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锥虫和利什曼原虫的寄生虫特异性 trypanothione 代谢。

The parasite-specific trypanothione metabolism of trypanosoma and leishmania.

作者信息

Krauth-Siegel R Luise, Meiering Svea K, Schmidt Heide

机构信息

Center of Biochemistry, University of Heidelberg, Im Neuenheimer Feld 504, D-69120 Heidelberg, Germany.

出版信息

Biol Chem. 2003 Apr;384(4):539-49. doi: 10.1515/BC.2003.062.

Abstract

The bis(glutathionyl)spermidine trypanothione exclusively occurs in parasitic protozoa of the order Kinetoplastida, such as trypanosomes and leishmania, some of which are the causative agents of several tropical diseases. The dithiol is kept reduced by the flavoenzyme trypanothione reductase and the trypanothione system replaces in these parasites the nearly ubiquitous glutathione/glutathione reductase couple. Trypanothione is a reductant of thioredoxin and tryparedoxin, small dithiol proteins, which in turn deliver reducing equivalents for the synthesis of deoxyribonucleotides as well as for the detoxification of hydroperoxides by different peroxidases. Depending on the individual organism and the developmental state, the parasites also contain significant amounts of glutathione, mono-glutathionylspermidine and ovothiol, whereby all four low molecular mass thiols are directly (trypanothione and mono-glutathionylspermidine) or indirectly (glutathione and ovothiol) maintained in the reduced state by trypanothione reductase. Thus the trypanothione system is central for any thiol regeneration and trypanothione reductase has been shown to be an essential enzyme in these parasites. The absence of this pathway from the mammalian host and the sensitivity of trypanosomatids toward oxidative stress render the enzymes of the trypanothione metabolism attractive target molecules for the rational development of new drugs against African sleeping sickness, Chagas' disease and the different forms of leishmaniasis.

摘要

双(谷胱甘肽基)亚精胺锥虫硫醇仅存在于动基体目寄生原生动物中,如锥虫和利什曼原虫,其中一些是几种热带疾病的病原体。这种二硫醇通过黄素酶锥虫硫醇还原酶保持还原状态,并且锥虫硫醇系统在这些寄生虫中取代了几乎普遍存在的谷胱甘肽/谷胱甘肽还原酶对。锥虫硫醇是硫氧还蛋白和锥虫还蛋白(小的二硫醇蛋白)的还原剂,它们反过来为脱氧核苷酸的合成以及通过不同过氧化物酶对氢过氧化物的解毒提供还原当量。根据个体生物体和发育状态,这些寄生虫还含有大量的谷胱甘肽、单谷胱甘肽基亚精胺和卵硫醇,其中所有四种低分子量硫醇都由锥虫硫醇还原酶直接(锥虫硫醇和单谷胱甘肽基亚精胺)或间接(谷胱甘肽和卵硫醇)维持在还原状态。因此,锥虫硫醇系统对于任何硫醇的再生都至关重要,并且锥虫硫醇还原酶已被证明是这些寄生虫中的一种必需酶。哺乳动物宿主中不存在这条途径以及锥虫对氧化应激的敏感性使得锥虫硫醇代谢酶成为合理开发抗非洲昏睡病、恰加斯病和不同形式利什曼病新药的有吸引力的靶分子。

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