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Evolutionary and structural insights into the multifaceted glutathione peroxidase (Gpx) superfamily.

机译:进化和结构方面的见解,涉及多层面的谷胱甘肽过氧化物酶(Gpx)超家族。

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摘要

Glutathione peroxidase (GPx) is a widespread protein superfamily found in many organisms throughout all kingdoms of life. Although it was initially thought to use only glutathione as reductant, recent evidence suggests that the majority of GPxs have specificity for thioredoxin. We present a thorough in silico analysis performed on 724 sequences and 12 structures aimed to clarify the evolutionary, structural, and sequence determinants of GPx specificity. Structural variability was found to be limited to only two regions, termed oligomerization loop and functional helix, which modulate both reduced substrate specificity and oligomerization state. We show that mammalian GPx-1, the canonic selenocysteine-based tetrameric glutathione peroxidase, is a recent "invention" during evolution. Contrary to common belief, cysteine-based thioredoxin-specific GPx, which we propose the TGPx, are both more common and more ancient. This raises interesting evolutionary considerations regarding oligomerization and the use of active-site selenocysteine residue. In addition, phylogenetic analysis has revealed the presence of a novel member belonging to the GPx superfamily in Mammalia and Amphibia, for which we propose the name GPx-8, following the present numeric order of the mammalian GPxs.
机译:谷胱甘肽过氧化物酶(GPx)是在整个生命王国的许多生物中发现的广泛的蛋白质超家族。尽管最初认为仅使用谷胱甘肽作为还原剂,但最近的证据表明,大多数GPx对硫氧还蛋白具有特异性。我们提出了对724个序列和12个结构进行的彻底的计算机分析,旨在阐明GPx特异性的进化,结构和序列决定因素。发现结构可变性仅限于两个区域,称为低聚环和功能性螺旋,其调节降低的底物特异性和低聚状态。我们表明,哺乳动物GPx-1,基于经典的硒代半胱氨酸的四聚谷胱甘肽过氧化物酶,是进化过程中的最新“发明”。与通常的看法相反,我们建议使用TGPx的基于半胱氨​​酸的硫氧还蛋白特异性GPx更为普遍和古老。这引起了关于低聚和使用活性位点硒代半胱氨酸残基的有趣的进化考虑。此外,系统发育分析表明,在哺乳动物和两栖动物中存在一个属于GPx超家族的新成员,我们按照哺乳动物GPx的当前数字顺序为其命名为GPx-8。

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