Alternative splicing networks regulated by signaling in human T cells
0301 basic medicine
Sequence Analysis, RNA
Gene Expression Profiling
T-Lymphocytes
Receptors, Antigen, T-Cell
Computational Biology
Exons
Lymphocyte Activation
Cell Line
3. Good health
Alternative Splicing
03 medical and health sciences
Gene Expression Regulation
Humans
RNA, Messenger
Nucleotide Motifs
Signal Transduction
DOI:
10.1261/rna.032243.112
Publication Date:
2012-03-28T04:30:24Z
AUTHORS (10)
ABSTRACT
The formation and execution of a productive immune response requires the maturation of competent T cells and a robust change in cellular activity upon antigen challenge. Such changes in cellular function depend on regulated alterations to protein expression. Previous research has focused on defining transcriptional changes that regulate protein expression during T-cell maturation and antigen stimulation. Here, we globally analyze another critical process in gene regulation during T-cell stimulation, alternative splicing. Specifically, we use RNA-seq profiling to identify 178 exons in 168 genes that exhibit robust changes in inclusion in response to stimulation of a human T-cell line. Supporting an important role for the global coordination of alternative splicing following T-cell stimulation, these signal-responsive exons are significantly enriched in genes with functional annotations specifically related to immune response. The vast majority of these genes also exhibit differential alternative splicing between naive and activated primary T cells. Comparison of the responsiveness of splicing to various stimuli in the cultured and primary T cells further reveals at least three distinct networks of signal-induced alternative splicing events. Importantly, we find that each regulatory network is specifically associated with distinct sequence features, suggesting that they are controlled by independent regulatory mechanisms. These results thus provide a basis for elucidating mechanisms of signal pathway–specific regulation of alternative splicing during T-cell stimulation.
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