EPR spectroscopy of putative enzyme intermediates in the NO reductase and the auto-nitrosylation reaction of Desulfovibrio vulgaris hybrid cluster protein

Journal article (2019)

Authors

W.R. Hagen BT/Biocatalysis -

Research Group

BT/Biocatalysis () (TU Delft)

EPR Nitric oxide NO reductase Desulfovibrio Hybrid cluster protein Nitrosylation

To reference this document use:

http://resolver.tudelft.nl/uuid:8ac720d9-5e2a-41bd-9890-49dec0431ee0

More Info

expand_more

Published Date

2019

Language

English

Reuse Rights

Other than for strictly personal use, it is not permitted to download, forward or distribute the text or part of it, without the consent of the author(s) and/or copyright holder(s), unless the work is under an open content license such as Creative Commons.

Faculty

Applied Sciences

Department

BT/Biotechnologie

Research Group

BT/Biocatalysis

Abstract

The hybrid cluster protein (Hcp) contains a unique 4Fe cluster that is a hybrid of μ-S and μ-O bridges. Escherichia coli Hcp has recently been found to carry NO reductase activity as well as S-nitrosylation activity in NO-based signaling. In other species, the physiological activity has not been established. No reaction mechanism of any Hcp has been proposed. Here, we show that Desulfovibrio vulgaris (Hildenborough) Hcp has nitric oxide reductase activity with benzyl viologen as electron donor. With EPR spectroscopy, we identify three unexpected putative reaction intermediates: both in reduced and oxidized Hcp, dinitrosyl iron complexes are formed. Also, the hybrid cluster in reduced Hcp, but not in oxidized Hcp, binds the product N₂O. Possible implications for a reaction mechanism are discussed.

Files

1873_3468.13539.pdf

(pdf | 0.964 Mb)

Unknown license

Download not available