Please use this identifier to cite or link to this item: http://dr.iiserpune.ac.in:8080/xmlui/handle/123456789/3088
Title: Intracellular calcium stores mediate metaplasticity at hippocampal dendritic spines
Authors: MAHAJAN, GAURANG
NADKARNI, SUHITA
Dept. of Biology
Keywords: Synaptic plasticity
Intracellular calcium stores
Calcium signaling
Metaplasticity
Biophysical modeling
TOC-MAY-2019
2019
Issue Date: May-2019
Publisher: Wiley
Citation: Journal of Physiology, 597(13), 3473-3502.
Abstract: Long‐term plasticity mediated by NMDA receptors supports input‐specific, Hebbian forms of learning at excitatory CA3–CA1 connections in the hippocampus. There exists an additional layer of stabilizing mechanisms that act globally as well as locally over multiple time scales to ensure that plasticity occurs in a constrained manner. Here, we investigated the role of calcium (Ca2+) stores associated with the endoplasmic reticulum (ER) in the local regulation of plasticity at individual CA1 synapses. Our study was spurred by (1) the curious observation that ER is sparsely distributed in dendritic spines, but over‐represented in larger spines that are likely to have undergone activity‐dependent strengthening, and (2) evidence suggesting that ER motility at synapses can be rapid, and accompany activity‐regulated spine remodelling. We constructed a physiologically realistic computational model of an ER‐bearing CA1 spine, and examined how IP3‐sensitive Ca2+ stores affect spine Ca2+ dynamics during activity patterns mimicking the induction of long‐term potentiation and long‐term depression (LTD). Our results suggest that the presence of ER modulates NMDA receptor‐dependent plasticity in a graded manner that selectively enhances LTD induction. We propose that ER may locally tune Ca2+‐based plasticity, providing a braking mechanism to mitigate runaway strengthening at potentiated synapses. Our study provides a biophysically accurate description of postsynaptic Ca2+ regulation, and suggests that ER in the spine may promote the re‐use of hippocampal synapses with saturated strengths.
URI: http://dr.iiserpune.ac.in:8080/xmlui/handle/123456789/3088
https://doi.org/10.1113/JP277726
ISSN: 1469-7793
Appears in Collections:JOURNAL ARTICLES

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