Synaptic Input and ACh Modulation Regulate Dendritic Ca2+ Spike Duration in Pyramidal Neurons, Directly Affecting Their Somatic Output

Amir Dudai; Michael Doron; Idan Segev; Michael London

doi:10.1523/JNEUROSCI.1470-21.2021

Synaptic Input and ACh Modulation Regulate Dendritic Ca²⁺ Spike Duration in Pyramidal Neurons, Directly Affecting Their Somatic Output

Amir Dudai, Michael Doron, Idan Segev, Michael London^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

Nonlinear synaptic integration in dendrites is a fundamental aspect of neural computation. One such key mechanism is the Ca²⁺ spike at the apical tuft of pyramidal neurons. Characterized by a plateau potential sustained for tens of milliseconds, the Ca²⁺ spike amplifies excitatory input, facilitates somatic action potentials (APs), and promotes synaptic plasticity. Despite its essential role, the mechanisms regulating it are largely unknown. Using a compartmental model of a layer 5 pyramidal cell (L5PC), we explored the plateau and termination phases of the Ca²⁺ spike under input current perturbations, long-step current-injections, and variations in the dendritic high-voltage-activated Ca²⁺ conductance (that occur during cholinergic modulation). We found that, surprisingly, timed excitatory input can shorten the Ca²⁺ spike duration while inhibitory input can either elongate or terminate it. A significant elongation also occurs when the high-voltage-activated Ca²+ channels (Ca_HVA) conductance is increased. To mechanistically understand these phenomena, we analyzed the currents involved in the spike. The plateau and termination phases are almost exclusively controlled by the Ca_HVA inward current and the I_m outward K⁺ current. We reduced the full model to a single-compartment model that faithfully preserved the responses of the Ca²⁺ spike to interventions and consisted of two dynamic variables: the membrane potential and the K⁺-channel activation level. A phase-plane analysis of the reduced model provides testable predictions for modulating the Ca²⁺ spike and reveals various dynamical regimes that explain the robust nature of the spike. Regulating the duration of the Ca²⁺ spike significantly impacts the cell synaptic-plasticity window and, as we show, its input-output relationship.

Original language	American English
Pages (from-to)	1184-1195
Number of pages	12
Journal	Journal of Neuroscience
Volume	42
Issue number	7
DOIs	https://doi.org/10.1523/JNEUROSCI.1470-21.2021
State	Published - 16 Feb 2022

Bibliographical note

Funding Information:
Received July 18, 2021; revised Nov. 25, 2021; accepted Nov. 29, 2021. Author contributions: A.D., M.D., and M.L. designed research; A.D. and M.D. performed research; A.D. contributed unpublished reagents/analytic tools; A.D. analyzed data; A.D. wrote the first draft of the paper; A.D., I.S., and M.L. edited the paper; A.D. and M.L. wrote the paper. This work was supported by the Israeli Science Foundation Grant 1024/17, the Einstein Foundation (M.L.), and the Gatsby Charitable Foundation. A.D. is an H. & S. Hoffman fellow. M.L. is a Sachs Family Lecturer in Brain Science. The authors declare no competing financial interests. Correspondence should be addressed to Michael London at mickey.london@mail.huji.ac.il. https://doi.org/10.1523/JNEUROSCI.1470-21.2021 Copyright © 2022 the authors

Publisher Copyright:
Copyright © 2022 the authors

Keywords

Ca spike
dendrites
phase plane
synaptic perturbation

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10.1523/JNEUROSCI.1470-21.2021

Cite this

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title = "Synaptic Input and ACh Modulation Regulate Dendritic Ca2+ Spike Duration in Pyramidal Neurons, Directly Affecting Their Somatic Output",

abstract = "Nonlinear synaptic integration in dendrites is a fundamental aspect of neural computation. One such key mechanism is the Ca2+ spike at the apical tuft of pyramidal neurons. Characterized by a plateau potential sustained for tens of milliseconds, the Ca2+ spike amplifies excitatory input, facilitates somatic action potentials (APs), and promotes synaptic plasticity. Despite its essential role, the mechanisms regulating it are largely unknown. Using a compartmental model of a layer 5 pyramidal cell (L5PC), we explored the plateau and termination phases of the Ca2+ spike under input current perturbations, long-step current-injections, and variations in the dendritic high-voltage-activated Ca2+ conductance (that occur during cholinergic modulation). We found that, surprisingly, timed excitatory input can shorten the Ca2+ spike duration while inhibitory input can either elongate or terminate it. A significant elongation also occurs when the high-voltage-activated Ca2+ channels (CaHVA) conductance is increased. To mechanistically understand these phenomena, we analyzed the currents involved in the spike. The plateau and termination phases are almost exclusively controlled by the CaHVA inward current and the Im outward K+ current. We reduced the full model to a single-compartment model that faithfully preserved the responses of the Ca2+ spike to interventions and consisted of two dynamic variables: the membrane potential and the K+-channel activation level. A phase-plane analysis of the reduced model provides testable predictions for modulating the Ca2+ spike and reveals various dynamical regimes that explain the robust nature of the spike. Regulating the duration of the Ca2+ spike significantly impacts the cell synaptic-plasticity window and, as we show, its input-output relationship.",

