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首页> 外文期刊>Molecular and Cellular Biology >Far3 and Five Interacting Proteins Prevent Premature Recovery from Pheromone Arrest in the Budding Yeast Saccharomyces cerevisiae
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Far3 and Five Interacting Proteins Prevent Premature Recovery from Pheromone Arrest in the Budding Yeast Saccharomyces cerevisiae

机译:Far3和5种相互作用的蛋白质可防止酵母发酵酵母中信息素被捕过早地恢复

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摘要

In budding yeast, diffusible mating pheromones initiate a signaling pathway that culminates in several responses, including cell cycle arrest. Only a handful of genes required for the interface between pheromone response and the cell cycle have been identified, among them FAR1 and FAR3; of these, only FAR1 has been extensively characterized. In an effort to learn about the mechanism by which Far3 acts, we used the two-hybrid method to identify interacting proteins. We identified five previously uncharacterized open reading frames, dubbed FAR7, FAR8, FAR9, FAR10, and FAR11, that cause a far3-like pheromone arrest defect when disrupted. Using two-hybrid and coimmunoprecipitation analysis, we found that all six Far proteins interact with each other. Moreover, velocity sedimentation experiments suggest that Far3 and Far7 to Far11 form a complex. The phenotype of a sextuple far3far7-far11 mutant is no more severe than any single mutant. Thus, FAR3 and FAR7 to FAR11 all participate in the same pathway leading to G1 arrest. These mutants initially arrest in response to pheromone but resume budding after 10 h. Under these conditions, wild-type cells fail to resume budding even after several days whereas far1 mutant cells resume budding within 1 h. We conclude that the FAR3-dependent arrest pathway is functionally distinct from that which employs FAR1.
机译:在发芽的酵母中,可扩散的交配信息素启动一个信号通路,最终达到多种反应,包括细胞周期停滞。仅鉴定了少数几个信息素应答与细胞周期之间的接口基因,其中包括 FAR1 FAR3 。其中,只有 FAR1 被广泛表征。为了了解Far3发挥作用的机制,我们使用了两种杂交方法来识别相互作用的蛋白质。我们确定了五个以前没有特征的开放阅读框,分别称为 FAR7 FAR8 FAR9 FAR10 FAR11 ,当被破坏时会导致类似 far3 的信息素​​停滞缺陷。使用两杂交和共免疫沉淀分析,我们发现所有六个Far蛋白彼此相互作用。此外,速度沉降实验表明,Far3和Far7至Far11形成复合物。一个六元组 far3far7-far11 突变体的表型并不比任何单个突变体严重。因此, FAR3 FAR7 FAR11 都参与同一条导致G 1 逮捕的途径。这些突变体最初对信息素起反应而停止,但在10小时后恢复萌芽。在这种条件下,即使几天后野生型细胞也无法恢复萌芽,而 far1 突变细胞却在1小时内恢复萌芽。我们得出的结论是, FAR3 依赖的逮捕途径在功能上不同于采用 FAR1 的途径。

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