The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice

Thesis (M.Sc.)--Memorial University of Newfoundland, 2008. Psychology Includes bibliographical references (leaves 39-52) The goal of this study was to examine the role of the read-through variant of acetylcholinesterase (AChE-R) in the changes in affective behaviour using the predator stress model o...

Full description

Bibliographic Details
Main Author: Head, David Martin, 1981-
Other Authors: Memorial University of Newfoundland. Dept. of Psychology
Format: Thesis
Language:English
Published: 2008
Subjects:
Acetylcholinesterase > Physiological effect.
Predatory animals > Effect of stress on
Newfoundland studies
University of Newfoundland
Online Access:http://collections.mun.ca/cdm/ref/collection/theses4/id/172671
id ftmemorialunivdc:oai:collections.mun.ca:theses4/172671
record_format openpolar
spelling ftmemorialunivdc:oai:collections.mun.ca:theses4/172671 2023-05-15T17:23:34+02:00 The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice Head, David Martin, 1981- Memorial University of Newfoundland. Dept. of Psychology 2008 vii, 67 leaves : ill. Image/jpeg; Application/pdf http://collections.mun.ca/cdm/ref/collection/theses4/id/172671 Eng eng Electronic Theses and Dissertations (7.78 MB) -- http://collections.mun.ca/PDFs/theses/Head_DavidM.pdf a2543867 http://collections.mun.ca/cdm/ref/collection/theses4/id/172671 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 Acetylcholinesterase--Physiological effect. Predatory animals--Effect of stress on Text Electronic thesis or dissertation 2008 ftmemorialunivdc 2015-08-06T19:22:48Z Thesis (M.Sc.)--Memorial University of Newfoundland, 2008. Psychology Includes bibliographical references (leaves 39-52) The goal of this study was to examine the role of the read-through variant of acetylcholinesterase (AChE-R) in the changes in affective behaviour using the predator stress model of PTSD. This read through variant has been shown to exist at higher levels in the brain following stress (Pick, Flores-Flores, & Soreq, 2004, Meshorer et al., 2002). -- The role of acetylcholinesterase in predator stress was examined in mice using a novel drug EN 101, a systematically administered central acting antisense mRNA for AChE-R. Research by Pollak at el. (2005) demonstrated that cholinergic enhancement using EN 101 produces central and peripheral anti-inflammatory effects. EN101 acts to disrupt the stress precipitated induction of the transcription of the read-through variant of AChE by selectively targeting the mRNA sequence for AChE-R. It is AChE-R in limbic cholinergic circuitry that contributes to anxiogenic effects of traumatic stress (Talma et al., 2003). We administered multiple injections of the drug to the same animals at specific time points prior to and after a predator stress exposure in male C57 mice. This was done to ascertain whether the specific action of EN 101 on AChE-R expression had any effect on stress induced lasting changes in multiple tests of murine affective behaviour. -- Predator stress caused a significant increase in startle amplitude, which EN 101 blocked. This effect was specific to EN 101, as the control inverse drug INVEN101 was without effect on stress effects on startle amplitude. INVEN101 is the inverse of the EN 101 drug consisting of the same mRNA base pairs only in a different order than EN 101. This evidence suggests that EN101 is acting to lower the levels of the read-through variant of acetylcholinesterase in brain regions responsible for startle amplitude (hyperarousal) in rodents. Neither drug affected the impact of predator stress on behaviour in the plus maze, and both drugs partially reduced stress suppression of time active in the hole board. In the light dark box test INVEN101 appeared to exhibit a weak effect partially inhibiting the effects of predator stress on light dark box behaviour. This behavioural change would require replication in order to accept. Together the data reinforce the supposition that multiple neural systems are responsible for the different changes in behaviour produced by predator stress. -- This study provides evidence for a role of AChE-R in specific changes in anxiety-like behaviour following stress. Further research is necessary to pinpoint the exact time window for administration of the drug in order to prevent or inhibit changes in affective behaviour following predator stress. Work is also needed to determine whether other systemic effects of the drug might occur. Thesis Newfoundland studies University of Newfoundland Memorial University of Newfoundland: Digital Archives Initiative (DAI)
