is present in chromosomal spindle fibres, with consistent polarity. Physiological experiments using ultraviolet microbeam irradiations suggest that the force is due to an actin and myosin (or myosin-equivalent) system. Other physiological experiments (using inhibitors in "leaky" cells or antibodies injected into cells) that on the face of it would seem to rule out actin and myosin on closer scrutiny do not really do so at all. I argue that in vivo the "on" ends of chromosomal spindle fibre microtubules are at the kinetochores; I discuss the apparent contradiction between this conclusion and those from experiments on microtubules in vitro. From what we know of treadmilling in microtubules in vitro, the poleward movements of irradiation-induced areas of reduced birefringence (arb) can not be explained as treadmilling of microtubules: additional assumptions need to be made for arb movements toward the pole to be due to treadmilling. If arb movement does indeed represent treadmilling along chromosomal spindle fibre microtubules, treadmilling continues throughout anaphase. Thus I suggest that chromosomal spindle fibres shorten in anaphase not because polymerization is stopped at the kinetochore (the on end), as previously assumed, but rather because there is increased depolymerization at the pole (the "off" end).

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KCC2 overexpression prevents the paradoxical seizure-promoting action of somatic inhibition

10.1101/279539 ◽

2018 ◽

Cited By ~ 1

Author(s):

Vincent Magloire ◽

Jonathan Cornford ◽

Andreas Lieb ◽

Dimitri M. Kullmann ◽

Ivan Pavlov

Keyword(s):

Potassium Chloride ◽

Cortical Neurons ◽

Closed Loop ◽

Network Activity ◽

Intracellular Chloride ◽

Cortical Interneurons ◽

The Face ◽

Somatic Inhibition

AbstractAlthough cortical interneurons are apparently well-placed to suppress seizures, several recent reports have highlighted a paradoxical role of parvalbumin-positive perisomatic-targeting (PV+) interneurons in ictogenesis. Here, we use an acute in vivo model of focal cortical seizures in awake behaving mice, together with closed-loop optogenetic manipulation of PV+ interneurons, to investigate their function during seizures. We show that photo-depolarization of PV+ interneurons rapidly switches from an anti-ictal to a pro-ictal effect within a few seconds of seizure initiation. The pro-ictal effect of delayed photostimulation of PV+ interneurons was not shared with dendrite-targeting somatostatin-positive (SOM+) interneurons. We also show that this switch can be prevented by overexpression of the neuronal potassium-chloride co-transporter KCC2 in principal cortical neurons. These results suggest that strategies aimed at improving the ability of principal neurons to maintain intracellular chloride levels in the face of excessive network activity can prevent interneurons from contributing to seizure perpetuation.

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Separating Spike Count Correlation from Firing Rate Correlation

Neural Computation ◽

10.1162/neco_a_00831 ◽

2016 ◽

Vol 28 (5) ◽

pp. 849-881 ◽

Cited By ~ 3

Author(s):

Giuseppe Vinci ◽

Valérie Ventura ◽

Matthew A. Smith ◽

Robert E. Kass

Keyword(s):

Firing Rate ◽

Cortical Neurons ◽

Experimental Manipulation ◽

Response Variability ◽

Spike Count ◽

Firing Rates ◽

Area V4 ◽

Rate Correlation ◽

Over Time

Populations of cortical neurons exhibit shared fluctuations in spiking activity over time. When measured for a pair of neurons over multiple repetitions of an identical stimulus, this phenomenon emerges as correlated trial-to-trial response variability via spike count correlation (SCC). However, spike counts can be viewed as noisy versions of firing rates, which can vary from trial to trial. From this perspective, the SCC for a pair of neurons becomes a noisy version of the corresponding firing rate correlation (FRC). Furthermore, the magnitude of the SCC is generally smaller than that of the FRC and is likely to be less sensitive to experimental manipulation. We provide statistical methods for disambiguating time-averaged drive from within-trial noise, thereby separating FRC from SCC. We study these methods to document their reliability, and we apply them to neurons recorded in vivo from area V4 in an alert animal. We show how the various effects we describe are reflected in the data: within-trial effects are largely negligible, while attenuation due to trial-to-trial variation dominates and frequently produces comparisons in SCC that, because of noise, do not accurately reflect those based on the underlying FRC.

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Firing rate homeostasis occurs in the absence of neuronal activity-regulated transcription

10.1101/675728 ◽

2019 ◽

Author(s):

Kelsey M. Tyssowski ◽

Katherine C. Letai ◽

Samuel D. Rendall ◽

Anastasia Nizhnik ◽

Jesse M. Gray

Keyword(s):

