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酿酒酵母gpa1Val50突变体通过默认交配途径进行交配的证据以及泛素介导的蛋白水解作用的暗示。

Evidence that mating by the Saccharomyces cerevisiae gpa1Val50 mutant occurs through the default mating pathway and a suggestion of a role for ubiquitin-mediated proteolysis.

作者信息

Xu B E, Kurjan J

机构信息

Department of Microbiology and Molecular Genetics, University of Vermont, College of Medicine, Burlington, USA.

出版信息

Mol Biol Cell. 1997 Sep;8(9):1649-64. doi: 10.1091/mbc.8.9.1649.

Abstract

The yeast G alpha subunit, Gpa1p, plays a negative role in the pheromone response pathway. The gpa1Val50 mutant was previously shown to have a growth defect, consistent with the GTPase defect predicted for this mutation, and greatly reduced mating. Various explanations for the mating defect have been proposed. One approach to analyze the gpa1Val50 mating defect involved epistasis analysis. The low mating of the gpa1Val50 mutant was independent of the pheromone receptor; therefore, it results from intracellular activation of the pathway, consistent with a GTPase defect. This result suggests that gpa1Val50 mating occurs through the default rather than the chemotropic pathway involved in pheromone response. We therefore tested the effect of a spa2 mutation on gpa1Val50 mating, because Spa2p has been implicated in the default pathway. The spa2 mutation greatly reduced the mating of the gpa1Val50 mutant, suggesting that gpa1Val50 mating occurs predominantly through the default pathway. In a second approach to investigate the gpa1Val50 phenotypes, suppressors of the gpa1Val50 mating defect were isolated. Two suppressor genes corresponded to SON1/UFD5 and SEN3, which are implicated in ubiquitin-mediated proteolysis. On the basis of these results, we suggest that a positive component of the default mating pathway is subject to ubiquitin-mediated degradation.

摘要

酵母Gα亚基Gpa1p在信息素反应途径中起负向作用。gpa1Val50突变体先前已被证明存在生长缺陷,这与该突变预测的GTP酶缺陷一致,且其交配能力大大降低。针对交配缺陷已提出了各种解释。一种分析gpa1Val50交配缺陷的方法涉及上位性分析。gpa1Val50突变体的低交配率与信息素受体无关;因此,它是由该途径的细胞内激活导致的,这与GTP酶缺陷一致。这一结果表明,gpa1Val50的交配是通过默认途径而非信息素反应中涉及的向化性途径发生的。因此,我们测试了spa2突变对gpa1Val50交配的影响,因为Spa2p与默认途径有关。spa2突变大大降低了gpa1Val50突变体的交配率,这表明gpa1Val50的交配主要通过默认途径发生。在研究gpa1Val50表型的第二种方法中,分离出了gpa1Val50交配缺陷的抑制子。两个抑制基因对应于SON1/UFD5和SEN3,它们与泛素介导的蛋白水解有关。基于这些结果,我们认为默认交配途径的一个正向组分受到泛素介导的降解作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f554/305726/f5962ce6cc5d/mbc00111-0013-a.jpg

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