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Series GSE27199 Query DataSets for GSE27199
Status Public on Nov 01, 2011
Title Genome-wide consequences of compromised NMD and their relavence for variable clinical phenotype of patients with UPF3B mutations [RNA-seq]
Organism Homo sapiens
Experiment type Expression profiling by high throughput sequencing
Summary Nonsense-mediated mRNA decay (NMD) surveillance pathways are best known to be involved in the degradation of mRNA with premature termination codons (PTCs). More recent studies demonstrate that the role of NMD pathways goes well beyond the degradation of PTC containing mRNA, into the regulation of cell function and thus normal development.
We have taken advantage of the availability of naturally occurring loss of function mutations in the UPF3B gene, a major component of the exon junction complex (EJC), to inquire about genome-wide consequences of compromised NMD. We identify that about 5% of the lymphoblastoid cell transcriptome is directly or indirectly impacted upon in patients with UPF3B mutations with minimal effect on alternative splicing. We identify UPF3A-NMD as a likely, major modifier of the UPF3B patient phenotype through variable UPF3A protein stabilisation. Among the most consistently deregulated direct targets of UPF3B-NMD we identify the ARHGAP24 as the most likely gene implicated in the neuronal phenotype of UPF3B patients.
 
Overall design To assess the impact of UPF3B-NMD deficiency on human transcriptome, we sequenced polyA RNA extracted from lymphoblastoid cell lines of patients (n=4) and controls (n=2). We complemented the analysis using Affymetrix Human Exon 1.0 St array using total RNA of the same cell line from patients (n=5, 3 of whom were also sequenced) and controls (n=5). Moreover, we overlapped identified differently expressed genes with copy number variation data of the patients, obtained using Illumina Human Omniexpress chip, to exclude possible false positive.

Supplementary file: A splice junction reference file generated for alignment of junction reads.
Alignment files linked to individual Sample records.
 
Contributor(s) Nguyen LS, Jolly L, Shoubridge C, Chan W, Huang L, Laumonnier F, Raynaud M, Rodriguez J, Srivastava A, Addington AM, Wilkinson MF, Corbett M, Gecz J
Citation(s) 22182939
Submission date Feb 09, 2011
Last update date May 15, 2019
Contact name Jozef Gecz
Organization name SA Pathology
Department Genetics Medicine
Lab Neurogenetics
Street address 72 King William Rd
City North Adelaide
State/province South Australia
ZIP/Postal code 5006
Country Australia
 
Platforms (1)
GPL9115 Illumina Genome Analyzer II (Homo sapiens)
Samples (6)
GSM672020 Patient 1 [RNA-Seq]
GSM672021 Patient 2 [RNA-Seq]
GSM672022 Patient 3 [RNA-Seq]
This SubSeries is part of SuperSeries:
GSE27433 Genome-wide consequences of compromised NMD and their relavence for variable clinical phenotype of patients with UPF3B mutations
Relations
SRA SRP005899
BioProject PRJNA142073

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE27199_RAW.tar 2.8 Gb (http)(custom) TAR (of TXT)
GSE27199_Splice_Sites_45.fa.txt.gz 7.7 Mb (ftp)(http) TXT
GSE27199_processed_data.txt.gz 499.4 Kb (ftp)(http) TXT
SRA Run SelectorHelp
Raw data are available in SRA
Processed data provided as supplementary file
Processed data are available on Series record

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