A hyper-recombination mutation in S. cerevisiae identifies a novel eukaryotic topoisomerase

A hyper-recombination mutation was isolated that causes an increase in recombination between short repeated δ sequences surrounding the SUP4-o gene in S. cerevisiae. The wild-type copy of this gene was cloned by complementation of one of its pleiotropic phenotypes, slow growth. DNA sequence of the c...

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Veröffentlicht in:Cell 1989-07, Vol.58 (2), p.409-419
Hauptverfasser: Wallis, John W., Chrebet, Gary, Brodsky, Gary, Rolfe, Mark, Rothstein, Rodney
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Sprache:eng
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Zusammenfassung:A hyper-recombination mutation was isolated that causes an increase in recombination between short repeated δ sequences surrounding the SUP4-o gene in S. cerevisiae. The wild-type copy of this gene was cloned by complementation of one of its pleiotropic phenotypes, slow growth. DNA sequence of the clone revealed a 656 amino acid open reading frame capable of encoding a protein homologous to the bacterial type I topoisomerase. No homology was detected with previously identified eukaryotic topoisomerases. Construction of double mutants with either of the two known yeast topoisomerase genes revealed synergistic effects on growth suggesting overlapping functions. Expression of bacterial topoisomerase I in yeast can fully complement the slow growth defect of a null mutation. We have named this locus TOP3 and suggest that it defines a novel eukaryotic topoisomerase gene.
ISSN:0092-8674
1097-4172
DOI:10.1016/0092-8674(89)90855-6