The comparison of metal-binding ability of the C-terminal region of Y. pestis, K. pneumoniae, and S. typhimurium FeoB protein

21 August 2025, Version 1
This content is an early or alternative research output and has not been peer-reviewed by Cambridge University Press at the time of posting.

Abstract

In our previous work, we have analyzed the coordination chemistry of the peptidic model of the C-terminal part of E. coli FeoB protein, regarded as the most important Fe(II) bacterial transporter in Gram-positive and Gram-negative bacteria. The C-terminal region of FeoB contains conserved cysteine and histidine residues, which create a potent metal-binding site, exhibiting high affinity towards Fe(II), Mn(II), and Zn(II). The C-terminal FeoB sequences in Gram-negative bacteria vary in the number and position of additional potential metal-binding residues, aspartic and glutamic acids, which could affect the affinity of the region towards metal ions and potentially even the specificity of the metal binding. Therefore, in this work, we have decided to investigate the metal-binding properties of the peptidic models of the C-terminal FeoB region of three Gram-negative bacteria: Y. pestis (L1, Ac-RRARSRVTVRLQNSEPANCCRSSGSNCH), K. pneumoniae (L2, Ac-RRARSRVDVSLLATRKTPASCCSSPAGDCH), and S. typhimurium (L3, Ac-RRARSRVDIELLATRKNVSSCCSGTAGNCH). With a variety of physicochemical methods (potentiometry, ESI-MS, NMR, CD), we have described complexes of Fe(II), Mn(II), and Zn(II) with the studied ligands and discussed the influence of the specific residues on the metal-binding properties of the peptidic models. These findings enhance our understanding of FeoB-mediated metal transport and provide insights into pathogen-specific metal homeostasis mechanisms.

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Supplementary Information for the paper: The comparison of metal-binding ability of the C-terminal region of Y. pestis, K. pneumoniae, and S. typhimurium FeoB protein
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This file includes additional data: mass spectra, speciation plots, NMR and CD spectra.
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