Publications by authors named "Natalia Goriounova"

Hippocampal pyramidal neuron activity underlies episodic memory and spatial navigation. Although extensively studied in rodents, extremely little is known about human hippocampal pyramidal neurons, even though the human hippocampus underwent strong evolutionary reorganization and shows lower theta rhythm frequencies. To test whether biophysical properties of human Cornu Amonis subfield 1 (CA1) pyramidal neurons can explain observed rhythms, we map the morpho-electric properties of individual CA1 pyramidal neurons in human, non-pathological hippocampal slices from neurosurgery.

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  • Recent studies on human cortex have shown that GABAergic neurons have a complex hierarchical organization with various subclasses and specific types.
  • Researchers used advanced techniques to study these neurons in human brain slices, combining viral labeling and single-cell RNA sequencing.
  • The findings revealed detailed differences within GABAergic neuron types, including variations between human and mouse neurons and highlighted the need for comprehensive analysis to better understand brain cell properties.
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Neocortical layer 1 (L1) is a site of convergence between pyramidal-neuron dendrites and feedback axons where local inhibitory signaling can profoundly shape cortical processing. Evolutionary expansion of human neocortex is marked by distinctive pyramidal neurons with extensive L1 branching, but whether L1 interneurons are similarly diverse is underexplored. Using Patch-seq recordings from human neurosurgical tissue, we identified four transcriptomic subclasses with mouse L1 homologs, along with distinct subtypes and types unmatched in mouse L1.

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Fast-spiking interneurons (FSINs) provide fast inhibition that synchronizes neuronal activity and is critical for cognitive function. Fast synchronization frequencies are evolutionary conserved in the expanded human neocortex despite larger neuron-to-neuron distances that challenge fast input-output transfer functions of FSINs. Here, we test in human neurons from neurosurgery tissue, which mechanistic specializations of human FSINs explain their fast-signaling properties in human cortex.

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Human cortical pyramidal neurons are large, have extensive dendritic trees, and yet have unexpectedly fast input-output properties: Rapid subthreshold synaptic membrane potential changes are reliably encoded in timing of action potentials (APs). Here, we tested whether biophysical properties of voltage-gated sodium (Na) and potassium (K) currents in human pyramidal neurons can explain their fast input-output properties. Human Na and K currents exhibited more depolarized voltage dependence, slower inactivation, and faster recovery from inactivation compared with their mouse counterparts.

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GWAS have identified numerous genes associated with human cognition but their cell type expression profiles in the human brain are unknown. These genes overlap with human accelerated regions (HARs) implicated in human brain evolution and might act on the same biological processes. Here, we investigated whether these gene sets are expressed in adult human cortical neurons, and how their expression relates to neuronal function and structure.

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Synaptic transmission constitutes the primary mode of communication between neurons. It is extensively studied in rodent but not human neocortex. We characterized synaptic transmission between pyramidal neurons in layers 2 and 3 using neurosurgically resected human middle temporal gyrus (MTG, Brodmann area 21), which is part of the distributed language circuitry.

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The neocortex is disproportionately expanded in human compared with mouse, both in its total volume relative to subcortical structures and in the proportion occupied by supragranular layers composed of neurons that selectively make connections within the neocortex and with other telencephalic structures. Single-cell transcriptomic analyses of human and mouse neocortex show an increased diversity of glutamatergic neuron types in supragranular layers in human neocortex and pronounced gradients as a function of cortical depth. Here, to probe the functional and anatomical correlates of this transcriptomic diversity, we developed a robust platform combining patch clamp recording, biocytin staining and single-cell RNA-sequencing (Patch-seq) to examine neurosurgically resected human tissues.

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Temporal lobe epilepsy (TLE) patients are at risk of memory deficits, which have been linked to functional network disturbances, particularly of integration of the default mode network (DMN). However, the cellular substrates of functional network integration are unknown. We leverage a unique cross-scale dataset of drug-resistant TLE patients (n = 31), who underwent pseudo resting-state functional magnetic resonance imaging (fMRI), resting-state magnetoencephalography (MEG) and/or neuropsychological testing before neurosurgery.

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To understand the function of cortical circuits, it is necessary to catalog their cellular diversity. Past attempts to do so using anatomical, physiological or molecular features of cortical cells have not resulted in a unified taxonomy of neuronal or glial cell types, partly due to limited data. Single-cell transcriptomics is enabling, for the first time, systematic high-throughput measurements of cortical cells and generation of datasets that hold the promise of being complete, accurate and permanent.

