首页> 美国卫生研究院文献>Applied and Environmental Microbiology >Functional Expression of Human Dihydroorotate Dehydrogenase (DHODH) in pyr4 Mutants of Ustilago maydis Allows Target Validation of DHODH Inhibitors In Vivo
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Functional Expression of Human Dihydroorotate Dehydrogenase (DHODH) in pyr4 Mutants of Ustilago maydis Allows Target Validation of DHODH Inhibitors In Vivo

机译:人二氢乳清酸脱氢酶(DHODH)的功能表达在草til鱼的pyr4突变体中允许体内DHODH抑制剂的目标验证。

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摘要

Dihydroorotate dehydrogenase (DHODH; EC 1.3.99.11) is a central enzyme of pyrimidine biosynthesis and catalyzes the oxidation of dihydroorotate to orotate. DHODH is an important target for antiparasitic and cytostatic drugs since rapid cell proliferation often depends on the de novo synthesis of pyrimidine nucleotides. We have cloned the pyr4 gene encoding mitochondrial DHODH from the basidiomycetous plant pathogen Ustilago maydis. We were able to show that pyr4 contains a functional mitochondrial targeting signal. The deletion of pyr4 resulted in uracil auxotrophy, enhanced sensitivity to UV irradiation, and a loss of pathogenicity on corn plants. The biochemical characterization of purified U. maydis DHODH overproduced in Escherichia coli revealed that the U. maydis enzyme uses quinone electron acceptor Q6 and is resistant to several commonly used DHODH inhibitors. Here we show that the expression of the human DHODH gene fused to the U. maydis mitochondrial targeting signal is able to complement the auxotrophic phenotype of pyr4 mutants. While U. maydis wild-type cells were resistant to the DHODH inhibitor brequinar, strains expressing the human DHODH gene became sensitive to this cytostatic drug. Such engineered U. maydis strains can be used in sensitive in vivo assays for the development of novel drugs specifically targeted at either human or fungal DHODH.
机译:二氢乳清酸酯脱氢酶(DHODH; EC 1.3.99.11)是嘧啶生物合成的核心酶,催化二氢乳清酸酯氧化为乳清酸酯。 DHODH是抗寄生虫和抑制细胞生长药物的重要靶标,因为细胞的快速增殖通常取决于嘧啶核苷酸的从头合成。我们已经从担子菌植物病原体Ustilago maydis中克隆了编码线粒体DHODH的pyr4基因。我们能够证明pyr4包含功能性线粒体靶向信号。 pyr4的缺失导致尿嘧啶营养缺陷,增强了对紫外线辐射的敏感性,并使玉米植株失去致病性。在大肠杆菌中过量产生的纯化的马氏杆菌DHODH的生化特性表明,马氏杆菌酶使用醌电子受体Q6,并且对几种常用的DHODH抑制剂具有抗性。在这里,我们显示人DHODH基因与U. maydis线粒体靶向信号融合的表达能够补充pyr4突变体的营养缺陷型。尽管马氏假单胞菌野生型细胞对DHODH抑制剂布雷喹纳具有抗性,但表达人DHODH基因的菌株对该细胞抑制药物敏感。这样的工程化的美伊斯氏菌菌株可以用于敏感的体内测定中,以开发专门针对人或真菌DHODH的新药。

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