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鉴定和表征古菌和细菌 F 依赖性硫氧还蛋白还原酶。

Identification and characterization of archaeal and bacterial F -dependent thioredoxin reductases.

机构信息

Molecular Enzymology Group, University of Groningen, The Netherlands.

IMIBIO-SL CONICET, Facultad de Química Bioquímica y Farmacia, Universidad Nacional de San Luis, Argentina.

出版信息

FEBS J. 2023 Oct;290(19):4777-4791. doi: 10.1111/febs.16896. Epub 2023 Jul 14.

Abstract

The thioredoxin pathway is an antioxidant system present in most organisms. Electrons flow from a thioredoxin reductase to thioredoxin at the expense of a specific electron donor. Most known thioredoxin reductases rely on NADPH as a reducing cofactor. Yet, in 2016, a new type of thioredoxin reductase was discovered in Archaea which utilize instead a reduced deazaflavin cofactor (F H ). For this reason, the respective enzyme was named deazaflavin-dependent flavin-containing thioredoxin reductase (DFTR). To have a broader understanding of the biochemistry of DFTRs, we identified and characterized two other archaeal representatives. A detailed kinetic study, which included pre-steady state kinetic analyses, revealed that these two DFTRs are highly specific for F H while displaying marginal activity with NADPH. Nevertheless, they share mechanistic features with the canonical thioredoxin reductases that are dependent on NADPH (NTRs). A detailed structural analysis led to the identification of two key residues that tune cofactor specificity of DFTRs. This allowed us to propose a DFTR-specific sequence motif that enabled for the first time the identification and experimental characterization of a bacterial DFTR.

摘要

硫氧还蛋白途径是一种存在于大多数生物中的抗氧化系统。电子从硫氧还蛋白还原酶流向硫氧还蛋白,代价是特定的电子供体。大多数已知的硫氧还蛋白还原酶依赖 NADPH 作为还原辅助因子。然而,在 2016 年,在古菌中发现了一种新型的硫氧还蛋白还原酶,它利用还原的去氮黄素辅因子(F H )。因此,相应的酶被命名为去氮黄素依赖黄素含硫氧还蛋白还原酶(DFTR)。为了更全面地了解 DFTR 的生物化学特性,我们鉴定并表征了另外两种古菌代表。详细的动力学研究,包括预稳态动力学分析,表明这两种 DFTR 对 F H 具有高度特异性,而与 NADPH 的活性则微不足道。然而,它们与依赖 NADPH 的典型硫氧还蛋白还原酶(NTRs)具有共同的机制特征。详细的结构分析确定了两个关键残基,它们调节 DFTR 的辅助因子特异性。这使我们能够提出一个 DFTR 特异性的序列基序,首次实现了细菌 DFTR 的鉴定和实验表征。

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