Diverse calcium dynamics underlie place field formation in hippocampal CA1 pyramidal cells (hdl:21.15109/ARP/YGNZNJ)

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Document Description

Citation

Title:

Diverse calcium dynamics underlie place field formation in hippocampal CA1 pyramidal cells

Identification Number:

hdl:21.15109/ARP/YGNZNJ

Distributor:

ARP

Date of Distribution:

2025-09-05

Version:

1

Bibliographic Citation:

Sumegi, Mate; Olah, Gaspar; Lukacs, Istvan Paul; Blazsek, Martin; Makara, K. Judit; Nusser, Zoltan, 2025, "Diverse calcium dynamics underlie place field formation in hippocampal CA1 pyramidal cells", https://hdl.handle.net/21.15109/ARP/YGNZNJ, ARP, V1

Study Description

Citation

Title:

Diverse calcium dynamics underlie place field formation in hippocampal CA1 pyramidal cells

Identification Number:

hdl:21.15109/ARP/YGNZNJ

Authoring Entity:

Sumegi, Mate (HUN-REN Institute of Experimental Medicine)

Olah, Gaspar (HUN-REN Institute of Experimental Medicine)

Lukacs, Istvan Paul (HUN-REN Institute of Experimental Medicine)

Blazsek, Martin (HUN-REN Institute of Experimental Medicine)

Makara, K. Judit (HUN-REN Institute of Experimental Medicine)

Nusser, Zoltan (HUN-REN Institute of Experimental Medicine)

Distributor:

ARP

Access Authority:

Nusser, Zoltan

Depositor:

Sumegi, Mate

Date of Deposit:

2025-09-05

Holdings Information:

https://hdl.handle.net/21.15109/ARP/YGNZNJ

Study Scope

Keywords:

Medicine, Health and Life Sciences

Abstract:

Every explored environment is represented in the hippocampus by the activity of distinct populations of pyramidal cells (PCs) that typically fire at specific locations called their place fields (PFs). New PFs are constantly born even in familiar surroundings (during representational drift), and many rapidly emerge when the animal explores a new or altered environment (during global or partial remapping). Behavioral time scale synaptic plasticity (BTSP), a plasticity mechanism based on prolonged somatic action potential (AP) bursts induced by dendritic Ca2+/NMDA plateau potentials, was recently proposed as the main cellular mechanism underlying new PF formations (PFF), but it is unclear whether burst-associated large somatic [Ca2+] transients are always necessary and/or sufficient for PFF. To address this issue, here we performed in vivo two-photon [Ca2+] imaging of hippocampal CA1 PCs in head-restrained mice to investigate somatic [Ca2+] dynamics underlying PFFs in familiar and novel virtual environments. Our results demonstrate that although many PFs are formed by BTSP-like events, PFs also emerge with initial [Ca2+] dynamics that do not match any of the characteristics of BTSP. BTSP and non-BTSP-like new PFFs occur spontaneously in familiar environments, during neuronal representational switches and instantaneously in new environments. Our data also reveal that solitary [Ca2+] transients with larger amplitudes than those evoking BTSP-like PFFs, frequently occur without inducing PFs, demonstrating that large [Ca2+] transients per se are not sufficient for PFF

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