Biased exon/intron distribution of cryptic and de novo 3' splice sites
Biased exon/intron distribution of cryptic and de novo 3' splice sites
We compiled sequences of previously published aberrant 3' splice sites (3'ss) that were generated by mutations in human disease genes. Cryptic 3'ss, defined here as those resulting from a mutation of the 3'YAG consensus, were more frequent in exons than in introns. They clustered in ~20 nt region adjacent to authentic 3'ss, suggesting that their under-representation in introns is due to a depletion of AG dinucleotides in the polypyrimidine tract (PPT). In contrast, most aberrant 3'ss that were induced by mutations outside the 3'YAG consensus (designated ‘de novo’) were in introns. The activation of intronic de novo 3'ss was largely due to AG-creating mutations in the PPT. In contrast, exonic de novo 3'ss were more often induced by mutations improving the PPT, branchpoint sequence (BPS) or distant auxiliary signals, rather than by direct AG creation. The Shapiro–Senapathy matrix scores had a good prognostic value for cryptic, but not de novo 3'ss. Finally, AG-creating mutations in the PPT that produced aberrant 3'ss upstream of the predicted BPS in vivo shared a similar ‘BPS-new AG’ distance. Reduction of this distance and/or the strength of the new AG PPT in splicing reporter pre-mRNAs improved utilization of authentic 3'ss, suggesting that AG-creating mutations that are located closer to the BPS and are preceded by weaker PPT may result in less severe splicing defects.
4882-4898
Královičová, Jana
b3e0c1e7-05ed-445d-b3d9-ace11e3b4878
Christensen, Mikkel B.
0cc34863-5f5a-4b99-819c-bfee76aac294
Vořechovský, Igor
7245de2f-8c9b-4034-8935-9a451d9b682e
2005
Královičová, Jana
b3e0c1e7-05ed-445d-b3d9-ace11e3b4878
Christensen, Mikkel B.
0cc34863-5f5a-4b99-819c-bfee76aac294
Vořechovský, Igor
7245de2f-8c9b-4034-8935-9a451d9b682e
Královičová, Jana, Christensen, Mikkel B. and Vořechovský, Igor
(2005)
Biased exon/intron distribution of cryptic and de novo 3' splice sites.
Nucleic Acids Research, 33 (15), .
(doi:10.1093/nar/gki811).
Abstract
We compiled sequences of previously published aberrant 3' splice sites (3'ss) that were generated by mutations in human disease genes. Cryptic 3'ss, defined here as those resulting from a mutation of the 3'YAG consensus, were more frequent in exons than in introns. They clustered in ~20 nt region adjacent to authentic 3'ss, suggesting that their under-representation in introns is due to a depletion of AG dinucleotides in the polypyrimidine tract (PPT). In contrast, most aberrant 3'ss that were induced by mutations outside the 3'YAG consensus (designated ‘de novo’) were in introns. The activation of intronic de novo 3'ss was largely due to AG-creating mutations in the PPT. In contrast, exonic de novo 3'ss were more often induced by mutations improving the PPT, branchpoint sequence (BPS) or distant auxiliary signals, rather than by direct AG creation. The Shapiro–Senapathy matrix scores had a good prognostic value for cryptic, but not de novo 3'ss. Finally, AG-creating mutations in the PPT that produced aberrant 3'ss upstream of the predicted BPS in vivo shared a similar ‘BPS-new AG’ distance. Reduction of this distance and/or the strength of the new AG PPT in splicing reporter pre-mRNAs improved utilization of authentic 3'ss, suggesting that AG-creating mutations that are located closer to the BPS and are preceded by weaker PPT may result in less severe splicing defects.
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Published date: 2005
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Local EPrints ID: 24813
URI: http://eprints.soton.ac.uk/id/eprint/24813
ISSN: 0305-1048
PURE UUID: dcb7f80b-3152-4959-9f53-090e782c5ad7
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Date deposited: 03 Apr 2006
Last modified: 16 Mar 2024 03:32
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Author:
Jana Královičová
Author:
Mikkel B. Christensen
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