keywords = "Ca spike, dendrites, phase plane, synaptic perturbation",

author = "Amir Dudai and Michael Doron and Idan Segev and Michael London",

note = "Funding Information: Received July 18, 2021; revised Nov. 25, 2021; accepted Nov. 29, 2021. Author contributions: A.D., M.D., and M.L. designed research; A.D. and M.D. performed research; A.D. contributed unpublished reagents/analytic tools; A.D. analyzed data; A.D. wrote the first draft of the paper; A.D., I.S., and M.L. edited the paper; A.D. and M.L. wrote the paper. This work was supported by the Israeli Science Foundation Grant 1024/17, the Einstein Foundation (M.L.), and the Gatsby Charitable Foundation. A.D. is an H. & S. Hoffman fellow. M.L. is a Sachs Family Lecturer in Brain Science. The authors declare no competing financial interests. Correspondence should be addressed to Michael London at mickey.london@mail.huji.ac.il. https://doi.org/10.1523/JNEUROSCI.1470-21.2021 Copyright {\textcopyright} 2022 the authors Publisher Copyright: Copyright {\textcopyright} 2022 the authors",

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T1 - Synaptic Input and ACh Modulation Regulate Dendritic Ca2+ Spike Duration in Pyramidal Neurons, Directly Affecting Their Somatic Output

AU - Dudai, Amir

AU - Doron, Michael

AU - Segev, Idan

AU - London, Michael

N1 - Funding Information: Received July 18, 2021; revised Nov. 25, 2021; accepted Nov. 29, 2021. Author contributions: A.D., M.D., and M.L. designed research; A.D. and M.D. performed research; A.D. contributed unpublished reagents/analytic tools; A.D. analyzed data; A.D. wrote the first draft of the paper; A.D., I.S., and M.L. edited the paper; A.D. and M.L. wrote the paper. This work was supported by the Israeli Science Foundation Grant 1024/17, the Einstein Foundation (M.L.), and the Gatsby Charitable Foundation. A.D. is an H. & S. Hoffman fellow. M.L. is a Sachs Family Lecturer in Brain Science. The authors declare no competing financial interests. Correspondence should be addressed to Michael London at mickey.london@mail.huji.ac.il. https://doi.org/10.1523/JNEUROSCI.1470-21.2021 Copyright © 2022 the authors Publisher Copyright: Copyright © 2022 the authors

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N2 - Nonlinear synaptic integration in dendrites is a fundamental aspect of neural computation. One such key mechanism is the Ca2+ spike at the apical tuft of pyramidal neurons. Characterized by a plateau potential sustained for tens of milliseconds, the Ca2+ spike amplifies excitatory input, facilitates somatic action potentials (APs), and promotes synaptic plasticity. Despite its essential role, the mechanisms regulating it are largely unknown. Using a compartmental model of a layer 5 pyramidal cell (L5PC), we explored the plateau and termination phases of the Ca2+ spike under input current perturbations, long-step current-injections, and variations in the dendritic high-voltage-activated Ca2+ conductance (that occur during cholinergic modulation). We found that, surprisingly, timed excitatory input can shorten the Ca2+ spike duration while inhibitory input can either elongate or terminate it. A significant elongation also occurs when the high-voltage-activated Ca2+ channels (CaHVA) conductance is increased. To mechanistically understand these phenomena, we analyzed the currents involved in the spike. The plateau and termination phases are almost exclusively controlled by the CaHVA inward current and the Im outward K+ current. We reduced the full model to a single-compartment model that faithfully preserved the responses of the Ca2+ spike to interventions and consisted of two dynamic variables: the membrane potential and the K+-channel activation level. A phase-plane analysis of the reduced model provides testable predictions for modulating the Ca2+ spike and reveals various dynamical regimes that explain the robust nature of the spike. Regulating the duration of the Ca2+ spike significantly impacts the cell synaptic-plasticity window and, as we show, its input-output relationship.

AB - Nonlinear synaptic integration in dendrites is a fundamental aspect of neural computation. One such key mechanism is the Ca2+ spike at the apical tuft of pyramidal neurons. Characterized by a plateau potential sustained for tens of milliseconds, the Ca2+ spike amplifies excitatory input, facilitates somatic action potentials (APs), and promotes synaptic plasticity. Despite its essential role, the mechanisms regulating it are largely unknown. Using a compartmental model of a layer 5 pyramidal cell (L5PC), we explored the plateau and termination phases of the Ca2+ spike under input current perturbations, long-step current-injections, and variations in the dendritic high-voltage-activated Ca2+ conductance (that occur during cholinergic modulation). We found that, surprisingly, timed excitatory input can shorten the Ca2+ spike duration while inhibitory input can either elongate or terminate it. A significant elongation also occurs when the high-voltage-activated Ca2+ channels (CaHVA) conductance is increased. To mechanistically understand these phenomena, we analyzed the currents involved in the spike. The plateau and termination phases are almost exclusively controlled by the CaHVA inward current and the Im outward K+ current. We reduced the full model to a single-compartment model that faithfully preserved the responses of the Ca2+ spike to interventions and consisted of two dynamic variables: the membrane potential and the K+-channel activation level. A phase-plane analysis of the reduced model provides testable predictions for modulating the Ca2+ spike and reveals various dynamical regimes that explain the robust nature of the spike. Regulating the duration of the Ca2+ spike significantly impacts the cell synaptic-plasticity window and, as we show, its input-output relationship.

KW - Ca spike

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