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酿酒酵母中需要DNA拓扑异构酶I的突变体的分离

Isolation of mutants of Saccharomyces cerevisiae requiring DNA topoisomerase I.

作者信息

Sadoff B U, Heath-Pagliuso S, Castaño I B, Zhu Y, Kieff F S, Christman M F

机构信息

Department of Radiation Oncology, University of California, San Francisco 94143, USA.

出版信息

Genetics. 1995 Oct;141(2):465-79. doi: 10.1093/genetics/141.2.465.

Abstract

Despite evidence that DNA topoisomerase I is required to relieve torsional stress during DNA replication and transcription, yeast strains with a top1 null mutation are viable and display no gross defects in DNA or RNA synthesis, possibly because other proteins provide overlapping functions. We isolated mutants whose inviablility or growth defect is relieved when TOP1 is expressed [trf mutants (topoisomerase one-requiring function)]. The TRF genes define at least four complementation groups. TRF3 is allelic to TOP2. TRF1 is allelic to HPR1, previously shown to be homologous to TOP1 over two short regions. TRF4 encodes a novel 584-amino acid protein with homology to the N-terminus of Saccharomyces cerevisiae topo I. Like top1 mutants, trf4 mutants have elevated rDNA recombination and fail to shut off RNA polymerase II transcription in stationary phase. trf4 null mutants are cs for viability, display reduced expression of GAL1 and Cell Cycle Box UAS::LacZ fusions, and are inviable in combination with trfI null mutants, indicating that both proteins may share a common function with DNA topoisomerase I. The existence of multiple TRF complementation groups suggests that not all biological functions of topo I can be carried out by topo II.

摘要

尽管有证据表明DNA拓扑异构酶I在DNA复制和转录过程中对于缓解扭转应力是必需的,但具有top1缺失突变的酵母菌株仍可存活,并且在DNA或RNA合成中未表现出明显缺陷,这可能是因为其他蛋白质具有重叠功能。我们分离出了一些突变体,当表达TOP1时,它们的不可存活或生长缺陷得以缓解[trf突变体(拓扑异构酶一依赖功能)]。TRF基因至少定义了四个互补群。TRF3与TOP2等位。TRF1与HPR1等位,先前已证明HPR1在两个短区域与TOP1同源。TRF4编码一种新型的584个氨基酸的蛋白质,与酿酒酵母拓扑异构酶I的N端具有同源性。与top1突变体一样,trf4突变体的rDNA重组增加,并且在稳定期无法关闭RNA聚合酶II转录。trf4缺失突变体的生存能力为cs,GAL1和细胞周期框UAS::LacZ融合蛋白的表达降低,并且与trfI缺失突变体组合时不可存活,这表明这两种蛋白质可能与DNA拓扑异构酶I具有共同功能。多个TRF互补群的存在表明,拓扑异构酶I的并非所有生物学功能都可由拓扑异构酶II执行。

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