Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore

To replicate in mammalian hosts, bacterial pathogens must acquire iron. The majority of iron is coordinated to the protoporphyrin ring of heme, which is further bound to hemoglobin. Pathogenic bacteria utilize secreted hemophores to acquire heme from heme sources such as hemoglobin. Bacillus anthrac...

Descripción completa

Detalles Bibliográficos
Autores principales: Ekworomadu, MarCia T., Poor, Catherine B., Owens, Cedric P., Balderas, Miriam A., Fabian, Marian, Olson, John S., Murphy, Frank, Balkabasi, Erol, Honsa, Erin S., He, Chuan, Goulding, Celia W., Maresso, Anthony W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3297588/
https://www.ncbi.nlm.nih.gov/pubmed/22412371
http://dx.doi.org/10.1371/journal.ppat.1002559
_version_ 1782225894597722112
author Ekworomadu, MarCia T.
Poor, Catherine B.
Owens, Cedric P.
Balderas, Miriam A.
Fabian, Marian
Olson, John S.
Murphy, Frank
Balkabasi, Erol
Honsa, Erin S.
He, Chuan
Goulding, Celia W.
Maresso, Anthony W.
author_facet Ekworomadu, MarCia T.
Poor, Catherine B.
Owens, Cedric P.
Balderas, Miriam A.
Fabian, Marian
Olson, John S.
Murphy, Frank
Balkabasi, Erol
Honsa, Erin S.
He, Chuan
Goulding, Celia W.
Maresso, Anthony W.
author_sort Ekworomadu, MarCia T.
collection PubMed
description To replicate in mammalian hosts, bacterial pathogens must acquire iron. The majority of iron is coordinated to the protoporphyrin ring of heme, which is further bound to hemoglobin. Pathogenic bacteria utilize secreted hemophores to acquire heme from heme sources such as hemoglobin. Bacillus anthracis, the causative agent of anthrax disease, secretes two hemophores, IsdX1 and IsdX2, to acquire heme from host hemoglobin and enhance bacterial replication in iron-starved environments. Both proteins contain NEAr-iron Transporter (NEAT) domains, a conserved protein module that functions in heme acquisition in Gram-positive pathogens. Here, we report the structure of IsdX1, the first of a Gram-positive hemophore, with and without bound heme. Overall, IsdX1 forms an immunoglobin-like fold that contains, similar to other NEAT proteins, a 3(10)-helix near the heme-binding site. Because the mechanistic function of this helix in NEAT proteins is not yet defined, we focused on the contribution of this region to hemophore and NEAT protein activity, both biochemically and biologically in cultured cells. Site-directed mutagenesis of amino acids in and adjacent to the helix identified residues important for heme and hemoglobin association, with some mutations affecting both properties and other mutations affecting only heme stabilization. IsdX1 with mutations that reduced the ability to associate with hemoglobin and bind heme failed to restore the growth of a hemophore-deficient strain of B. anthracis on hemoglobin as the sole iron source. These data indicate that not only is the 3(10)-helix important for NEAT protein biology, but also that the processes of hemoglobin and heme binding can be both separate as well as coupled, the latter function being necessary for maximal heme-scavenging activity. These studies enhance our understanding of NEAT domain and hemophore function and set the stage for structure-based inhibitor design to block NEAT domain interaction with upstream ligands.
format Online
Article
Text
id pubmed-3297588
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-32975882012-03-12 Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore Ekworomadu, MarCia T. Poor, Catherine B. Owens, Cedric P. Balderas, Miriam A. Fabian, Marian Olson, John S. Murphy, Frank Balkabasi, Erol Honsa, Erin S. He, Chuan Goulding, Celia W. Maresso, Anthony W. PLoS Pathog Research Article To replicate in mammalian hosts, bacterial pathogens must acquire iron. The majority of iron is coordinated to the protoporphyrin ring of heme, which is further bound to hemoglobin. Pathogenic bacteria utilize secreted hemophores to acquire heme from heme sources such as hemoglobin. Bacillus anthracis, the causative agent of anthrax disease, secretes two hemophores, IsdX1 and IsdX2, to acquire heme from host hemoglobin and enhance bacterial replication in iron-starved environments. Both proteins contain NEAr-iron Transporter (NEAT) domains, a conserved protein module that functions in heme acquisition in Gram-positive pathogens. Here, we report the structure of IsdX1, the first of a Gram-positive hemophore, with and without bound heme. Overall, IsdX1 forms an immunoglobin-like fold that contains, similar to other NEAT proteins, a 3(10)-helix near the heme-binding site. Because the mechanistic function of this helix in NEAT proteins is not yet defined, we focused on the contribution of this region to hemophore and NEAT protein activity, both biochemically and biologically in cultured cells. Site-directed mutagenesis of amino acids in and adjacent to the helix identified residues important for heme and hemoglobin association, with some mutations affecting both properties and other mutations affecting only heme stabilization. IsdX1 with mutations that reduced the ability to associate with hemoglobin and bind heme failed to restore the growth of a hemophore-deficient strain of B. anthracis on hemoglobin as the sole iron source. These data indicate that not only is the 3(10)-helix important for NEAT protein biology, but also that the processes of hemoglobin and heme binding can be both separate as well as coupled, the latter function being necessary for maximal heme-scavenging activity. These studies enhance our understanding of NEAT domain and hemophore function and set the stage for structure-based inhibitor design to block NEAT domain interaction with upstream ligands. Public Library of Science 2012-03-08 /pmc/articles/PMC3297588/ /pubmed/22412371 http://dx.doi.org/10.1371/journal.ppat.1002559 Text en Ekworomadu et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Ekworomadu, MarCia T.
Poor, Catherine B.
Owens, Cedric P.
Balderas, Miriam A.
Fabian, Marian
Olson, John S.
Murphy, Frank
Balkabasi, Erol
Honsa, Erin S.
He, Chuan
Goulding, Celia W.
Maresso, Anthony W.
Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore
title Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore
title_full Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore
title_fullStr Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore
title_full_unstemmed Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore
title_short Differential Function of Lip Residues in the Mechanism and Biology of an Anthrax Hemophore
title_sort differential function of lip residues in the mechanism and biology of an anthrax hemophore
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3297588/
https://www.ncbi.nlm.nih.gov/pubmed/22412371
http://dx.doi.org/10.1371/journal.ppat.1002559
work_keys_str_mv AT ekworomadumarciat differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT poorcatherineb differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT owenscedricp differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT balderasmiriama differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT fabianmarian differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT olsonjohns differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT murphyfrank differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT balkabasierol differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT honsaerins differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT hechuan differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT gouldingceliaw differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore
AT maressoanthonyw differentialfunctionoflipresiduesinthemechanismandbiologyofananthraxhemophore

Ejemplares similares