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富马酸盐是前循环型布氏锥虫产生的一种必需中间代谢产物。

Fumarate is an essential intermediary metabolite produced by the procyclic Trypanosoma brucei.

作者信息

Coustou Virginie, Biran Marc, Besteiro Sébastien, Rivière Loïc, Baltz Théo, Franconi Jean-Michel, Bringaud Frédéric

机构信息

Laboratoire de Génomique Fonctionnelle des Trypanosomatides, UMR-5162 CNRS and Résonance Magnétique des Systèmes Biologiques, UMR-5536 CNRS, Université Victor Segalen Bordeaux 2, 146 rue Léo Saignat, 33076 Bordeaux, France.

出版信息

J Biol Chem. 2006 Sep 15;281(37):26832-46. doi: 10.1074/jbc.M601377200. Epub 2006 Jul 20.

Abstract

The procyclic stage of Trypanosoma brucei, a parasitic protist responsible for sleeping sickness in humans, converts most of the consumed glucose into excreted succinate, by succinic fermentation. Succinate is produced by the glycosomal and mitochondrial NADH-dependent fumarate reductases, which are not essential for parasite viability. To further explore the role of the succinic fermentation pathways, we studied the trypanosome fumarases, the enzymes providing fumarate to fumarate reductases. The T. brucei genome contains two class I fumarase genes encoding cytosolic (FHc) and mitochondrial (FHm) enzymes, which account for total cellular fumarase activity as shown by RNA interference. The growth arrest of a double RNA interference mutant cell line showing no fumarase activity indicates that fumarases are essential for the parasite. Interestingly, addition of fumarate to the medium rescues the growth phenotype, indicating that fumarate is an essential intermediary metabolite of the insect stage trypanosomes. We propose that trypanosomes use fumarate as an essential electron acceptor, as exemplified by the fumarate dependence previously reported for an enzyme of the essential de novo pyrimidine synthesis (Takashima, E., Inaoka, D. K., Osanai, A., Nara, T., Odaka, M., Aoki, T., Inaka, K., Harada, S., and Kita, K. (2002) Mol. Biochem. Parasitol. 122, 189-200).

摘要

布氏锥虫的前循环期是一种导致人类昏睡病的寄生原生生物,它通过琥珀酸发酵将大部分消耗的葡萄糖转化为分泌的琥珀酸。琥珀酸由糖体和线粒体中依赖NADH的延胡索酸还原酶产生,这些酶对寄生虫的生存能力并非必不可少。为了进一步探究琥珀酸发酵途径的作用,我们研究了锥虫中的延胡索酸酶,即那些为延胡索酸还原酶提供延胡索酸的酶。布氏锥虫基因组包含两个I类延胡索酸酶基因,分别编码胞质(FHc)和线粒体(FHm)酶,RNA干扰实验表明这两种酶构成了细胞总的延胡索酸酶活性。一个双RNA干扰突变细胞系生长停滞,且无延胡索酸酶活性,这表明延胡索酸酶对寄生虫至关重要。有趣的是,向培养基中添加延胡索酸可挽救生长表型,这表明延胡索酸是昆虫阶段锥虫的一种必需中间代谢物。我们提出锥虫将延胡索酸用作必需的电子受体,这一点已在之前报道的必需的从头嘧啶合成酶对延胡索酸的依赖性中得到体现(高岛英树、稻冈健二、小佐内明、奈良隆、小高真、青木隆、稻中健、原田修、北佳子,(2002年)《分子生物化学寄生虫学》122卷,第189 - 200页)。

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