Literature DB >> 15802507

Subdivision of large introns in Drosophila by recursive splicing at nonexonic elements.

James M Burnette1, Etsuko Miyamoto-Sato, Marc A Schaub, Jamie Conklin, A Javier Lopez.   

Abstract

Many genes with important roles in development and disease contain exceptionally long introns, but special mechanisms for their expression have not been investigated. We present bioinformatic, phylogenetic, and experimental evidence in Drosophila for a mechanism that subdivides many large introns by recursive splicing at nonexonic elements and alternative exons. Recursive splice sites predicted with highly stringent criteria are found at much higher frequency than expected in the sense strands of introns >20 kb, but they are found only at the expected frequency on the antisense strands, and they are underrepresented within introns <10 kb. The predicted sites in long introns are highly conserved between Drosophila melanogaster and Drosophila pseudoobscura, despite extensive divergence of other sequences within the same introns. These patterns of enrichment and conservation indicate that recursive splice sites are advantageous in the context of long introns. Experimental analyses of in vivo processing intermediates and lariat products from four large introns in the unrelated genes kuzbanian, outspread, and Ultrabithorax confirmed that these introns are removed by a series of recursive splicing steps using the predicted nonexonic sites. Mutation of nonexonic site RP3 within Ultrabithorax also confirmed that recursive splicing is the predominant processing pathway even with a shortened version of the intron. We discuss currently known and potential roles for recursive splicing.

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Year:  2005        PMID: 15802507      PMCID: PMC1450422          DOI: 10.1534/genetics.104.039701

Source DB:  PubMed          Journal:  Genetics        ISSN: 0016-6731            Impact factor:   4.562


  41 in total

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Authors:  A M Reugels; R Kurek; U Lammermann; H Bünemann
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7.  Molecular aspects of intron evolution in dynein encoding mega-genes on the heterochromatic Y chromosome of Drosophila sp.

Authors:  R Kurek; A M Reugels; U Lammermann; H Bünemann
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8.  Human genomic sequences that inhibit splicing.

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9.  The correlation between intron length and recombination in drosophila. Dynamic equilibrium between mutational and selective forces.

Authors:  J M Comeron; M Kreitman
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10.  Alternative RNA products from the Ultrabithorax domain of the bithorax complex.

Authors:  M B O'Connor; R Binari; L A Perkins; W Bender
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  62 in total

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4.  Identification of seven novel cryptic exons embedded in the dystrophin gene and characterization of 14 cryptic dystrophin exons.

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6.  A nonsense exon in the Tpm1 gene is silenced by hnRNP H and F.

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7.  Dynamic reconfiguration of long human genes during one transcription cycle.

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8.  Mathematical modeling identifies potential gene structure determinants of co-transcriptional control of alternative pre-mRNA splicing.

Authors:  Jeremy Davis-Turak; Tracy L Johnson; Alexander Hoffmann
Journal:  Nucleic Acids Res       Date:  2018-11-16       Impact factor: 16.971

9.  The peculiarities of large intron splicing in animals.

Authors:  Samuel Shepard; Mark McCreary; Alexei Fedorov
Journal:  PLoS One       Date:  2009-11-16       Impact factor: 3.240

10.  Rates of in situ transcription and splicing in large human genes.

Authors:  Jarnail Singh; Richard A Padgett
Journal:  Nat Struct Mol Biol       Date:  2009-10-11       Impact factor: 15.369

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