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在布氏锥虫中对半胱氨酸亚砜还原酶系的功能表征。

Functional characterisation of the methionine sulfoxide reductase repertoire in Trypanosoma brucei.

机构信息

Instituto de Agrobiotecnología del Litoral, CONICET-Universidad Nacional del Litoral, 3000 Santa Fe, Argentina.

School of Biological & Chemical Sciences, Queen Mary University of London, Mile End Road, London E1 4NS, UK.

出版信息

Free Radic Biol Med. 2017 Nov;112:524-533. doi: 10.1016/j.freeradbiomed.2017.08.023. Epub 2017 Sep 1.

DOI:10.1016/j.freeradbiomed.2017.08.023
PMID:28865997
Abstract

To combat the deleterious effects that oxidation of the sulfur atom in methionine to sulfoxide may bring, aerobic cells express repair pathways involving methionine sulfoxide reductases (MSRs) to reverse the above reaction. Here, we show that Trypanosoma brucei, the causative agent of African trypanosomiasis, expresses two distinct trypanothione-dependent MSRs that can be distinguished from each other based on sequence, sub-cellular localisation and substrate preference. One enzyme found in the parasite's cytosol, shows homology to the MSRA family of repair proteins and preferentially metabolises the S epimer of methionine sulfoxide. The second, which contains sequence motifs present in MSRBs, is restricted to the mitochondrion and can only catalyse reduction of the R form of peptide-bound methionine sulfoxide. The importance of these proteins to the parasite was demonstrated using functional genomic-based approaches to produce cells with reduced or elevated expression levels of MSRA, which exhibited altered susceptibility to exogenous HO. These findings identify new reparative pathways that function to fix oxidatively damaged methionine within this medically important parasite.

摘要

为了对抗蛋氨酸的硫原子氧化为亚砜可能带来的有害影响,需氧细胞表达了涉及蛋氨酸亚砜还原酶(MSRs)的修复途径,以逆转上述反应。在这里,我们表明,引起非洲锥虫病的病原体布氏锥虫表达了两种不同的依赖于 trypanothione 的 MSR,可以根据序列、亚细胞定位和底物偏好将它们彼此区分开来。一种存在于寄生虫细胞质中的酶与 MSRA 家族的修复蛋白具有同源性,优先代谢蛋氨酸亚砜的 S 对映异构体。第二种酶包含存在于 MSRBs 中的序列基序,仅限于线粒体,并且只能催化肽结合的蛋氨酸亚砜的 R 形式的还原。使用基于功能基因组的方法产生 MSRA 表达水平降低或升高的细胞,这些细胞对 HO 的敏感性发生改变,从而证明了这些蛋白对寄生虫的重要性。这些发现确定了新的修复途径,可修复这种医学上重要的寄生虫内氧化损伤的蛋氨酸。

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