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The physiological variability of channel density in hippocampal CA1 pyramidal cells and interneurons explored using a unified data-driven modeling workflow

Author

Listed:
  • Rosanna Migliore
  • Carmen A Lupascu
  • Luca L Bologna
  • Armando Romani
  • Jean-Denis Courcol
  • Stefano Antonel
  • Werner A H Van Geit
  • Alex M Thomson
  • Audrey Mercer
  • Sigrun Lange
  • Joanne Falck
  • Christian A Rössert
  • Ying Shi
  • Olivier Hagens
  • Maurizio Pezzoli
  • Tamas F Freund
  • Szabolcs Kali
  • Eilif B Muller
  • Felix Schürmann
  • Henry Markram
  • Michele Migliore

Abstract

Every neuron is part of a network, exerting its function by transforming multiple spatiotemporal synaptic input patterns into a single spiking output. This function is specified by the particular shape and passive electrical properties of the neuronal membrane, and the composition and spatial distribution of ion channels across its processes. For a variety of physiological or pathological reasons, the intrinsic input/output function may change during a neuron’s lifetime. This process results in high variability in the peak specific conductance of ion channels in individual neurons. The mechanisms responsible for this variability are not well understood, although there are clear indications from experiments and modeling that degeneracy and correlation among multiple channels may be involved. Here, we studied this issue in biophysical models of hippocampal CA1 pyramidal neurons and interneurons. Using a unified data-driven simulation workflow and starting from a set of experimental recordings and morphological reconstructions obtained from rats, we built and analyzed several ensembles of morphologically and biophysically accurate single cell models with intrinsic electrophysiological properties consistent with experimental findings. The results suggest that the set of conductances expressed in any given hippocampal neuron may be considered as belonging to two groups: one subset is responsible for the major characteristics of the firing behavior in each population and the other is responsible for a robust degeneracy. Analysis of the model neurons suggests several experimentally testable predictions related to the combination and relative proportion of the different conductances that should be expressed on the membrane of different types of neurons for them to fulfill their role in the hippocampus circuitry.Author summary: The peak conductance of many ion channel types measured in any given animal is highly variable across neurons, both within and between neuronal populations. The current view is that this occurs because a neuron needs to adapt its intrinsic electrophysiological properties either to maintain the same operative range in the presence of abnormal inputs or to compensate for the effects of pathological conditions. Limited experimental and modeling evidence suggests this might be implemented via the correlation and/or degeneracy in the function of multiple types of conductances. To study this mechanism in hippocampal CA1 neurons and interneurons, we systematically generated a set of morphologically and biophysically accurate models. We then analyzed the ensembles of peak conductance obtained for each model neuron. The results suggest that the set of conductances expressed in the various neuron types may be divided into two groups: one group is responsible for the major characteristics of the firing behavior in each population and the other is more involved with degeneracy. These models provide experimentally testable predictions on the combination and relative proportion of the different conductance types that should be present in hippocampal CA1 pyramidal cells and interneurons.

Suggested Citation

  • Rosanna Migliore & Carmen A Lupascu & Luca L Bologna & Armando Romani & Jean-Denis Courcol & Stefano Antonel & Werner A H Van Geit & Alex M Thomson & Audrey Mercer & Sigrun Lange & Joanne Falck & Chri, 2018. "The physiological variability of channel density in hippocampal CA1 pyramidal cells and interneurons explored using a unified data-driven modeling workflow," PLOS Computational Biology, Public Library of Science, vol. 14(9), pages 1-25, September.
    • Handle: RePEc:plo:pcbi00:1006423
    DOI: 10.1371/journal.pcbi.1006423
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    1. Nathan W. Gouwens & Jim Berg & David Feng & Staci A. Sorensen & Hongkui Zeng & Michael J. Hawrylycz & Christof Koch & Anton Arkhipov, 2018. "Systematic generation of biophysically detailed models for diverse cortical neuron types," Nature Communications, Nature, vol. 9(1), pages 1-13, December.
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    1. Michalis Pagkalos & Spyridon Chavlis & Panayiota Poirazi, 2023. "Introducing the Dendrify framework for incorporating dendrites to spiking neural networks," Nature Communications, Nature, vol. 14(1), pages 1-16, December.

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