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Mouse Cortex

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mouse cortex

Discover seminars, jobs, and research tagged with mouse cortex across World Wide.
15 curated items9 ePosters6 Seminars
Updated over 1 year ago
15 items · mouse cortex
15 results
SeminarNeuroscience

Modeling human brain development and disease: the role of primary cilia

Kyrousi Christina
Medical School, National and Kapodistrian University of Athens, Athens, Greece
Apr 23, 2024

Neurodevelopmental disorders (NDDs) impose a global burden, affecting an increasing number of individuals. While some causative genes have been identified, understanding the human-specific mechanisms involved in these disorders remains limited. Traditional gene-driven approaches for modeling brain diseases have failed to capture the diverse and convergent mechanisms at play. Centrosomes and cilia act as intermediaries between environmental and intrinsic signals, regulating cellular behavior. Mutations or dosage variations disrupting their function have been linked to brain formation deficits, highlighting their importance, yet their precise contributions remain largely unknown. Hence, we aim to investigate whether the centrosome/cilia axis is crucial for brain development and serves as a hub for human-specific mechanisms disrupted in NDDs. Towards this direction, we first demonstrated species-specific and cell-type-specific differences in the cilia-genes expression during mouse and human corticogenesis. Then, to dissect their role, we provoked their ectopic overexpression or silencing in the developing mouse cortex or in human brain organoids. Our findings suggest that cilia genes manipulation alters both the numbers and the position of NPCs and neurons in the developing cortex. Interestingly, primary cilium morphology is disrupted, as we find changes in their length, orientation and number that lead to disruption of the apical belt and altered delamination profiles during development. Our results give insight into the role of primary cilia in human cortical development and address fundamental questions regarding the diversity and convergence of gene function in development and disease manifestation. It has the potential to uncover novel pharmacological targets, facilitate personalized medicine, and improve the lives of individuals affected by NDDs through targeted cilia-based therapies.

SeminarNeuroscienceRecording

Dynamics of cortical circuits: underlying mechanisms and computational implications

Alessandro Sanzeni
Bocconi University, Milano
Jan 24, 2023

A signature feature of cortical circuits is the irregularity of neuronal firing, which manifests itself in the high temporal variability of spiking and the broad distribution of rates. Theoretical works have shown that this feature emerges dynamically in network models if coupling between cells is strong, i.e. if the mean number of synapses per neuron K is large and synaptic efficacy is of order 1/\sqrt{K}. However, the degree to which these models capture the mechanisms underlying neuronal firing in cortical circuits is not fully understood. Results have been derived using neuron models with current-based synapses, i.e. neglecting the dependence of synaptic current on the membrane potential, and an understanding of how irregular firing emerges in models with conductance-based synapses is still lacking. Moreover, at odds with the nonlinear responses to multiple stimuli observed in cortex, network models with strongly coupled cells respond linearly to inputs. In this talk, I will discuss the emergence of irregular firing and nonlinear response in networks of leaky integrate-and-fire neurons. First, I will show that, when synapses are conductance-based, irregular firing emerges if synaptic efficacy is of order 1/\log(K) and, unlike in current-based models, persists even under the large heterogeneity of connections which has been reported experimentally. I will then describe an analysis of neural responses as a function of coupling strength and show that, while a linear input-output relation is ubiquitous at strong coupling, nonlinear responses are prominent at moderate coupling. I will conclude by discussing experimental evidence of moderate coupling and loose balance in the mouse cortex.

SeminarNeuroscience

Epigenome regulation in neocortex expansion and generation of neuronal subtypes

Tran Tuoc, PhD
Ruhruniversität-Bochum, Humangenetik
Aug 23, 2022

Evolutionarily, the expansion of the human neocortex accounts for many of the unique cognitive abilities of humans. This expansion appears to reflect the increased proliferative potential of basal progenitors (BPs) in mammalian evolution. Further cortical progenitors generate both glutamatergic excitatory neurons (ENs) and GABAergic inhibitory interneurons (INs) in human cortex, whereas they produce exclusively ENs in rodents. The increased proliferative capacity and neuronal subtype generation of cortical progenitors in mammalian evolution may have evolved through epigenetic alterations. However, whether or how the epigenome in cortical progenitors differs between humans and other species is unknown. Here, we report that histone H3 acetylation is a key epigenetic regulation in BP profiling of sorted BPs, we show that H3K9 acetylation is low in murine BPs and high in amplification, neuronal subtype generation and cortical expansion. Through epigenetic profiling of sorted BPs, we show that H3K9 acetylation is low in murine BPs and high in human BPs. Elevated H3K9ac preferentially increases BP proliferation, increasing the size and folding of the normally smooth mouse neocortex. Furthermore, we found that the elevated H3 acetylation activates expression of IN genes in in developing mouse cortex and promote proliferation of IN progenitor-like cells in cortex of Pax6 mutant mouse models. Mechanistically, H3K9ac drives the BP amplification and proliferation of these IN progenitor-like cells by increasing expression of the evolutionarily regulated gene, TRNP1. Our findings demonstrate a previously unknown mechanism that controls neocortex expansion and generation of neuronal subtypes. Keywords: Cortical development, neurogenesis, basal progenitors, cortical size, gyrification, excitatory neuron, inhibitory interneuron, epigenetic profiling, epigenetic regulation, H3 acetylation, H3K9ac, TRNP1, PAX6

SeminarNeuroscience

Merging of cues and hunches by the mouse cortex

Matteo Carandini
UCL
Oct 28, 2021

Many everyday decisions are based on both external cues and internal hunches. How does the brain put these together? We addressed this question in mice trained to make decisions based on sensory stimuli and on past events. While mice made these decisions, we causally probed the roles of cortical areas and recorded from thousands of neurons throughout the brain, with an emphasis on frontal cortex. The results are not what we thought based on textbook notions of how the brain works. This talk is based on work led by Nick Steinmetz, Peter Zatka-Haas, Armin Lak, and Pip Coen, in the laboratory I share with Kenneth Harris

