Alternative splicing in the human transcriptome: Functional and structural influence on proteins
- đ¤ Speaker: Dr. Kei Yura, Quantum Bioinformatics Team, Japan Atomic Energy Agency, Kyoto, Japan
- đ Date & Time: Wednesday 12 September 2007, 13:00 - 14:00
- đ Venue: Bateson Room, Department of Genetics
Abstract
Alternative splicing is a molecular mechanism that produces multiple proteins from a single gene, and is thought to produce variety in proteins translated from a limited number of genes. Here we analyzed how alternative splicing produced variety in protein structure and function, by using human full-length cDNAs on the assumption that all of the alternatively spliced mRNAs were translated to proteins. We found that the length of alternatively spliced amino acid sequences, in most cases, fell into a size shorter than that of average protein domain. We evaluated comprehensively the presumptive three-dimensional structures of the alternatively spliced products to assess the impact of alternative splicing on gene function. We found that more than half of the products encoded proteins which were involved in signal transduction, transcription and translation, and more than half of alternatively spliced regions comprised interaction sites between proteins and their binding partners, including substrates, DNA /RNA, and other proteins. Intriguingly, 67% of the alternatively spliced isoforms showed significant alterations to regions of the protein structural core, which likely resulted in large conformational change. Based on those findings, we speculate that there are a large number of cases that alternative splicing modulates protein networks through significant alteration in protein conformation.
Series This talk is part of the Genetics Seminar Series series.
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Dr. Kei Yura, Quantum Bioinformatics Team, Japan Atomic Energy Agency, Kyoto, Japan
Wednesday 12 September 2007, 13:00-14:00