Does Hsp27 protect cortical neurons against amyloid?

Thesis (M.Sc.)--Memorial University of Newfoundland, 2009. Medicine Includes bibliographical references (leaves 94-105) Neurofibrillary tangles (NFTs) and plaques are considered to be hallmarks of Alzheimer's disease (AD), although it is still not clear whether these aggregates contribute to di...

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Bibliographic Details
Main Author: King, Michael T. C. (Michael Thomas Cecil)
Other Authors: Memorial University of Newfoundland. Faculty of Medicine
Format: Thesis
Language:English
Published: 2009
Subjects:
Amyloid beta-protein
Heat shock proteins
Neurons > Growth
Neurons > Protection
HSP27 Heat-Shock Proteins
Neurons
Amyloid beta-Peptides
Rats
Newfoundland studies
University of Newfoundland
Online Access:http://collections.mun.ca/cdm/ref/collection/theses4/id/44377
id ftmemorialunivdc:oai:collections.mun.ca:theses4/44377
record_format openpolar
institution Open Polar
collection Memorial University of Newfoundland: Digital Archives Initiative (DAI)
op_collection_id ftmemorialunivdc
language English
topic Amyloid beta-protein
Heat shock proteins
Neurons--Growth
Neurons--Protection
HSP27 Heat-Shock Proteins
Neurons
Amyloid beta-Peptides
Rats
spellingShingle Amyloid beta-protein
Heat shock proteins
Neurons--Growth
Neurons--Protection
HSP27 Heat-Shock Proteins
Neurons
Amyloid beta-Peptides
Rats
King, Michael T. C. (Michael Thomas Cecil)
Does Hsp27 protect cortical neurons against amyloid?
topic_facet Amyloid beta-protein
Heat shock proteins
Neurons--Growth
Neurons--Protection
HSP27 Heat-Shock Proteins
Neurons
Amyloid beta-Peptides
Rats
description Thesis (M.Sc.)--Memorial University of Newfoundland, 2009. Medicine Includes bibliographical references (leaves 94-105) Neurofibrillary tangles (NFTs) and plaques are considered to be hallmarks of Alzheimer's disease (AD), although it is still not clear whether these aggregates contribute to disease progress or whether they might even play an initial protective role. A number of studies have shown that the small heat shock protein Hsp27 can afford protection against oxidative stress, growth factor withdrawal or excitotoxicity in neuronal cell types. A moderate preconditioning heat shock (HS) is sufficient to upregulate levels of Hsp27 in cells, and the degree of protection correlates with the level of expression of Hsp27. There are reports of increased Hsp27 in AD brains and accumulation of Hsps in plaques, NFTs and Lewy bodies. Whether this represents a potentially protective response to the stress or is part of the disease process is not known. My hypothesis is that increased expression of Hsp27 can promote survival and stabilize the axonal cy to skeleton resulting in maintenance of neurite growth and axonal transport in the face of stressors such as amyloid. My specific aim was to determine whether Hsp27 is important for neuronal survival and neurite growth in primary cortical neurons in the presence or absence of β-amyloid peptides. -- Cultures of primary rat cortical neurons were subjected to HS in an effort to upregulate endogenous Hsp27, while in other experiments Hsp27 was overexpressed in cortical neurons by nucleofection. Efforts to upregulate endogenous Hsp27 in cortical neurons were unsuccessful, despite the fact that the neurons do express heat shock factor-1 (Hsfl) and increase activation of Hsfl in response to heat stress. In fact, it was seen that HS resulted in a reduction in neuronal survival, although previous data from our lab and the literature suggest that a thermal stress can provide protection against a more lethal subsequent stress. Consequently, I introduced a GFP-Hsp27 fusion protein at the time of plating and examined the potential effects of exogenous Hsp27 on neurite survival and growth using morphological and biochemical analyses. -- My results suggest that the presence of Hsp27 in cortical neurons provides them with a level of protection against β-amyloid. After treatment with Aβ1-42, cells with Hsp27 appeared healthier and had greater survival than those without. Interestingly, Aβ25-35 was not shown to be toxic to these neurons, whereas it has been previously shown to be toxic in a variety of experimental paradigms. Further, my data indicate that cells expressing Hsp27 have greater total neurite growth compared to the empty vector alone. Knowing that phosphorylation affects Hsp27 activity, I also investigated the effects of Hsp27Δ on survival and growth. Hsp27Δ is a mutated form of Hsp27 lacking the S15 phosphorylation site. My data show that HspΔ has similar effects on neurite outgrowth and survival as Hsp27WT, providing important preliminary data for future studies investigating the importance of phosphorylation in Hsp27 activity.
author2 Memorial University of Newfoundland. Faculty of Medicine
format Thesis
author King, Michael T. C. (Michael Thomas Cecil)
author_facet King, Michael T. C. (Michael Thomas Cecil)
author_sort King, Michael T. C. (Michael Thomas Cecil)
title Does Hsp27 protect cortical neurons against amyloid?
title_short Does Hsp27 protect cortical neurons against amyloid?
