Department of Molecular Biology, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, CA 92037, USA.
Yeast. 2012 Oct;29(10):425-34. doi: 10.1002/yea.2920. Epub 2012 Sep 12.
The ability to regulate the expression of a gene greatly aids the process of uncovering its functions. The fission yeast Schizosaccharomyces pombe has so far lacked a system for rapidly controlling the expression of chromosomal genes, hindering its full potential as a model organism. Although the widely used nmt1 promoter displays a wide dynamic range of activity, it takes > 14-15 h to derepress. The urg1 promoter also shows a large dynamic range and can be induced quickly (< 2 h), but its implementation requires laborious strain construction and it cannot be used to study meiosis. To overcome these limitations, we constructed a tetracycline-regulated system for inducible expression of chromosomal genes in fission yeast, which is easily established and implemented. In this system the promoter of a gene is replaced by simple one-step substitution techniques with a tetracycline-regulated promoter cassette (tetO(7) -TATA(CYC1) ) in cells where TetR/TetR'-based transcription activators/repressors are also produced. Using top1 and nse6 as reporter genes, we show that Top1 and Nse6 appear after just 30 min of activating tetO(7) -TATA(CYC1) and plateau after -4-6 h. The amount of synthesised protein is comparable to that produced from the attenuated nmt1 promoter P(nmt8) , which should be closer to wild-type levels for most genes than those generated from excessively strong promoters and can be controlled by changing the concentration of the effector antibiotic. This system also works efficiently during meiosis, thus making it a useful addition to the toolkit of the fission yeast community.
调控基因表达的能力极大地帮助了揭示基因功能的过程。裂殖酵母 Schizosaccharomyces pombe 迄今为止缺乏一种快速控制染色体基因表达的系统,这阻碍了其作为模式生物的全部潜力。尽管广泛使用的 nmt1 启动子显示出广泛的活性范围,但它需要超过 14-15 小时才能去抑制。urg1 启动子也显示出较大的动态范围并且可以快速诱导(<2 小时),但它的实现需要艰苦的菌株构建,并且不能用于研究减数分裂。为了克服这些限制,我们构建了裂殖酵母中染色体基因诱导表达的四环素调控系统,该系统易于建立和实施。在该系统中,通过简单的一步取代技术,用四环素调控启动子盒(tetO(7) -TATA(CYC1))替换基因的启动子,在细胞中还产生 TetR/TetR'-基于转录激活剂/抑制剂。使用 top1 和 nse6 作为报告基因,我们表明,在激活 tetO(7) -TATA(CYC1) 30 分钟后即可出现 Top1 和 Nse6,并在-4-6 小时后达到平台期。合成的蛋白质量与从衰减的 nmt1 启动子 P(nmt8)产生的蛋白质量相当,对于大多数基因而言,这应该比从过度强的启动子产生的蛋白质更接近野生型水平,并且可以通过改变效应抗生素的浓度来控制。该系统在减数分裂期间也能有效工作,因此成为裂殖酵母社区工具包的有用补充。