Histone acetylation is recruited in consolidation as a molecular feature of stronger memories

Gene expression is a key process for memory consolidation. Recently, the participation of epigenetic mechanisms like histone acetylation was evidenced in long-term memories. However, until now the training strength required and the persistence of the chromatin acetylation recruited are not well char...

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Autores principales: Federman, N., Fustiñana, M.S., Romano, A.
Formato: JOUR
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Acceso en línea:http://hdl.handle.net/20.500.12110/paper_10720502_v16_n10_p600_Federman
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spelling todo:paper_10720502_v16_n10_p600_Federman2023-10-03T16:02:43Z Histone acetylation is recruited in consolidation as a molecular feature of stronger memories Federman, N. Fustiñana, M.S. Romano, A. butyric acid histone histone H3 trichostatin A acetylation animal experiment animal tissue article biological model chromatin crab epigenetics gene expression regulation invertebrate long term memory male memory memory consolidation molecular interaction nonhuman parameter priority journal task performance training Western blotting Gene expression is a key process for memory consolidation. Recently, the participation of epigenetic mechanisms like histone acetylation was evidenced in long-term memories. However, until now the training strength required and the persistence of the chromatin acetylation recruited are not well characterized. Here we studied whether histone acetylation is involved in consolidation in invertebrates, whether it depends on the training strength, and whether it is a permanent or transient mechanism. We used a well-characterized memory model in invertebrates, the context-signal memory in crabs. Our results show no changes in histone 3 (H3) acetylation during consolidation of a standard training protocol. However, strong training induced a significant increase in H3 acetylation 1-h post-training, returning to basal levels afterward. Accordingly, the administration of histone deacetylase inhibitors sodium butyrate (NaB) and trichostatin A allowed a weak training to induce long-term memory. NaB enhanced memory in two phases during consolidation. These findings support that H3 acetylation (1) is involved in consolidation, (2) occurs only after strong training, (3) is a transient process, and (4) memory is enhanced in two phases. The coincidence of these phases with other mechanisms of gene expression is discussed. © 2009 Cold Spring Harbor Laboratory Press. JOUR info:eu-repo/semantics/openAccess http://creativecommons.org/licenses/by/2.5/ar http://hdl.handle.net/20.500.12110/paper_10720502_v16_n10_p600_Federman
institution Universidad de Buenos Aires
institution_str I-28
repository_str R-134
collection Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA)
topic butyric acid
histone
histone H3
trichostatin A
acetylation
animal experiment
animal tissue
article
biological model
chromatin
crab
epigenetics
gene expression regulation
invertebrate
long term memory
male
memory
memory consolidation
molecular interaction
nonhuman
parameter
priority journal
task performance
training
Western blotting
spellingShingle butyric acid
histone
histone H3
trichostatin A
acetylation
animal experiment
animal tissue
article
biological model
chromatin
crab
epigenetics
gene expression regulation
invertebrate
long term memory
male
memory
memory consolidation
molecular interaction
nonhuman
parameter
priority journal
task performance
training
Western blotting
Federman, N.
Fustiñana, M.S.
Romano, A.
Histone acetylation is recruited in consolidation as a molecular feature of stronger memories
topic_facet butyric acid
histone
histone H3
trichostatin A
acetylation
animal experiment
animal tissue
article
biological model
chromatin
crab
epigenetics
gene expression regulation
invertebrate
long term memory
male
memory
memory consolidation
molecular interaction
nonhuman
parameter
priority journal
task performance
training
Western blotting
description Gene expression is a key process for memory consolidation. Recently, the participation of epigenetic mechanisms like histone acetylation was evidenced in long-term memories. However, until now the training strength required and the persistence of the chromatin acetylation recruited are not well characterized. Here we studied whether histone acetylation is involved in consolidation in invertebrates, whether it depends on the training strength, and whether it is a permanent or transient mechanism. We used a well-characterized memory model in invertebrates, the context-signal memory in crabs. Our results show no changes in histone 3 (H3) acetylation during consolidation of a standard training protocol. However, strong training induced a significant increase in H3 acetylation 1-h post-training, returning to basal levels afterward. Accordingly, the administration of histone deacetylase inhibitors sodium butyrate (NaB) and trichostatin A allowed a weak training to induce long-term memory. NaB enhanced memory in two phases during consolidation. These findings support that H3 acetylation (1) is involved in consolidation, (2) occurs only after strong training, (3) is a transient process, and (4) memory is enhanced in two phases. The coincidence of these phases with other mechanisms of gene expression is discussed. © 2009 Cold Spring Harbor Laboratory Press.
format JOUR
author Federman, N.
Fustiñana, M.S.
Romano, A.
author_facet Federman, N.
Fustiñana, M.S.
Romano, A.
author_sort Federman, N.
title Histone acetylation is recruited in consolidation as a molecular feature of stronger memories
title_short Histone acetylation is recruited in consolidation as a molecular feature of stronger memories
title_full Histone acetylation is recruited in consolidation as a molecular feature of stronger memories
title_fullStr Histone acetylation is recruited in consolidation as a molecular feature of stronger memories
title_full_unstemmed Histone acetylation is recruited in consolidation as a molecular feature of stronger memories
title_sort histone acetylation is recruited in consolidation as a molecular feature of stronger memories
url http://hdl.handle.net/20.500.12110/paper_10720502_v16_n10_p600_Federman
work_keys_str_mv AT federmann histoneacetylationisrecruitedinconsolidationasamolecularfeatureofstrongermemories
AT fustinanams histoneacetylationisrecruitedinconsolidationasamolecularfeatureofstrongermemories
AT romanoa histoneacetylationisrecruitedinconsolidationasamolecularfeatureofstrongermemories
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