首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Generating disulfides enzymatically: Reaction products and electron acceptors of the endoplasmic reticulum thiol oxidase Ero1p
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Generating disulfides enzymatically: Reaction products and electron acceptors of the endoplasmic reticulum thiol oxidase Ero1p

机译:酶促生成二硫键:内质网硫醇氧化酶Ero1p的反应产物和电子受体

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摘要

Ero1p is a key enzyme in the disulfide bond formation pathway in eukaryotic cells in both aerobic and anaerobic environments. It was previously demonstrated that Ero1p can transfer electrons from thiol substrates to molecular oxygen. However, the fate of electrons under anaerobic conditions and the final fate of electrons under aerobic conditions remained obscure. To address these fundamental issues in the Ero1p mechanism, we studied the transfer of electrons from recombinant yeast Ero1p to various electron acceptors. Under aerobic conditions, reduction of molecular oxygen by Ero1p yielded stoichiometric hydrogen peroxide. Remarkably, we found that reduced Ero1 p can transfer electrons to a variety of small and macromolecular electron acceptors in addition to molecular oxygen. In particular, Ero1p can catalyze reduction of exogenous FAD in solution. Free FAD is not required for the catalysis of dithiol oxidation by Ero1p, but it is sufficient to drive disulfide bond formation under anaerobic conditions. These findings provide insight into mechanisms for regenerating oxidized Ero1p and maintaining disulfide bond formation under anaerobic conditions in the endoplasmic reticulum.
机译:Ero1p是有氧和厌氧环境中真核细胞中二硫键形成途径中的关键酶。先前已证明Ero1p可以将电子从硫醇底物转移到分子氧。然而,在厌氧条件下电子的命运和在有氧条件下电子的最终命运仍然不清楚。为了解决Ero1p机制中的这些基本问题,我们研究了电子从重组酵母Ero1p到各种电子受体的转移。在有氧条件下,Ero1p还原分子氧会产生化学计量的过氧化氢。值得注意的是,我们发现还原的Ero1p可以将电子转移到除分子氧之外的各种小分子和大分子电子受体上。特别地,Ero1p可以催化溶液中外源FAD的还原。游离的FAD不需要通过Ero1p催化二硫醇氧化,但是在厌氧条件下足以驱动二硫键的形成。这些发现为内质网厌氧条件下再生Ero1p并维持二硫键形成的机理提供了见识。

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