The roles of protein expression in synaptic plasticity and memory consolidation

Rosenberg, Tali; Gal-Ben-Ari, Shunit; Dieterich, Daniela C.; Kreutz, Michael R.; Ziv, Noam; Gundelfinger, Eckart D.; Rosenblum, Kobi

doi:10.3389/fnmol.2014.00086

Cited by 136 publications

(109 citation statements)

References 172 publications

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“…Estradiol may therefore act rapidly on early memory consolidation mechanisms through protein kinase cascades (Fortress et al, 2013;Sarkar et al, 2010;Srivastava, 2012) and/or by modifying dendritic spine morphology (Luine and Frankfurt, 2012;Phan et al, 2012;Srivastava, 2012). The effect observed here and by Phan et al (2012) at a time when memory consolidation is not yet completed (Rosenberg et al, 2014;Rudy, 2014) suggest that 17␤-E2 may also rapidly affect the early encoding of new memories.…”

Section: ␤-Estradiol Rapidly Facilitates Social Learning In the Stfpmentioning

confidence: 72%

Activation of the G protein-coupled estrogen receptor, but not estrogen receptor α or β, rapidly enhances social learning

Ervin

Mulvale

Gallagher

et al. 2015

Psychoneuroendocrinology

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Section: ␤-Estradiol Rapidly Facilitates Social Learning In the Stfpmentioning

confidence: 72%

Activation of the G protein-coupled estrogen receptor, but not estrogen receptor α or β, rapidly enhances social learning

Ervin

Mulvale

Gallagher

et al. 2015

Psychoneuroendocrinology

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“…Despite the abundant candidates involved even in a specific learning process, the actual number of neurons may be limited and a memory engram may be spatially curbed to specific subspaces of neurons. Learning is a dynamic process while protein expression and post-translational modification profiles may markedly change at different stages (33,72,73). Longterm synaptic plasticity is believed to be a cellular correlate of LTM.…”

Section: Discussionmentioning

confidence: 99%

“…Multiple synaptic activity-dependent signal transduction pathways (7)(8)(9)(10)(11)(12)(13)19) orchestrate the regulation of synaptic plasticity on the translational level (for review see (20,21)). Accumulated evidence shows that different types of LTM depend on protein synthesis, disregarding dependence on brain regions such as amygdala (22,23), hippocampus (24 -29), and medial prefrontal or insular cortex ((30 -32); for review see (33)). However, LTM perseveres significantly longer than duration of translation-dependent long-term plasticity.…”

mentioning

confidence: 99%

Dynamics of Hippocampal Protein Expression During Long-term Spatial Memory Formation

Borovok

Nesher

Levin

et al. 2016

Molecular & Cellular Proteomics

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Spatial memory depends on the hippocampus, which is particularly vulnerable to aging. This vulnerability has implications for the impairment of navigation capacities in older people, who may show a marked drop in performance of spatial tasks with advancing age. Contemporary understanding of long-term memory formation relies on molecular mechanisms underlying long-term synaptic plasticity. With memory acquisition, activity-dependent changes occurring in synapses initiate multiple signal transduction pathways enhancing protein turnover. This enhancement facilitates de novo synthesis of plasticity related proteins, crucial factors for establishing persistent long-term synaptic plasticity and forming memory engrams. Extensive studies have been performed to elucidate molecular mechanisms of memory traces formation; however, the identity of plasticity related proteins is still evasive. In this study, we investigated protein turnover in mouse hippocampus during long-term spatial memory formation using the reference memory version of radial arm maze (RAM) paradigm. We identified 1592 proteins, which exhibited a complex picture of expression changes during spatial memory formation. Variable linear decomposition reduced significantly data dimensionality and enriched three principal factors responsible for variance of memory-related protein levels at (1) the initial phase of memory acquisition (165 proteins), (2) during the steep learning improvement (148 proteins), and (3) the final phase of the learning curve (123 proteins). Gene ontology and signaling pathways analysis revealed a clear correlation between memory improvement and learning phasecurbed expression profiles of proteins belonging to specific functional categories. We found differential enrichment of (1) Long-term synaptic plasticity is considered a cellular correlate of long-term memory (LTM) 1 . Contemporary understanding of memory formation is based on the initiation and maintenance of long-term synaptic plasticity (1-4), for which de novo protein synthesis is a vital requirement. De novo protein synthesis itself is secondary to activity-dependent changes in synapses that occur during learning processes. These activity changes trigger post-translational modifications of proteins initiating and sustaining multiple signal transduction pathways. In turn, these signaling pathways regulate changes in synaptic strength and connectivity by governing gene expression and protein translation (5-13). Depending on time elapsed since triggering of long-term synaptic plasticity, protein synthesis may be limited to the dendrites directly involved in the plasticity processes (14 -18). Multiple synaptic From the ‡Department

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“…To establish long term memory, post encoding cellular and molecular processes take place over several hours, involving activation of many intracellular signaling pathways, eventually leading to new protein synthesis and changes in synaptic weights in relevant brain regions [10]. This is known as 'molecular memory consolidation' [11].…”

Section: Memory Consolidation and Long Term Plasticitymentioning

confidence: 99%