A novel RING-finger-like protein Ini1 is essential for cell cycle progression in fission yeast

Author:

Oltra Elisa1,Verde Fulvia1,Werner Rudolf1,D'Urso Gennaro1

Affiliation:

1. Department of Biochemistry and Molecular Biology, University of Miami School of Medicine, PO Box 016129, Miami, Florida 33101-1019, USA

Abstract

We have cloned a fission yeast (Schizosaccharomyces pombe) homologue of Ini, a novel RING-finger-like protein recently identified in rat that interacts with the connexin43 (cx43) promoter and might be important for the response of the cx43 gene to estrogen. S. pombe cells deleted for ini1+ fail to form colonies and arrest with an elongated cell phenotype, indicating a cell cycle block. Cell cycle arrest is dependent on expression of Wee1, but not Rad3, suggesting that it occurs independently of the DNA damage checkpoint control. Analysis of mRNA intermediates in cells depleted for Ini1 demonstrates that Ini1 is required for pre-mRNA splicing. We observe an accumulation of pre-mRNA for six of seven genes analysed, suggesting that Ini1 is required for general splicing activity. Interestingly, loss of Ini1 results in cell death that is partially suppressed by elimination of the Wee1 kinase. Therefore, Wee1 might promote cell death in the absence of Ini1.

Publisher

The Company of Biologists

Subject

Cell Biology

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