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Salmonella enterica BcfH Is a Trimeric Thioredoxin-Like Bifunctional Enzyme with Both Thiol Oxidase and Disulfide Isomerase Activities

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posted on 2025-02-07, 04:29 authored by Pramod SubediPramod Subedi, Jason PaxmanJason Paxman, Geqing WangGeqing Wang, Lilian HorLilian Hor, Y Hong, AD Verderosa, AE Whitten, S Panjikar, Carlos Fernando Santos MartinCarlos Fernando Santos Martin, JL Martin, M Totsika, Begona HerasBegona Heras

Aims: Thioredoxin (TRX)-fold proteins are ubiquitous in nature. This redox scaffold has evolved to enable a variety of functions, including redox regulation, protein folding, and oxidative stress defense. In bacteria, the TRX-like disulfide bond (Dsb) family mediates the oxidative folding of multiple proteins required for fitness and pathogenic potential. Conventionally, Dsb proteins have specific redox functions with monomeric and dimeric Dsbs exclusively catalyzing thiol oxidation and disulfide isomerization, respectively. This contrasts with the eukaryotic disulfide forming machinery where the modular TRX protein disulfide isomerase (PDI) mediates thiol oxidation and disulfide reshuffling. In this study, we identified and structurally and biochemically characterized a novel Dsb-like protein from Salmonella enterica termed bovine colonization factor protein H (BcfH) and defined its role in virulence. Results: In the conserved bovine colonization factor (bcf) fimbrial operon, the Dsb-like enzyme BcfH forms a trimeric structure, exceptionally uncommon among the large and evolutionary conserved TRX superfamily. This protein also displays very unusual catalytic redox centers, including an unwound α-helix holding the redox active site and a trans-proline instead of the conserved cis-proline active site loop. Remarkably, BcfH displays both thiol oxidase and disulfide isomerase activities contributing to Salmonella fimbrial biogenesis. Innovation and Conclusion: Typically, oligomerization of bacterial Dsb proteins modulates their redox function, with monomeric and dimeric Dsbs mediating thiol oxidation and disulfide isomerization, respectively. This study demonstrates a further structural and functional malleability in the TRX-fold protein family. BcfH trimeric architecture and unconventional catalytic sites permit multiple redox functions emulating in bacteria the eukaryotic PDI dual oxidoreductase activity.


Funding

This work was supported by the Australian Research Council (ARC) project grants (DP 190101613, DP180102987, and DP150102287), an ARC Future Fellowship (FT130100580), ARC DECRA (DE130101169), the National Health and Medical Research Council (NHMRC) Project Grants (GRT1144046, GRT1143638), and a Vera and Clive Ramaciotti Foundations Health Investment Grant (2017HIG0119). M.T. was supported by a Vice-Chancellor's Research Fellowship from the Queensland University of Technology.

History

Publication Date

2021-07-01

Journal

Antioxidants & Redox Signaling

Volume

35

Issue

1

Pagination

21-39

Publisher

Mary Ann Liebert, Inc.

ISSN

1523-0864

Rights Statement

© 2021 Mary Ann Liebert, Inc. This is the accepted version of the following article: Subedi, Pramod et al. “Salmonella Enterica BcfH Is a Trimeric Thioredoxin-Like Bifunctional Enzyme with Both Thiol Oxidase and Disulfide Isomerase Activities.” Antioxidants & Redox Signaling 35.1 (2021): 21–39, which has now been formally published in final form at Antioxidants & Redox Signaling at https://doi.org/10.1089/ars.2020.8218. This original submission version of the article may be used for non-commercial purposes in accordance with the Mary Ann Liebert, Inc., publishers’ self-archiving terms and conditions.

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    Keywords

    disulfide catalysisDsb proteinsthioredoxinredox homeostasiscolonizationbiofilmbacterial infection

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