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Snf1激酶连接了控制酿酒酵母减数分裂的营养途径。

Snf1 kinase connects nutritional pathways controlling meiosis in Saccharomyces cerevisiae.

作者信息

Honigberg S M, Lee R H

机构信息

Department of Biology, Syracuse University, Syracuse, New York 13244-1270, USA.

出版信息

Mol Cell Biol. 1998 Aug;18(8):4548-55. doi: 10.1128/MCB.18.8.4548.

DOI:10.1128/MCB.18.8.4548
PMID:9671464
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC109040/
Abstract

Glucose inhibits meiosis in Saccharomyces cerevisiae at three different steps (IME1 transcription, IME2 transcription, and entry into late stages of meiosis). Because many of the regulatory effects of glucose in yeast are mediated through the inhibition of Snf1 kinase, a component of the glucose repression pathway, we determined the role of SNF1 in regulating meiosis. Deleting SNF1 repressed meiosis at the same three steps that were inhibited by glucose, suggesting that glucose blocks meiosis by inhibiting Snf1. For example, the snf1Delta mutant completely failed to induce IME1 transcripts in sporulation medium. Furthermore, even when this block was bypassed by expression of IME1 from a multicopy plasmid, IME2 transcription and meiotic initiation occurred at only 10 to 20% of the levels seen in wild-type cells. The addition of glucose did not further inhibit IME2 transcription, suggesting that Snf1 is the primary mediator of glucose controls on IME2 expression. Finally, in snf1Delta cells in which both blocks on meiotic initiation were bypassed, early stages of meiosis (DNA replication and commitment to recombination) occurred, but later stages (chromosome segregation and spore formation) did not, suggesting that Snf1 controls later stages of meiosis independently from the two controls on meiotic initiation. Because Snf1 is known to activate the expression of genes required for acetate metabolism, it may also serve to connect glucose and acetate controls on meiotic differentiation.

摘要

葡萄糖在三个不同步骤抑制酿酒酵母的减数分裂(IME1转录、IME2转录以及进入减数分裂后期)。由于酵母中葡萄糖的许多调节作用是通过抑制葡萄糖阻遏途径的一个组分Snf1激酶介导的,我们确定了SNF1在调节减数分裂中的作用。缺失SNF1在被葡萄糖抑制的相同三个步骤抑制减数分裂,这表明葡萄糖通过抑制Snf1来阻断减数分裂。例如,snf1Delta突变体在孢子形成培养基中完全无法诱导IME1转录本。此外,即使通过多拷贝质粒表达IME1绕过了这一阻断,IME2转录和减数分裂起始也仅为野生型细胞中所见水平的10%至20%。添加葡萄糖并未进一步抑制IME2转录,这表明Snf1是葡萄糖对IME2表达控制的主要介导因子。最后,在绕过了减数分裂起始的两个阻断的snf1Delta细胞中,减数分裂的早期阶段(DNA复制和对重组的启动)发生了,但后期阶段(染色体分离和孢子形成)未发生,这表明Snf1独立于对减数分裂起始的两个控制来控制减数分裂的后期阶段。由于已知Snf1可激活乙酸代谢所需基因的表达,它也可能用于连接葡萄糖和乙酸对减数分裂分化的控制。

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