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通过将大肠杆菌UbiF多肽靶向线粒体来互补酿酒酵母coq7突变体:酵母Coq7多肽在辅酶Q生物合成中的两种功能

Complementation of Saccharomyces cerevisiae coq7 mutants by mitochondrial targeting of the Escherichia coli UbiF polypeptide: two functions of yeast Coq7 polypeptide in coenzyme Q biosynthesis.

作者信息

Tran UyenPhuong C, Marbois Beth, Gin Peter, Gulmezian Melissa, Jonassen Tanya, Clarke Catherine F

机构信息

Department of Chemistry and Biochemistry, and Molecular Biology Institute, University of California-Los Angeles, 607 Charles E. Young Drive East, Los Angeles, CA 90095, USA.

出版信息

J Biol Chem. 2006 Jun 16;281(24):16401-9. doi: 10.1074/jbc.M513267200. Epub 2006 Apr 19.

Abstract

Coenzyme Q (ubiquinone or Q) functions in the respiratory electron transport chain and serves as a lipophilic antioxidant. In the budding yeast Saccharomyces cerevisiae, Q biosynthesis requires nine Coq proteins (Coq1-Coq9). Previous work suggests both an enzymatic activity and a structural role for the yeast Coq7 protein. To define the functional roles of yeast Coq7p we test whether Escherichia coli ubiF can functionally substitute for yeast COQ7. The ubiF gene encodes a flavin-dependent monooxygenase that shares no homology to the Coq7 protein and is required for the final monooxygenase step of Q biosynthesis in E. coli. The ubiF gene expressed at low copy restores growth of a coq7 point mutant (E194K) on medium containing a non-fermentable carbon source, but fails to rescue a coq7 null mutant. However, expression of ubiF from a multicopy vector restores growth and Q synthesis for both mutants, although with a higher efficiency in the point mutant. We attribute the more efficient rescue of the coq7 point mutant to higher steady state levels of the Coq3, Coq4, and Coq6 proteins and to the presence of demethoxyubiquinone, the substrate of UbiF. Coq7p co-migrates with the Coq3 and Coq4 polypeptides as a high molecular mass complex. Here we show that addition of Q to the growth media also stabilizes the Coq3 and Coq4 polypeptides in the coq7 null mutant. The data suggest that Coq7p, and the lipid quinones (demethoxyubiquinone and Q) function to stabilize other Coq polypeptides.

摘要

辅酶Q(泛醌或Q)在呼吸电子传递链中发挥作用,并作为一种亲脂性抗氧化剂。在出芽酵母酿酒酵母中,Q生物合成需要九种Coq蛋白(Coq1-Coq9)。先前的研究表明酵母Coq7蛋白具有酶活性和结构作用。为了确定酵母Coq7p的功能作用,我们测试了大肠杆菌ubiF是否能在功能上替代酵母COQ7。ubiF基因编码一种黄素依赖性单加氧酶,它与Coq7蛋白没有同源性,是大肠杆菌中Q生物合成最后一步单加氧酶反应所必需的。以低拷贝表达的ubiF基因可恢复coq7点突变体(E194K)在含有非发酵碳源的培养基上的生长,但无法挽救coq7缺失突变体。然而,来自多拷贝载体的ubiF表达可恢复两个突变体的生长和Q合成,尽管在点突变体中的效率更高。我们将coq7点突变体更有效的挽救归因于Coq3、Coq4和Coq6蛋白的更高稳态水平以及UbiF的底物去甲氧基泛醌的存在。Coq7p与Coq3和Coq4多肽以高分子量复合物的形式共同迁移。在这里我们表明,向生长培养基中添加Q也能稳定coq7缺失突变体中的Coq3和Coq4多肽。数据表明,Coq7p和脂质醌(去甲氧基泛醌和Q)起到稳定其他Coq多肽的作用。

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