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De-repression of myelin-regulating gene expression after status epilepticus in mice lacking the C/EBP homologous protein CHOP
Date Issued
2014-12-15
Date Available
2020-12-01T15:50:05Z
Abstract
The C/EBP homologous protein CHOP is normally present at low levels in cells but increases rapidly after insults such as DNA damage or endoplasmatic reticulum stress where it contributes to cellular homeostasis and apoptosis. By forming heterodimers with other transcription factors, CHOP can either act as a dominant-negative regulator of gene expression or to induce the expression of target genes. Recent work demonstrated that seizure-induced hippocampal damage is significantly worse in mice lacking CHOP and these animals go on to develop an aggravated epileptic phenotype. To identify novel CHOP-controlled target genes which potentially influence the epileptic phenotype, we performed a bioinformatics analysis of tissue microarrays from chop-deficient mice after prolonged seizures. GO analysis revealed genes associated with biological membranes were prominent among those in the chop-deficient array dataset and we identified myelin-associated genes to be particularly de-repressed. These data suggest CHOP might act as an inhibitor of myelin-associated processes in the brain and could be targeted to influence axonal regeneration or reorganisation.
Sponsorship
Health Research Board
Science Foundation Ireland
Type of Material
Journal Article
Publisher
E-Century Publishing
Journal
International Journal of Physiology, Pathophysiology and Pharmacology
Volume
6
Issue
4
Start Page
185
End Page
198
Copyright (Published Version)
© 2014 E-Century Publishing Corporation.
Web versions
Language
English
Status of Item
Peer reviewed
ISSN
1944-8171
This item is made available under a Creative Commons License
File(s)
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Name
Sheedy_2014.pdf
Size
1.79 MB
Format
Adobe PDF
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