Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype
Angelman syndrome (AS) is an inheritable neurodevelopmental disorder resulting from the loss of function of the ubiquitin E3A ligase (UBE3A). Clinical features of the disorder include severe mental retardation, motor incoordination and perpetual happy disposition. Associated features of AS include h...
Saved in:
| Main Author: | |
|---|---|
| Other Authors: | |
| Format: | Theses and Dissertations |
| Language: | English |
| Published: |
2012
|
| Subjects: | |
| Online Access: | https://hdl.handle.net/10356/48088 |
| Tags: |
Add Tag
No Tags, Be the first to tag this record!
|
| Institution: | Nanyang Technological University |
| Language: | English |
| id |
sg-ntu-dr.10356-48088 |
|---|---|
| record_format |
dspace |
| spelling |
sg-ntu-dr.10356-480882023-02-28T18:44:41Z Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype Low, Daren Juan Hsuen Chen Ken-Shiung School of Biological Sciences DRNTU::Science::Biological sciences::Genetics Angelman syndrome (AS) is an inheritable neurodevelopmental disorder resulting from the loss of function of the ubiquitin E3A ligase (UBE3A). Clinical features of the disorder include severe mental retardation, motor incoordination and perpetual happy disposition. Associated features of AS include hypopigmentation and seizures. Despite many targets and interacting partners of UBE3A being identified, the detailed pathogenesis of the disorder, as well as how the lack of functional UBE3A upsets cellular homeostasis, remains vague. The aim of this project is to characterize the gene expression profile of the AS mouse model by performing a genome-wide microarray screening to identify differentially expressed genes and to unravel potential genotype-phenotype correlationship mechanisms. Results: Sixty-four differentially expressed genes (7 up-regulated and 57 down-regulated) in the AS mouse cerebellum were identified, which subsequent pathway analysis showed their involvement in 3 major networks including cell signaling, nervous system development and cell death. Representative genes (Fgf7, Glra1, Mc1r, Nr4a2, Slc5a7, Epha6) from each network were selected based on their functional relevance to AS and validated for their differential expression using qRT-PCR. The validation was extended towards the protein level using Western blot for Nr4a2 and Mc1r. Both showed reduction in their respective protein level in the mutant AS mouse. DOCTOR OF PHILOSOPHY (SBS) 2012-03-15T07:36:54Z 2012-03-15T07:36:54Z 2012 2012 Thesis Low, D. J. H. (2012). Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype. Doctoral thesis, Nanyang Technological University, Singapore. https://hdl.handle.net/10356/48088 10.32657/10356/48088 en 133 p. application/pdf |
| institution |
Nanyang Technological University |
| building |
NTU Library |
| continent |
Asia |
| country |
Singapore Singapore |
| content_provider |
NTU Library |
| collection |
DR-NTU |
| language |
English |
| topic |
DRNTU::Science::Biological sciences::Genetics |
| spellingShingle |
DRNTU::Science::Biological sciences::Genetics Low, Daren Juan Hsuen Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype |
| description |
Angelman syndrome (AS) is an inheritable neurodevelopmental disorder resulting from the loss of function of the ubiquitin E3A ligase (UBE3A). Clinical features of the disorder include severe mental retardation, motor incoordination and perpetual happy disposition. Associated features of AS include hypopigmentation and seizures. Despite many targets and interacting partners of UBE3A being identified, the detailed pathogenesis of the disorder, as well as how the lack of functional UBE3A upsets cellular homeostasis, remains vague. The aim of this project is to characterize the gene expression profile of the AS mouse model by performing a genome-wide microarray screening to identify differentially expressed genes and to unravel potential genotype-phenotype correlationship mechanisms. Results: Sixty-four differentially expressed genes (7 up-regulated and 57 down-regulated) in the AS mouse cerebellum were identified, which subsequent pathway analysis showed their involvement in 3 major networks including cell signaling, nervous system development and cell death. Representative genes (Fgf7, Glra1, Mc1r, Nr4a2, Slc5a7, Epha6) from each network were selected based on their functional relevance to AS and validated for their differential expression using qRT-PCR. The validation was extended towards the protein level using Western blot for Nr4a2 and Mc1r. Both showed reduction in their respective protein level in the mutant AS mouse. |
| author2 |
Chen Ken-Shiung |
| author_facet |
Chen Ken-Shiung Low, Daren Juan Hsuen |
| format |
Theses and Dissertations |
| author |
Low, Daren Juan Hsuen |
| author_sort |
Low, Daren Juan Hsuen |
| title |
Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype |
| title_short |
Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype |
| title_full |
Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype |
| title_fullStr |
Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype |
| title_full_unstemmed |
Genome-wide gene expression profiling of the Angelman syndrome mouse with Ube3a mutation : from genotype to phenotype |
| title_sort |
genome-wide gene expression profiling of the angelman syndrome mouse with ube3a mutation : from genotype to phenotype |
| publishDate |
2012 |
| url |
https://hdl.handle.net/10356/48088 |
| _version_ |
1759856530335727616 |