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与vps8 - 200的基因相互作用可部分抑制酿酒酵母中pep5突变引起的小液泡表型。

Genetic interaction with vps8-200 allows partial suppression of the vestigial vacuole phenotype caused by a pep5 mutation in Saccharomyces cerevisiae.

作者信息

Woolford C A, Bounoutas G S, Frew S E, Jones E W

机构信息

Department of Biological Sciences, Carnegie Mellon University, Pittsburgh, Pennsylvania 15213, USA.

出版信息

Genetics. 1998 Jan;148(1):71-83. doi: 10.1093/genetics/148.1.71.

Abstract

pep5 mutants of Saccharomyces cerevisiae accumulate inactive precursors to the vacuolar hydrolases. In addition, they show a vestigial vacuole morphology and a sensitivity to growth on media containing excess divalent cations. This pleiotropic phenotype observed for pep5::TRP1 mutants is partially suppressed by the vps8-200 allele. pep5::TRP1 vps8-200 mutants show near wild-type levels of mature-sized soluble vacuolar hydrolases, growth on zinc-containing medium, and a more "wild-type" vacuolar morphology; however, aminopeptidase I and alkaline phosphatase accumulate as precursors. These data suggest that Pep5p is a bifunctional protein and that the TRP1 insertion does not eliminate function, but results in a shorter peptide that can interact with Vps8-200p, allowing for partial function. vps8 deletion/disruption mutants contain a single enlarged vacuole. This genetic interaction was unexpected, since Pep5p was thought to interact more directly with the vacuole, and Vps8p is thought to play a role in transport between the Golgi complex and the prevacuolar compartment. The data are consistent with Pep5p functioning both at the site of Vps8p function and more closely proximal to the vacuole. They also provide evidence that the three transport pathways to the vacuole either converge or share gene products at late step(s) in the pathway(s).

摘要

酿酒酵母的pep5突变体积累了液泡水解酶的无活性前体。此外,它们表现出残余的液泡形态,并且对含有过量二价阳离子的培养基上的生长敏感。对于pep5::TRP1突变体观察到的这种多效性表型被vps8 - 200等位基因部分抑制。pep5::TRP1 vps8 - 200突变体显示出接近野生型水平的成熟大小的可溶性液泡水解酶,在含锌培养基上生长,以及更“野生型”的液泡形态;然而,氨肽酶I和碱性磷酸酶以前体形式积累。这些数据表明Pep5p是一种双功能蛋白,并且TRP1插入并没有消除功能,而是导致了一种更短的肽,该肽可以与Vps8 - 200p相互作用,从而实现部分功能。vps8缺失/破坏突变体含有单个增大的液泡。这种遗传相互作用是出乎意料的,因为Pep5p被认为更直接地与液泡相互作用,而Vps8p被认为在高尔基体复合体和前液泡区室之间的运输中起作用。数据与Pep5p在Vps8p功能位点以及更靠近液泡的位置发挥作用一致。它们还提供了证据,表明通向液泡的三条运输途径在途径的后期步骤中要么汇聚要么共享基因产物。

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