genome-wide identification of alternatively spliced mrna targets of specific rna-binding proteins全基因组的识别或者拼接mrna的目标特定的rna结合蛋白.pdfVIP
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genome-wide identification of alternatively spliced mrna targets of specific rna-binding proteins全基因组的识别或者拼接mrna的目标特定的rna结合蛋白
Genome-Wide Identification of Alternatively Spliced
mRNA Targets of Specific RNA-Binding Proteins
Mark D. Robida, Andrew Rahn, Ravinder Singh*
Department of Molecular, Cellular and Developmental Biology, University of Colorado at Boulder, Boulder, Colorado, United States of America
Background. Alternative splicing plays an important role in generating molecular and functional diversity in multi-cellular
organisms. RNA binding proteins play crucial roles in modulating splice site choice. The majority of known binding sites for
regulatory proteins are short, degenerate consensus sequences that occur frequently throughout the genome. This poses an
important challenge to distinguish between functionally relevant sequences and a vast array of those occurring by chance.
Methodology/Principal Findings. Here we have used a computational approach that combines a series of biological
constraints to identify uridine-rich sequence motifs that are present within relevant biological contexts and thus are potential
targets of the Drosophila master sex-switch protein Sex-lethal (SXL). This strategy led to the identification of one novel target.
Moreover, our systematic analysis provides a starting point for the molecular and functional characterization of an additional
target, which is dependent on SXL activity, either directly or indirectly, for regulation in a germline-specific manner.
Conclusions/Significance. This approach has successfully identified previously known, new, and potential SXL targets. Our
analysis suggests that only a subset of potential SXL sites are regulated by SXL. Finally, this approach should be directly
relevant to the large majority of splicing regulatory proteins for which bonafide targets are unknown.
Citation: Robida MD, Rahn A, Singh R (2007) Genome-Wide Identification of Alternatively Spli
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