title_full Does Hsp27 protect cortical neurons against amyloid?
title_fullStr Does Hsp27 protect cortical neurons against amyloid?
title_full_unstemmed Does Hsp27 protect cortical neurons against amyloid?
title_sort does hsp27 protect cortical neurons against amyloid?
publishDate 2009
url http://collections.mun.ca/cdm/ref/collection/theses4/id/44377
genre Newfoundland studies
University of Newfoundland
genre_facet Newfoundland studies
University of Newfoundland
op_source Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries
op_relation Electronic Theses and Dissertations
(11.76 MB) -- http://collections.mun.ca/PDFs/theses/King_MichaelTC.pdf
a3242515
http://collections.mun.ca/cdm/ref/collection/theses4/id/44377
op_rights The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission.
_version_ 1766113237732950016
spelling ftmemorialunivdc:oai:collections.mun.ca:theses4/44377 2023-05-15T17:23:33+02:00 Does Hsp27 protect cortical neurons against amyloid? King, Michael T. C. (Michael Thomas Cecil) Memorial University of Newfoundland. Faculty of Medicine 2009 xiii, 106 leaves : ill. (some col.) Image/jpeg; Application/pdf http://collections.mun.ca/cdm/ref/collection/theses4/id/44377 Eng eng Electronic Theses and Dissertations (11.76 MB) -- http://collections.mun.ca/PDFs/theses/King_MichaelTC.pdf a3242515 http://collections.mun.ca/cdm/ref/collection/theses4/id/44377 The author retains copyright ownership and moral rights in this thesis. Neither the thesis nor substantial extracts from it may be printed or otherwise reproduced without the author's permission. Paper copy kept in the Centre for Newfoundland Studies, Memorial University Libraries Amyloid beta-protein Heat shock proteins Neurons--Growth Neurons--Protection HSP27 Heat-Shock Proteins Neurons Amyloid beta-Peptides Rats Text Electronic thesis or dissertation 2009 ftmemorialunivdc 2015-08-06T19:21:57Z Thesis (M.Sc.)--Memorial University of Newfoundland, 2009. Medicine Includes bibliographical references (leaves 94-105) Neurofibrillary tangles (NFTs) and plaques are considered to be hallmarks of Alzheimer's disease (AD), although it is still not clear whether these aggregates contribute to disease progress or whether they might even play an initial protective role. A number of studies have shown that the small heat shock protein Hsp27 can afford protection against oxidative stress, growth factor withdrawal or excitotoxicity in neuronal cell types. A moderate preconditioning heat shock (HS) is sufficient to upregulate levels of Hsp27 in cells, and the degree of protection correlates with the level of expression of Hsp27. There are reports of increased Hsp27 in AD brains and accumulation of Hsps in plaques, NFTs and Lewy bodies. Whether this represents a potentially protective response to the stress or is part of the disease process is not known. My hypothesis is that increased expression of Hsp27 can promote survival and stabilize the axonal cy to skeleton resulting in maintenance of neurite growth and axonal transport in the face of stressors such as amyloid. My specific aim was to determine whether Hsp27 is important for neuronal survival and neurite growth in primary cortical neurons in the presence or absence of β-amyloid peptides. -- Cultures of primary rat cortical neurons were subjected to HS in an effort to upregulate endogenous Hsp27, while in other experiments Hsp27 was overexpressed in cortical neurons by nucleofection. Efforts to upregulate endogenous Hsp27 in cortical neurons were unsuccessful, despite the fact that the neurons do express heat shock factor-1 (Hsfl) and increase activation of Hsfl in response to heat stress. In fact, it was seen that HS resulted in a reduction in neuronal survival, although previous data from our lab and the literature suggest that a thermal stress can provide protection against a more lethal subsequent stress. Consequently, I introduced a GFP-Hsp27 fusion protein at the time of plating and examined the potential effects of exogenous Hsp27 on neurite survival and growth using morphological and biochemical analyses. -- My results suggest that the presence of Hsp27 in cortical neurons provides them with a level of protection against β-amyloid. After treatment with Aβ1-42, cells with Hsp27 appeared healthier and had greater survival than those without. Interestingly, Aβ25-35 was not shown to be toxic to these neurons, whereas it has been previously shown to be toxic in a variety of experimental paradigms. Further, my data indicate that cells expressing Hsp27 have greater total neurite growth compared to the empty vector alone. Knowing that phosphorylation affects Hsp27 activity, I also investigated the effects of Hsp27Δ on survival and growth. Hsp27Δ is a mutated form of Hsp27 lacking the S15 phosphorylation site. My data show that HspΔ has similar effects on neurite outgrowth and survival as Hsp27WT, providing important preliminary data for future studies investigating the importance of phosphorylation in Hsp27 activity. Thesis Newfoundland studies University of Newfoundland Memorial University of Newfoundland: Digital Archives Initiative (DAI)

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