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Studies of XIST and macroH2A1.2 independent of gene silencing : subtitle a unique hybrid cell model system Kwok, Edmund

Abstract

X chromosome inactivation results in the transcriptional silencing of one of the two X chromosomes present in mammalian female cells. XIST expression from the inactive X (Xi), and subsequent coating of the Xi by the XIST RNA, marks the initial major observable characteristic of X-inactivation. The Xi then begins to exhibit features of heterochromatin such as gene silencing, late replication, histone modification, hypermethylation, and the recruitment of core histone variants. However, the exact mechanistic events between XIST expression and the final heterochromatic state of the Xi remain unclear. To better understand the relationship between XIST, heterochromatin, and silenced gene expression, the first goal of this study was to develop and characterize a model system suitable for examination of those features of heterochromatin which can be induced by XIST independent of gene silencing. Previous work using rodent/human hybrids (containing active human and mouse X chromosomes) that had been demethylated to reactivate XIST/Xist expression showed that while human XIST RNA fails to localize properly to the human Xi, the mouse Xist localizes normally. In both cases no silencing of X-linked genes was observed. To verify this hybrid cell system as a model for studying the effects of XIST/Xist independent of inactivation, I examined the DNA methylation, H3 acetylation, and gene expression statuses of multiple human and mouse X-linked genes in these hybrids. The results confirm both i) the reactivation of XIST/Xist due to demethylation, and ii) the lack of gene silencing despite the presence of XIST/Xist.

Item Metadata

Title
Studies of XIST and macroH2A1.2 independent of gene silencing : subtitle a unique hybrid cell model system
Creator
Kwok, Edmund
Publisher
University of British Columbia
Date Issued
2002
Description
X chromosome inactivation results in the transcriptional silencing of one of the two X chromosomes present in mammalian female cells. XIST expression from the inactive X (Xi), and subsequent coating of the Xi by the XIST RNA, marks the initial major observable characteristic of X-inactivation. The Xi then begins to exhibit features of heterochromatin such as gene silencing, late replication, histone modification, hypermethylation, and the recruitment of core histone variants. However, the exact mechanistic events between XIST expression and the final heterochromatic state of the Xi remain unclear. To better understand the relationship between XIST, heterochromatin, and silenced gene expression, the first goal of this study was to develop and characterize a model system suitable for examination of those features of heterochromatin which can be induced by XIST independent of gene silencing. Previous work using rodent/human hybrids (containing active human and mouse X chromosomes) that had been demethylated to reactivate XIST/Xist expression showed that while human XIST RNA fails to localize properly to the human Xi, the mouse Xist localizes normally. In both cases no silencing of X-linked genes was observed. To verify this hybrid cell system as a model for studying the effects of XIST/Xist independent of inactivation, I examined the DNA methylation, H3 acetylation, and gene expression statuses of multiple human and mouse X-linked genes in these hybrids. The results confirm both i) the reactivation of XIST/Xist due to demethylation, and ii) the lack of gene silencing despite the presence of XIST/Xist.
Extent
9600883 bytes
Genre
Thesis/Dissertation
Type
Text
File Format
application/pdf
Language
eng
Date Available
2009-09-16
Provider
Vancouver : University of British Columbia Library
Rights
For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use.
DOI
10.14288/1.0099696
URI
http://hdl.handle.net/2429/12829
Degree
Master of Science - MSc
Program
Medical Genetics
Affiliation
Medicine, Faculty of; Medical Genetics, Department of
Degree Grantor
University of British Columbia
Graduation Date
2002-11
Campus
UBCV
Scholarly Level
Graduate
Aggregated Source Repository
DSpace

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For non-commercial purposes only, such as research, private study and education. Additional conditions apply, see Terms of Use https://open.library.ubc.ca/terms_of_use.