Abstract

The vast majority of human genes require RNA splicing for their expression, and at least 15% of the mutations that cause human diseases do so by disrupting splicing. The long term objective of this project remains: to understand the basis of RNA splicing specificity - the nature of the sequences in primary transcripts which are recognized by the RNA splicing machinery and used in the selection of splice sites in vertebrates and other organisms. This long-term objective is focused on four shorter-term aims: 1) to systematically identify sequences that can act as intronic splicing enhancer (ISE) and silencer (ISS) elements, to refine our knowledge of exonic splicing enhancer (ESE) and silencer (ESS) elements, and to determine rules for the context-dependent activity of these elements;2) to identify the trans-acting factors responsible for the splicing regulatory activity of a significant proportion of the exonic splicing regulatory elements identified previously;3) to develop and apply high-throughput technologies to map changes in expression of spliced isoforms that occur genome-wide during development and in response to external stimuli, using the murine hematopoietic system as a model;4) to determine functional relationships - additivity, sub-additivity, synergism, etc. - between different classes of splicing regulatory elements, to develop associated scoring systems to improve algorithms that simulate splicing and predict splicing phenotypes of mutations or polymorphisms in human genes. In addressing these questions, we will use a synergistic combination of computational methods with molecular genetic and functional genomic approaches. Knowledge of splicing regulatory sequences and proteins will aid in understanding the changes that occur in the expression of RNA versions (isoforms) of genes as cells proliferate, and may identify specific protein or RNA targets for therapuetic intervention in hyperproliferative diseases of the blood such as leukemias, lymphomas and autoimmune diseases. The ability to accurately simulate splicing will enable improved genome annotation and will facilitate identification of specific genes, mutations and polymorphisms associated with human diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Research Project (R01)
Project #
5R01HG002439-09
Application #
7768485
Study Section
Genomics, Computational Biology and Technology Study Section (GCAT)
Program Officer
Good, Peter J
Project Start
2002-02-06
Project End
2011-08-31
Budget Start
2010-02-01
Budget End
2011-08-31
Support Year
9
Fiscal Year
2010
Total Cost
$404,089
Indirect Cost

  Institution

Name
Massachusetts Institute of Technology
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
001425594
City
Cambridge
State
MA
Country
United States
Zip Code
02139

  Publications

Pai, Athma A; Henriques, Telmo; McCue, Kayla et al. (2017) The kinetics of pre-mRNA splicing in the Drosophila genome and the influence of gene architecture. Elife 6:
Taliaferro, J Matthew; Lambert, Nicole J; Sudmant, Peter H et al. (2016) RNA Sequence Context Effects Measured In Vitro Predict In Vivo Protein Binding and Regulation. Mol Cell 64:294-306
Taliaferro, J Matthew; Vidaki, Marina; Oliveira, Ruan et al. (2016) Distal Alternative Last Exons Localize mRNAs to Neural Projections. Mol Cell 61:821-33
Merkin, Jason J; Chen, Ping; Alexis, Maria S et al. (2015) Origins and impacts of new mammalian exons. Cell Rep 10:1992-2005
Katz, Yarden; Wang, Eric T; Silterra, Jacob et al. (2015) Quantitative visualization of alternative exon expression from RNA-seq data. Bioinformatics 31:2400-2
Lambert, Nicole; Robertson, Alex; Jangi, Mohini et al. (2014) RNA Bind-n-Seq: quantitative assessment of the sequence and structural binding specificity of RNA binding proteins. Mol Cell 54:887-900
Shalgi, Reut; Hurt, Jessica A; Krykbaeva, Irina et al. (2013) Widespread regulation of translation by elongation pausing in heat shock. Mol Cell 49:439-52
Spies, Noah; Burge, Christopher B; Bartel, David P (2013) 3' UTR-isoform choice has limited influence on the stability and translational efficiency of most mRNAs in mouse fibroblasts. Genome Res 23:2078-90
Han, Hong; Irimia, Manuel; Ross, P Joel et al. (2013) MBNL proteins repress ES-cell-specific alternative splicing and reprogramming. Nature 498:241-5
Hurt, Jessica A; Robertson, Alex D; Burge, Christopher B (2013) Global analyses of UPF1 binding and function reveal expanded scope of nonsense-mediated mRNA decay. Genome Res 23:1636-50

Showing the most recent 10 out of 30 publications