SeminarNeuroscience

Cell types of adult mouse cortex and hippocampus

Bosiljka Tasic
Molecular Genetics, Allen Institute for Brain Science, Seattle, USA
Jun 15, 2021
SeminarNeuroscienceRecording

A human-specific modifier of synaptic development, cortical circuit connectivity and function

Franck Polleux
Columbia University
Apr 29, 2020

The remarkable cognitive abilities characterizing humans has been linked to unique patterns of connectivity characterizing the neocortex. Comparative studies have shown that human cortical pyramidal neurons (PN) receive a significant increase of synaptic inputs when compared to other mammals, including non-human primates and rodents, but how this may relate to changes in cortical connectivity and function remained largely unknown. We previously identified a human-specific gene duplication (HSGD), SRGAP2C, that, when induced in mouse cortical PNs drives human-specific features of synaptic development, including a correlated increase in excitatory (E) and inhibitory (I) synapse density through inhibition of the ancestral SRGAP2A protein (Charrier et al. 2012; Fossatti et al. 2016; Schmidt et al. 2019). However, the origin and nature of this increased connectivity and its impact on cortical circuit function was unknown. I will present new results exploring these questions (see Schmidt et al. (2020) https://www.biorxiv.org/content/10.1101/852970v1). Using a combination of transgenic approaches and quantitative monosynaptic tracing, we discovered that humanization of SRGAP2C expression in the mouse cortex leads to a specific increase in local and long-range cortico-cortical inputs received by layer 2/3 cortical PNs. Moreover, using in vivo two-photon imaging in the barrel cortex of awake mice, we show that humanization of SRGAP2C expression increases the reliability and selectivity of sensory- evoked responses in layer 2/3 PNs. We also found that mice humanized for SRGAP2C in all cortical pyramidal neurons and throughout development are characterized by improved behavioural performance in a novel whisker-based sensory discrimination task compared to control wild-type mice. Our results suggest that the emergence of SRGAP2C during human evolution underlie a new substrate for human brain evolution whereby it led to increased local and long-range cortico-cortical connectivity and improved reliability of sensory-evoked cortical coding. References cited Charrier C.*, Joshi K. *, Coutinho-Budd J., Kim, J-E., Lambert N., de Marchena, J., Jin W-L., Vanderhaeghen P., Ghosh A., Sassa T, and Polleux F. (2012) Inhibition of SRGAP2 function by its human-specific paralogs induces neoteny of spine maturation. Cell 149:923-935. * Co-first authors. Fossati M, Pizzarelli R, Schmidt ER, Kupferman JV, Stroebel D, Polleux F*, Charrier C*. (2016) SRGAP2 and Its Human-Specific Paralog Co-Regulate the Development of Excitatory and Inhibitory Synapses. Neuron. 91(2):356-69. * Co-senior corresponding authors. Schmidt E.R.E., Kupferman J.V., Stackmann M., Polleux F. (2019) The human-specific paralogs SRGAP2 and SRGAP2C differentially modulate SRGAP2A-dependent synaptic development. Scientific Rep. 9(1):18692. Schmidt E.R.E, Zhao H.T., Hillman E.M.C., Polleux F. (2020) Humanization of SRGAP2C expression increases cortico-cortical connectivity and reliability of sensory-evoked responses in mouse brain. Submitted. See also: https://www.biorxiv.org/content/10.1101/852970v1

ePoster

Isolated correlates of somatosensory perception in the posterior mouse cortex

COSYNE 2022

ePoster

Isolated correlates of somatosensory perception in the posterior mouse cortex

COSYNE 2022

ePoster

Targeted single-cell ablation uncovers network homeostasis of sound representations in mouse cortex

Takahiro Noda, Jens-Bastian Eppler, Matthias Kaschube, Simon Rumpel, Eike Kienle, Yonatan Loewenstein

COSYNE 2023

ePoster

Topography of multisensory convergence throughout the mouse cortex

Kinjal Pravinbhai Patel, Avery Ryoo, Stefan Mihalas, Bryan Tripp

COSYNE 2023

ePoster

Inhibition-stabilized disordered dynamics in mouse cortex during navigational decision-making

Siyan Zhou, Ryan Badman, Charlotte Arlt, Kanaka Rajan, Christopher Harvey

COSYNE 2025

ePoster

Functional implications of traumatic brain injury-induced changes in serine/threonine kinase activity and peptide phosphorylation in mouse cortex

Celine Gallagher, Thomas Mittmann

FENS Forum 2024

ePoster

KIF5B plays important roles in dendritic spine plasticity and dendritic localization of PSD95 and FMRP in the mouse cortex in vivo

Cora Sau Wan Lai, Albert Hiu Ka Fok, Yuhua Huang, Beth Wing Lam So, Qiyu Zheng, Chun Sing Carlos Tse, Xiaoyang Li, Kenneth Kin-Yip Wong, Jiandong Huang, Kwok-On Lai

FENS Forum 2024

ePoster

Neural encoding of sensory “surprise” in the mouse cortex

Diego Benusiglio, Sofija Perovic, Richard Somervail, Gian Domenico Iannetti, Hiroki Asari

FENS Forum 2024

ePoster

Spontaneous mesoscale calcium dynamics reflect the development of the modular functional architecture of the mouse cortex

Davide Warm, Davide Bassetti, Levente Gellèrt, Jenq-Wei Yang, Heiko J. Luhmann, Anne Sinning

FENS Forum 2024