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蛋白质导入阴道毛滴虫氢化酶体涉及N端和内部靶向信号:以硫氧还蛋白还原酶为例的研究

Protein import into hydrogenosomes of Trichomonas vaginalis involves both N-terminal and internal targeting signals: a case study of thioredoxin reductases.

作者信息

Mentel Marek, Zimorski Verena, Haferkamp Patrick, Martin William, Henze Katrin

机构信息

Institute of Botany III, Heinrich-Heine University of Duesseldorf, Duesseldorf, Germany.

出版信息

Eukaryot Cell. 2008 Oct;7(10):1750-7. doi: 10.1128/EC.00206-08. Epub 2008 Aug 1.

Abstract

The parabasalian flagellate Trichomonas vaginalis harbors mitochondrion-related and H(2)-producing organelles of anaerobic ATP synthesis, called hydrogenosomes, which harbor oxygen-sensitive enzymes essential to its pyruvate metabolism. In the human urogenital tract, however, T. vaginalis is regularly exposed to low oxygen concentrations and therefore must possess antioxidant systems protecting the organellar environment against the detrimental effects of molecular oxygen and reactive oxygen species. We have identified two closely related hydrogenosomal thioredoxin reductases (TrxRs), the hitherto-missing component of a thioredoxin-linked hydrogenosomal antioxidant system. One of the two hydrogenosomal TrxR isoforms, TrxRh1, carried an N-terminal extension resembling known hydrogenosomal targeting signals. Expression of hemagglutinin-tagged TrxRh1 in transfected T. vaginalis cells revealed that its N-terminal extension was necessary to import the protein into the organelles. The second hydrogenosomal TrxR isoform, TrxRh2, had no N-terminal targeting signal but was nonetheless efficiently targeted to hydrogenosomes. N-terminal presequences from hydrogenosomal proteins with known processing sites, i.e., the alpha subunit of succinyl coenzyme A synthetase (SCSalpha) and pyruvate:ferredoxin oxidoreductase A, were investigated for their ability to direct mature TrxRh1 to hydrogenosomes. Neither presequence directed TrxRh1 to hydrogenosomes, indicating that neither extension is, by itself, sufficient for hydrogenosomal targeting. Moreover, SCSalpha lacking its N-terminal extension was efficiently imported into hydrogenosomes, indicating that this extension is not required for import of this major hydrogenosomal protein. The finding that some hydrogenosomal enzymes require N-terminal signals for import but that in others the N-terminal extension is not necessary for targeting indicates the presence of additional targeting signals within the mature subunits of several hydrogenosome-localized proteins.

摘要

巴氏鞭毛虫阴道毛滴虫含有与线粒体相关的、进行厌氧ATP合成并产生H₂的细胞器,称为氢化酶体,其中含有对其丙酮酸代谢至关重要的氧敏感酶。然而,在人类泌尿生殖道中,阴道毛滴虫经常暴露于低氧浓度环境,因此必须拥有抗氧化系统,以保护细胞器环境免受分子氧和活性氧的有害影响。我们鉴定出了两种密切相关的氢化酶体硫氧还蛋白还原酶(TrxRs),它们是硫氧还蛋白连接的氢化酶体抗氧化系统中迄今缺失的组分。两种氢化酶体TrxR同工型之一TrxRh1带有一个N端延伸,类似于已知的氢化酶体靶向信号。在转染的阴道毛滴虫细胞中表达血凝素标记的TrxRh1表明,其N端延伸对于将该蛋白导入细胞器是必需的。第二种氢化酶体TrxR同工型TrxRh2没有N端靶向信号,但仍能有效地靶向氢化酶体。对具有已知加工位点的氢化酶体蛋白的N端前序列,即琥珀酰辅酶A合成酶(SCSα)的α亚基和丙酮酸:铁氧化还原蛋白氧化还原酶A,进行了研究,以考察它们将成熟的TrxRh1导向氢化酶体的能力。这两种前序列均未将TrxRh1导向氢化酶体,表明单独任何一个延伸都不足以实现氢化酶体靶向。此外,缺少N端延伸的SCSα仍能有效地导入氢化酶体,表明该延伸对于这种主要的氢化酶体蛋白的导入并非必需。一些氢化酶体酶需要N端信号进行导入,但其他一些酶的N端延伸对于靶向并非必需,这一发现表明几种氢化酶体定位蛋白的成熟亚基中存在额外的靶向信号。

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