Estrogens Rapidly Enhance Neural Plasticity and Learning

Estrogens Rapidly Enhance Neural Plasticity and Learning

This thesis examines the rapid, non-genomic effects of estrogens on neural plasticity and learning. Estrogens are classically known to affect gene transcription events, however they have more recently been found to also rapidly activate second messenger systems within 1hr of administration. Therefor...

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Bibliographic Details
Main Author: Phan, Anna
Other Authors: Choleris, Elena
Language:en
Published: 2013
Subjects:
Estrogen
Estradiol
Learning
Memory
Object Placement
Object Recognition
Social Recognition
Non-genomic
AMPA
NMDA
Dendritic Spines
Electrophysiology
LTP
LTD
Hippocampus
CA1
GPER
ERα
ERβ
Mice
Immature synapse
Synaptic plasticity
Structural plasticity
Glutamate
Learning spine
Memory spine
Online Access:http://hdl.handle.net/10214/7288
id ndltd-LACETR-oai-collectionscanada.gc.ca-OGU.10214-7288
record_format oai_dc
spelling ndltd-LACETR-oai-collectionscanada.gc.ca-OGU.10214-72882013-10-04T04:14:29ZEstrogens Rapidly Enhance Neural Plasticity and LearningPhan, AnnaEstrogenEstradiolLearningMemoryObject PlacementObject RecognitionSocial RecognitionNon-genomicAMPANMDADendritic SpinesElectrophysiologyLTPLTDHippocampusCA1GPERERαERβMiceImmature synapseSynaptic plasticityStructural plasticityGlutamateLearning spineMemory spineThis thesis examines the rapid, non-genomic effects of estrogens on neural plasticity and learning. Estrogens are classically known to affect gene transcription events, however they have more recently been found to also rapidly activate second messenger systems within 1hr of administration. Therefore, we first examined the rapid effects of 17β-estradiol, and an estrogen receptor (ER) α and ERβ agonist on three different learning paradigms: object placement, object recognition, and social recognition. We found that both systemic injections and intrahippocampal delivery of 17β-estradiol and the ERα agonist improved performance on all 3 learning paradigms within 40min of hormone administration. However, the ERβ agonist administered systemically or intrahippocampally, improved performance only on the object placement learning paradigm, while having no effect on object recognition, and impairing social recognition at high doses. To elucidate how estrogens might rapidly affect learning, we examined how estrogens rapidly affect the neural plasticity of CA1 hippocampal neurons. We found that 17β-estradiol and the ERα agonist increased dendritic spine density in CA1 hippocampal neurons within 40min of administration, suggesting that estrogens rapidly increase the density of synapses within this brain region. Conversely, the ERβ agonist did not affect spine density, or decreased spine density. In addition, by using whole-cell patch clamp recordings of CA1 pyramidal neurons, we were able to determine that 17β-estradiol and the ERα agonist rapidly reduced AMPA receptor (but not NMDA receptor) mediated membrane depolarizations after 15min of hormone application. Similar to above, the ERβ agonist had no effect on AMPA or NMDA receptor mediated membrane depolarizations. These data suggest that estrogens rapidly promote the development of immature synapses (which contain low levels of synaptic AMPA receptors) within the CA1 hippocampus. Immature spines provide synaptic sites at which new memories can be stored and are thought of as “learning spines” (Kasai et al, 2003). Therefore, estrogens (through ERα) may rapidly induce the formation of hippocampal immature spines to promote learning.Funded by NSERCCholeris, ElenaMacLusky, Neil2013-06-212013-07-24T14:42:06Z2013-07-24T14:42:06Z2013-07-24Thesishttp://hdl.handle.net/10214/7288en
collection NDLTD
language en
sources NDLTD
topic Estrogen
Estradiol
Learning
Memory
Object Placement
Object Recognition
Social Recognition
Non-genomic
AMPA
NMDA
Dendritic Spines
Electrophysiology
LTP
LTD
Hippocampus
CA1
GPER
ERα
ERβ
Mice
Immature synapse
Synaptic plasticity
Structural plasticity
Glutamate
Learning spine
Memory spine
spellingShingle Estrogen
Estradiol
Learning
Memory
Object Placement
Object Recognition
Social Recognition
Non-genomic
AMPA
NMDA
Dendritic Spines
Electrophysiology
LTP
LTD
Hippocampus
CA1
GPER
ERα
ERβ
Mice
Immature synapse
Synaptic plasticity
Structural plasticity
Glutamate
Learning spine
Memory spine
Phan, Anna
Estrogens Rapidly Enhance Neural Plasticity and Learning
description This thesis examines the rapid, non-genomic effects of estrogens on neural plasticity and learning. Estrogens are classically known to affect gene transcription events, however they have more recently been found to also rapidly activate second messenger systems within 1hr of administration. Therefore, we first examined the rapid effects of 17β-estradiol, and an estrogen receptor (ER) α and ERβ agonist on three different learning paradigms: object placement, object recognition, and social recognition. We found that both systemic injections and intrahippocampal delivery of 17β-estradiol and the ERα agonist improved performance on all 3 learning paradigms within 40min of hormone administration. However, the ERβ agonist administered systemically or intrahippocampally, improved performance only on the object placement learning paradigm, while having no effect on object recognition, and impairing social recognition at high doses. To elucidate how estrogens might rapidly affect learning, we examined how estrogens rapidly affect the neural plasticity of CA1 hippocampal neurons. We found that 17β-estradiol and the ERα agonist increased dendritic spine density in CA1 hippocampal neurons within 40min of administration, suggesting that estrogens rapidly increase the density of synapses within this brain region. Conversely, the ERβ agonist did not affect spine density, or decreased spine density. In addition, by using whole-cell patch clamp recordings of CA1 pyramidal neurons, we were able to determine that 17β-estradiol and the ERα agonist rapidly reduced AMPA receptor (but not NMDA receptor) mediated membrane depolarizations after 15min of hormone application. Similar to above, the ERβ agonist had no effect on AMPA or NMDA receptor mediated membrane depolarizations. These data suggest that estrogens rapidly promote the development of immature synapses (which contain low levels of synaptic AMPA receptors) within the CA1 hippocampus. Immature spines provide synaptic sites at which new memories can be stored and are thought of as “learning spines” (Kasai et al, 2003). Therefore, estrogens (through ERα) may rapidly induce the formation of hippocampal immature spines to promote learning. === Funded by NSERC
author2 Choleris, Elena
author_facet Choleris, Elena
Phan, Anna
author Phan, Anna
author_sort Phan, Anna
title Estrogens Rapidly Enhance Neural Plasticity and Learning
title_short Estrogens Rapidly Enhance Neural Plasticity and Learning
title_full Estrogens Rapidly Enhance Neural Plasticity and Learning
title_fullStr Estrogens Rapidly Enhance Neural Plasticity and Learning
title_full_unstemmed Estrogens Rapidly Enhance Neural Plasticity and Learning
title_sort estrogens rapidly enhance neural plasticity and learning
publishDate 2013
url http://hdl.handle.net/10214/7288
work_keys_str_mv AT phananna estrogensrapidlyenhanceneuralplasticityandlearning
_version_ 1716601950887215104

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