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Prp4 Kinase Grants the License to Splice: Control of Weak Splice Sites during Spliceosome Activation.


ABSTRACT: The genome of the fission yeast Schizosaccharomyces pombe encodes 17 kinases that are essential for cell growth. These include the cell-cycle regulator Cdc2, as well as several kinases that coordinate cell growth, polarity, and morphogenesis during the cell cycle. In this study, we further characterized another of these essential kinases, Prp4, and showed that the splicing of many introns is dependent on Prp4 kinase activity. For detailed characterization, we chose the genes res1 and ppk8, each of which contains one intron of typical size and position. Splicing of the res1 intron was dependent on Prp4 kinase activity, whereas splicing of the ppk8 intron was not. Extensive mutational analyses of the 5' splice site of both genes revealed that proper transient interaction with the 5' end of snRNA U1 governs the dependence of splicing on Prp4 kinase activity. Proper transient interaction between the branch sequence and snRNA U2 was also important. Therefore, the Prp4 kinase is required for recognition and efficient splicing of introns displaying weak exon1/5' splice sites and weak branch sequences.

SUBMITTER: Eckert D 

PROVIDER: S-EPMC4701394 | biostudies-literature | 2016 Jan

REPOSITORIES: biostudies-literature

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Prp4 Kinase Grants the License to Splice: Control of Weak Splice Sites during Spliceosome Activation.

Eckert Daniela D   Andrée Nicole N   Razanau Aleh A   Zock-Emmenthal Susanne S   Lützelberger Martin M   Plath Susann S   Schmidt Henning H   Guerra-Moreno Angel A   Cozzuto Luca L   Ayté José J   Käufer Norbert F NF  

PLoS genetics 20160105 1


The genome of the fission yeast Schizosaccharomyces pombe encodes 17 kinases that are essential for cell growth. These include the cell-cycle regulator Cdc2, as well as several kinases that coordinate cell growth, polarity, and morphogenesis during the cell cycle. In this study, we further characterized another of these essential kinases, Prp4, and showed that the splicing of many introns is dependent on Prp4 kinase activity. For detailed characterization, we chose the genes res1 and ppk8, each  ...[more]

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