Firing Rate ◽

Neuronal Activity ◽

Cortical Neurons ◽

Molecular Mechanisms ◽

Neuronal Circuits ◽

Electrode Arrays ◽

Knock Out ◽

Firing Rates ◽

The Face ◽

Homeostatic Mechanisms

ABSTRACTDespite dynamic inputs, neuronal circuits maintain relatively stable firing rates over long periods. This maintenance of firing rate, or firing rate homeostasis, is likely mediated by homeostatic mechanisms such as synaptic scaling and regulation of intrinsic excitability. Because some of these homeostatic mechanisms depend on transcription of activity-regulated genes, including Arc and Homer1a, we hypothesized that activity-regulated transcription would be required for firing rate homeostasis. Surprisingly, however, we found that cultured mouse cortical neurons grown on multi-electrode arrays homeostatically adapt their firing rates to persistent pharmacological stimulation even when activity-regulated transcription is disrupted. Specifically, we observed firing rate homeostasis Arc knock-out neurons, as well as knock-out neurons lacking activity-regulated transcription factors, AP1 and SRF. Firing rate homeostasis also occurred normally during acute pharmacological blockade of transcription. Thus, firing rate homeostasis in response to increased neuronal activity can occur in the absence of neuronal-activity-regulated transcription.SIGNIFICANCE STATEMENTNeuronal circuits maintain relatively stable firing rates even in the face of dynamic circuit inputs. Understanding the molecular mechanisms that enable this firing rate homeostasis could potentially provide insight into neuronal diseases that present with an imbalance of excitation and inhibition. However, the molecular mechanisms underlying firing rate homeostasis are largely unknown.It has long been hypothesized that firing rate homeostasis relies upon neuronal activity-regulated transcription. For example, a 2012 review (PMID 22685679) proposed it, and a 2014 modeling approach established that transcription could theoretically both measure and control firing rate (PMID 24853940). Surprisingly, despite this prediction, we found that cortical neurons undergo firing rate homeostasis in the absence of activity-regulated transcription, indicating that firing rate homeostasis is controlled by non-transcriptional mechanisms.

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The Effect of Agents which Modify Platelet Behaviour and of Magnesium Ions on Thrombus Formation In Vivo

Thrombosis and Haemostasis ◽

10.1055/s-0038-1666898 ◽

1979 ◽

Vol 42 (02) ◽

pp. 603-610 ◽

Cited By ~ 59

Author(s):

J H Adams ◽

J R A Mitchell

Keyword(s):

Thrombus Formation ◽

Cerebral Arteries ◽

Magnesium Ions ◽

Body Formation ◽

Inflammatory Agent ◽

Platelet Thrombus ◽

Magnesium Salts ◽

Higher Doses ◽

Do So

SummaryThe ability of potential anti-thrombotic agents to modify platelet-thrombus formation in injured cerebral arteries in the rabbit was tested. Low doses of heparin were without effect, while higher doses produced variable suppression of white body formation but at the expense of bleeding. Aspirin did not inhibit white body formation but another non-steroid anti-inflammatory agent, flurbiprofen was able to do so, as was the anti-gout agent, sulphinpyrazone. Magnesium salts both topically and parenterally, suppressed thrombus formation and increased the concentration of ADP which was required to initiate thrombus production at minor injury sites.

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Challenging Gender Hierarchies in Narratives of the Nation: Representations of Women in Zintgraff and the Battle of Mankon and Hard Choice

Imbizo ◽

10.25159/2663-6565/7815 ◽

2020 ◽

Vol 11 (2) ◽

Author(s):

Naomi Epongse Nkealah ◽

Olutoba Gboyega Oluwasuji

Keyword(s):

The Other ◽

Literary Texts ◽

Gender Differentiation ◽

Hard Choice ◽

Other Hand ◽

Gender Hierarchies ◽

The Face ◽

The One ◽

Representations Of Women ◽

Do So

Ideas of nationalisms as masculine projects dominate literary texts by African male writers. The texts mirror the ways in which gender differentiation sanctions nationalist discourses and in turn how nationalist discourses reinforce gender hierarchies. This article draws on theoretical insights from the work of Anne McClintock and Elleke Boehmer to analyse two plays: Zintgraff and the Battle of Mankon by Bole Butake and Gilbert Doho and Hard Choice by Sunnie Ododo. The article argues that women are represented in these two plays as having an ambiguous relationship to nationalism. On the one hand, women are seen actively changing the face of politics in their societies, but on the other hand, the means by which they do so reduces them to stereotypes of their gender.

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Faculty Opinions recommendation of Functional mapping of single spines in cortical neurons in vivo.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.12240956.14688103 ◽

2011 ◽

Author(s):

Leonard Maler

Keyword(s):

Cortical Neurons ◽

Functional Mapping

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Molecular basis of adaptive evolution of sperm motility involved in in vivo fertilization of terrestrial animals

Impact ◽

10.21820/23987073.2020.6.73 ◽

2020 ◽

Vol 2020 (6) ◽

pp. 73-75

Author(s):

Akihiko Watanabe

Keyword(s):