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  • An amendment to the original paper has been published.
  • You can find the amendment through a link provided at the top of the paper.
  • This additional information could be important for understanding the updated content.
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  • ChAT-VIP interneurons, a special type of neuron in the brain's cortex, play a key role in signaling by directly exciting nearby neurons using acetylcholine (ACh) for fast communication.
  • These neurons are connected to both interneurons and pyramidal neurons across different layers of the medial prefrontal cortex (mPFC), highlighting their widespread influence.
  • Importantly, ChAT-VIP neurons help regulate attention behaviors in a unique way compared to other ACh sources in the brain, indicating their distinct functional role in cognitive processes.
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  • Group I metabotropic glutamate receptors (mGluRs) are key players in brain signaling and are being studied as potential targets for treating neuropsychiatric and developmental disorders.
  • Research primarily focused on rodent brains has begun exploring how these receptors impact human neocortex microcircuits, revealing significant effects on neuron activity.
  • Activation of group I mGluRs increases inhibitory action from Martinotti cells, affects other interneurons differently, and depresses excitatory synapses in human pyramidal neurons, suggesting a crucial shift in the balance of excitation and inhibition in the brain.
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What is the neurobiological basis of human intelligence? The brains of some people seem to be more efficient than those of others. Understanding the biological foundations of these differences is of great interest to basic and applied neuroscience. Somehow, the secret must lie in the cells in our brain with which we think.

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It is generally assumed that human intelligence relies on efficient processing by neurons in our brain. Although grey matter thickness and activity of temporal and frontal cortical areas correlate with IQ scores, no direct evidence exists that links structural and physiological properties of neurons to human intelligence. Here, we find that high IQ scores and large temporal cortical thickness associate with larger, more complex dendrites of human pyramidal neurons.

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  • Inhibitory pathways involving different types of interneurons, like basket cells (BCs) and Martinotti cells (MCs), influence the activity of neocortical pyramidal neurons, with BCs providing fast and MCs providing delayed lateral inhibition.
  • Acetylcholine plays a critical role in modulating cortical functions and has a notable effect on MC firing by enhancing and speeding up the lateral inhibition mediated by MCs specifically, rather than BCs.
  • The study demonstrates that cholinergic inputs act through specific receptors to recruit more MCs, which helps emphasize particular neural circuits in the neocortex, a mechanism that is also present in humans.
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  • Synaptic plasticity is key to understanding learning and memory in the adult human brain, but studying it is challenging due to limited access to live human neurons.
  • Research methods have yielded insights into the properties and plasticity of adult human synapses, uncovering some surprising findings.
  • This text explores experimental approaches, mechanisms of Hebbian spike timing-dependent plasticity (STDP), and how these principles relate to human learning and memory.
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The size and shape of dendrites and axons are strong determinants of neuronal information processing. Our knowledge on neuronal structure and function is primarily based on brains of laboratory animals. Whether it translates to human is not known since quantitative data on "full" human neuronal morphologies are lacking.

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The diuretic agent bumetanide has recently been put forward as a novel, promising treatment of behavioral symptoms in autism spectrum disorder (ASD) and related conditions. Bumetanide can decrease neuronal chloride concentrations and may thereby reinstate γ-aminobutyric acid (GABA)-ergic inhibition in patients with neurodevelopmental disorders. However, strategies to select appropriate candidates for bumetanide treatment are lacking.

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  • The neocortex stores long-term memories by altering neuron connections, but the details of these processes in humans are not well-understood.
  • Researchers studied human pyramidal neurons to explore how synaptic strength changes with spike timing, finding that both strengthening (long-term potentiation) and weakening (long-term depression) of connections involve NMDA receptors and occur throughout adulthood.
  • Unlike in rodents, human synapses can respond to temporal events over a broader range, influenced by the activation of L-type voltage-gated Ca2+ channels during neuron firing, which affects whether synapses grow stronger or weaker.
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More than 70% of adolescents report to have smoked a cigarette at least once. At the adolescent stage the brain has not completed its maturation. The prefrontal cortex (PFC), the brain area responsible for executive functions and attention performance, is one of the last brain areas to mature and is still developing during adolescence.

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The majority of adolescents report to have smoked a cigarette at least once. Adolescence is a critical period of brain development during which maturation of areas involved in cognitive functioning, such as the medial prefrontal cortex (mPFC), is still ongoing. Tobacco smoking during this age may compromise the normal course of prefrontal development and lead to cognitive impairments in later life.

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