institution Open Polar
collection Memorial University of Newfoundland: Digital Archives Initiative (DAI)
op_collection_id ftmemorialunivdc
language English
topic Acetylcholinesterase--Physiological effect.
Predatory animals--Effect of stress on
spellingShingle Acetylcholinesterase--Physiological effect.
Predatory animals--Effect of stress on
Head, David Martin, 1981-
The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
topic_facet Acetylcholinesterase--Physiological effect.
Predatory animals--Effect of stress on
description Thesis (M.Sc.)--Memorial University of Newfoundland, 2008. Psychology Includes bibliographical references (leaves 39-52) The goal of this study was to examine the role of the read-through variant of acetylcholinesterase (AChE-R) in the changes in affective behaviour using the predator stress model of PTSD. This read through variant has been shown to exist at higher levels in the brain following stress (Pick, Flores-Flores, & Soreq, 2004, Meshorer et al., 2002). -- The role of acetylcholinesterase in predator stress was examined in mice using a novel drug EN 101, a systematically administered central acting antisense mRNA for AChE-R. Research by Pollak at el. (2005) demonstrated that cholinergic enhancement using EN 101 produces central and peripheral anti-inflammatory effects. EN101 acts to disrupt the stress precipitated induction of the transcription of the read-through variant of AChE by selectively targeting the mRNA sequence for AChE-R. It is AChE-R in limbic cholinergic circuitry that contributes to anxiogenic effects of traumatic stress (Talma et al., 2003). We administered multiple injections of the drug to the same animals at specific time points prior to and after a predator stress exposure in male C57 mice. This was done to ascertain whether the specific action of EN 101 on AChE-R expression had any effect on stress induced lasting changes in multiple tests of murine affective behaviour. -- Predator stress caused a significant increase in startle amplitude, which EN 101 blocked. This effect was specific to EN 101, as the control inverse drug INVEN101 was without effect on stress effects on startle amplitude. INVEN101 is the inverse of the EN 101 drug consisting of the same mRNA base pairs only in a different order than EN 101. This evidence suggests that EN101 is acting to lower the levels of the read-through variant of acetylcholinesterase in brain regions responsible for startle amplitude (hyperarousal) in rodents. Neither drug affected the impact of predator stress on behaviour in the plus maze, and both drugs partially reduced stress suppression of time active in the hole board. In the light dark box test INVEN101 appeared to exhibit a weak effect partially inhibiting the effects of predator stress on light dark box behaviour. This behavioural change would require replication in order to accept. Together the data reinforce the supposition that multiple neural systems are responsible for the different changes in behaviour produced by predator stress. -- This study provides evidence for a role of AChE-R in specific changes in anxiety-like behaviour following stress. Further research is necessary to pinpoint the exact time window for administration of the drug in order to prevent or inhibit changes in affective behaviour following predator stress. Work is also needed to determine whether other systemic effects of the drug might occur.
author2 Memorial University of Newfoundland. Dept. of Psychology
format Thesis
author Head, David Martin, 1981-
author_facet Head, David Martin, 1981-
author_sort Head, David Martin, 1981-
title The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
title_short The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
title_full The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
title_fullStr The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
title_full_unstemmed The role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
title_sort role of the read through variant of acetylcholinesterase in anxiogenic effects of predator stress in mice
publishDate 2008
url http://collections.mun.ca/cdm/ref/collection/theses4/id/172671
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
(7.78 MB) -- http://collections.mun.ca/PDFs/theses/Head_DavidM.pdf
a2543867
http://collections.mun.ca/cdm/ref/collection/theses4/id/172671
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_ 1766113353210527744

Similar Items