Sexual Reproduction ◽

Sperm Motility ◽

Asexual Reproduction ◽

Acrosome Reaction ◽

Sperm Morphology ◽

Adaptive Potential ◽

Selective Pressures ◽

The Face ◽

Genetic Profiles

One of the unifying traits of life on this planet is reproduction, or life's ability to make copies of itself. The mode of reproduction has evolved over time, having almost certainly begun with simple asexual reproduction when the ancestral single celled organism divided into two. Since these beginnings' life has tried out numerous strategies, and perhaps one of the most important and successful has been sexual reproduction. This form of reproduction relies on the union of gametes, otherwise known as sperm and egg. Evolutionarily, sexual reproduction allows for greater adaptive potential because the genes of two unique individuals have a chance to recombine and mix in order to produce a new individual. Unlike asexual reproduction which produces genetically-identical clones of the parent individual, sex produces offspring with novel genes and combinations of genes. Therefore, in the face of new selective pressures there is a higher chance that one of these novel genetic profiles will produce an adaptation that is advantageous in the new circumstances. Dr Akihiko Watanabe is a reproductive biologist based in the Department of Biology, Faculty of Science Yamagata University in Japan, he is currently working on three research projects; a comparative study on the signalling pathways for inducing sperm motility and acrosome reaction in amphibians, the mechanism behind the adaptive modification of sperm morphology and motility, and the origin of sperm motility initiating substance (SMIS).

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A deep convolutional visual encoding model of neuronal responses in the LGN

Brain Informatics ◽

10.1186/s40708-021-00132-6 ◽

2021 ◽

Vol 8 (1) ◽

Author(s):

Eslam Mounier ◽

Bassem Abdullah ◽

Hani Mahdi ◽

Seif Eldawlatly

Keyword(s):

Firing Rate ◽

Visual Information ◽

Visual Stimulation ◽

Neuronal Population ◽

Neuronal Firing ◽

Electrode Arrays ◽

Deep Convolutional Neural Networks ◽

Firing Rates ◽

Spatiotemporal Representation

AbstractThe Lateral Geniculate Nucleus (LGN) represents one of the major processing sites along the visual pathway. Despite its crucial role in processing visual information and its utility as one target for recently developed visual prostheses, it is much less studied compared to the retina and the visual cortex. In this paper, we introduce a deep learning encoder to predict LGN neuronal firing in response to different visual stimulation patterns. The encoder comprises a deep Convolutional Neural Network (CNN) that incorporates visual stimulus spatiotemporal representation in addition to LGN neuronal firing history to predict the response of LGN neurons. Extracellular activity was recorded in vivo using multi-electrode arrays from single units in the LGN in 12 anesthetized rats with a total neuronal population of 150 units. Neural activity was recorded in response to single-pixel, checkerboard and geometrical shapes visual stimulation patterns. Extracted firing rates and the corresponding stimulation patterns were used to train the model. The performance of the model was assessed using different testing data sets and different firing rate windows. An overall mean correlation coefficient between the actual and the predicted firing rates of 0.57 and 0.7 was achieved for the 10 ms and the 50 ms firing rate windows, respectively. Results demonstrate that the model is robust to variability in the spatiotemporal properties of the recorded neurons outperforming other examined models including the state-of-the-art Generalized Linear Model (GLM). The results indicate the potential of deep convolutional neural networks as viable models of LGN firing.

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TRAF3 mediates neuronal apoptosis in early brain injury following subarachnoid hemorrhage via targeting TAK1-dependent MAPKs and NF-κB pathways

Cell Death and Disease ◽

10.1038/s41419-020-03278-z ◽

2021 ◽

Vol 12 (1) ◽

Author(s):

Yan Zhou ◽

Tao Tao ◽

Guangjie Liu ◽

Xuan Gao ◽

Yongyue Gao ◽

...

Keyword(s):

Subarachnoid Hemorrhage ◽

Brain Injury ◽

Therapeutic Target ◽

Cortical Neurons ◽

Neuronal Apoptosis ◽

Early Brain Injury ◽

Neurological Deficits ◽

Human Brain Tissue

AbstractNeuronal apoptosis has an important role in early brain injury (EBI) following subarachnoid hemorrhage (SAH). TRAF3 was reported as a promising therapeutic target for stroke management, which covered several neuronal apoptosis signaling cascades. Hence, the present study is aimed to determine whether downregulation of TRAF3 could be neuroprotective in SAH-induced EBI. An in vivo SAH model in mice was established by endovascular perforation. Meanwhile, primary cultured cortical neurons of mice treated with oxygen hemoglobin were applied to mimic SAH in vitro. Our results demonstrated that TRAF3 protein expression increased and expressed in neurons both in vivo and in vitro SAH models. TRAF3 siRNA reversed neuronal loss and improved neurological deficits in SAH mice, and reduced cell death in SAH primary neurons. Mechanistically, we found that TRAF3 directly binds to TAK1 and potentiates phosphorylation and activation of TAK1, which further enhances the activation of NF-κB and MAPKs pathways to induce neuronal apoptosis. Importantly, TRAF3 expression was elevated following SAH in human brain tissue and was mainly expressed in neurons. Taken together, our study demonstrates that TRAF3 is an upstream regulator of MAPKs and NF-κB pathways in SAH-induced EBI via its interaction with and activation of TAK1. Furthermore, the TRAF3 may serve as a novel therapeutic target in SAH-induced EBI.

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