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致癌人类肝吸虫——华支睾吸虫硫氧还蛋白的分子表达及酶学特性

Molecular expression and enzymatic characterization of thioredoxin from the carcinogenic human liver fluke Opisthorchis viverrini.

作者信息

Suttiprapa Sutas, Matchimakul Pitchaya, Loukas Alex, Laha Thewarach, Wongkham Sopit, Kaewkes Sasithorn, Brindley Paul J, Sripa Banchob

机构信息

Graduate School, Khon Kaen University, Khon Kaen 40002, Thailand.

出版信息

Parasitol Int. 2012 Mar;61(1):101-6. doi: 10.1016/j.parint.2011.06.018. Epub 2011 Jun 29.

Abstract

The human liver fluke, Opisthorchis viverrini, induces inflammation of the hepatobiliary system. Despite being constantly exposed to inimical oxygen radicals released from inflammatory cells, the parasite survives for years. Defense against oxidative damage can be mediated through glutathione and/or thioredoxin utilizing systems. Here, we report the molecular expression and biochemical characterization of a thioredoxin (Trx) from O. viverrini. O. viverrini Trx cDNA encoded a polypeptide of 105 amino acid residues, of molecular mass 11.63 kDa. The predicted protein has similarity to previously characterized thioredoxins with 26-51% identity. Recombinant O. viverrini Trx (Ov-Trx-1) was expressed as soluble protein in E. coli. The recombinant protein showed insulin reduction activity and supported the enzymatic function of O. viverrini thioredoxin peroxidase. Expression of Ov-Trx-1 at mRNA and protein levels was observed in all obtainable developmental stages of the liver fluke. Ov-Trx-1 was also detected in excretory-secretory products released by adult O. viverrini. Immunohistochemistry, Ov-Trx-1 was expressed in nearly all parasite tissue excepted ovary and mature sperms. Interestingly, Ov-Trx-1 was observed in the infected biliary epithelium but not in normal bile ducts. These results suggest that Ov-Trx-1 is essential for the parasite throughout the life cycle. In the host-parasite interaction aspect, Ov-Trx-1 may support thioredoxin peroxidase in protecting the parasite against damage induced by reactive oxygen species from inflammation.

摘要

人体肝吸虫,即华支睾吸虫,会引发肝胆系统炎症。尽管该寄生虫持续暴露于炎症细胞释放的有害氧自由基中,但仍能存活数年。对氧化损伤的防御可通过谷胱甘肽和/或利用硫氧还蛋白的系统介导。在此,我们报告了华支睾吸虫硫氧还蛋白(Trx)的分子表达及生化特性。华支睾吸虫Trx cDNA编码一个由105个氨基酸残基组成的多肽,分子量为11.63 kDa。预测的蛋白质与先前已鉴定的硫氧还蛋白具有相似性,同一性为26 - 51%。重组华支睾吸虫Trx(Ov-Trx-1)在大肠杆菌中表达为可溶性蛋白。该重组蛋白具有胰岛素还原活性,并支持华支睾吸虫硫氧还蛋白过氧化物酶的酶功能。在肝吸虫所有可获得的发育阶段均观察到Ov-Trx-1在mRNA和蛋白质水平的表达。在成年华支睾吸虫释放的排泄 - 分泌产物中也检测到了Ov-Trx-1。免疫组织化学显示,除卵巢和成熟精子外,Ov-Trx-1在几乎所有寄生虫组织中均有表达。有趣的是,在受感染的胆管上皮中观察到了Ov-Trx-1,但在正常胆管中未观察到。这些结果表明,Ov-Trx-1在寄生虫的整个生命周期中至关重要。在宿主 - 寄生虫相互作用方面,Ov-Trx-1可能支持硫氧还蛋白过氧化物酶保护寄生虫免受炎症中活性氧引起的损伤。

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