Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes

Methicillin-resistant Staphylococcus aureus (MRSA) regulates resistance to β-lactams via preferential production of an alternative penicillin-binding protein (PBP), PBP2a. PBP2a binds many β-lactam antibiotics with less affinity than PBPs which are predominant in methicillin-susceptible (MSSA) strai...

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Autores principales: Ersoy, Selvi C., Chan, Liana C., Yeaman, Michael R., Chambers, Henry F., Proctor, Richard A., Ludwig, Kevin C., Schneider, Tanja, Manna, Adhar C., Cheung, Ambrose, Bayer, Arnold S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9028190/
https://www.ncbi.nlm.nih.gov/pubmed/35453214
http://dx.doi.org/10.3390/antibiotics11040462
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author Ersoy, Selvi C.
Chan, Liana C.
Yeaman, Michael R.
Chambers, Henry F.
Proctor, Richard A.
Ludwig, Kevin C.
Schneider, Tanja
Manna, Adhar C.
Cheung, Ambrose
Bayer, Arnold S.
author_facet Ersoy, Selvi C.
Chan, Liana C.
Yeaman, Michael R.
Chambers, Henry F.
Proctor, Richard A.
Ludwig, Kevin C.
Schneider, Tanja
Manna, Adhar C.
Cheung, Ambrose
Bayer, Arnold S.
author_sort Ersoy, Selvi C.
collection PubMed
description Methicillin-resistant Staphylococcus aureus (MRSA) regulates resistance to β-lactams via preferential production of an alternative penicillin-binding protein (PBP), PBP2a. PBP2a binds many β-lactam antibiotics with less affinity than PBPs which are predominant in methicillin-susceptible (MSSA) strains. A novel, rather frequent in vitro phenotype was recently identified among clinical MRSA bloodstream isolates, termed “NaHCO(3)-responsiveness”. This phenotype features β-lactam susceptibility of certain MRSA strains only in the presence of NaHCO(3). Two distinct PBP2a variants, 246G and 246E, have been linked to the NaHCO(3)-responsive and NaHCO(3)-non-responsive MRSA phenotypes, respectively. To determine the mechanistic impact of PBP2a variants on β-lactam susceptibility, binding profiles of a fluorescent penicillin probe (Bocillin-FL) to each purified PBP2a variant were assessed and compared to whole-cell binding profiles characterized by flow cytometry in the presence vs. absence of NaHCO(3). These investigations revealed that NaHCO(3) differentially influenced the binding of the fluorescent penicillin, Bocillin-FL, to the PBP2a variants, with binding intensity and rate of binding significantly enhanced in the 246G compared to the 246E variant. Of note, the NaHCO(3)-β-lactam (oxacillin)-responsive JE2 strain, which natively harbors the 246G variant, had enhanced Bocillin-FL whole-cell binding following exposure to NaHCO(3). This NaHCO(3)-mediated increase in whole-cell Bocillin-FL binding was not observed in the NaHCO(3)-non-responsive parental strain, COL, which contains the 246E PBP2a variant. Surprisingly, genetic swaps of the mecA coding sites between JE2 and COL did not alter the NaHCO(3)-enhanced binding seen in JE2 vs. COL. These data suggest that the non-coding regions of mecA may be involved in NaHCO(3)-responsiveness. This investigation also provides strong evidence that the NaHCO(3)-responsive phenotype in MRSA may involve NaHCO(3)-mediated increases in both initial cell surface β-lactam binding, as well as ultimate PBP2a binding of β-lactams.
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spelling pubmed-90281902022-04-23 Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes Ersoy, Selvi C. Chan, Liana C. Yeaman, Michael R. Chambers, Henry F. Proctor, Richard A. Ludwig, Kevin C. Schneider, Tanja Manna, Adhar C. Cheung, Ambrose Bayer, Arnold S. Antibiotics (Basel) Article Methicillin-resistant Staphylococcus aureus (MRSA) regulates resistance to β-lactams via preferential production of an alternative penicillin-binding protein (PBP), PBP2a. PBP2a binds many β-lactam antibiotics with less affinity than PBPs which are predominant in methicillin-susceptible (MSSA) strains. A novel, rather frequent in vitro phenotype was recently identified among clinical MRSA bloodstream isolates, termed “NaHCO(3)-responsiveness”. This phenotype features β-lactam susceptibility of certain MRSA strains only in the presence of NaHCO(3). Two distinct PBP2a variants, 246G and 246E, have been linked to the NaHCO(3)-responsive and NaHCO(3)-non-responsive MRSA phenotypes, respectively. To determine the mechanistic impact of PBP2a variants on β-lactam susceptibility, binding profiles of a fluorescent penicillin probe (Bocillin-FL) to each purified PBP2a variant were assessed and compared to whole-cell binding profiles characterized by flow cytometry in the presence vs. absence of NaHCO(3). These investigations revealed that NaHCO(3) differentially influenced the binding of the fluorescent penicillin, Bocillin-FL, to the PBP2a variants, with binding intensity and rate of binding significantly enhanced in the 246G compared to the 246E variant. Of note, the NaHCO(3)-β-lactam (oxacillin)-responsive JE2 strain, which natively harbors the 246G variant, had enhanced Bocillin-FL whole-cell binding following exposure to NaHCO(3). This NaHCO(3)-mediated increase in whole-cell Bocillin-FL binding was not observed in the NaHCO(3)-non-responsive parental strain, COL, which contains the 246E PBP2a variant. Surprisingly, genetic swaps of the mecA coding sites between JE2 and COL did not alter the NaHCO(3)-enhanced binding seen in JE2 vs. COL. These data suggest that the non-coding regions of mecA may be involved in NaHCO(3)-responsiveness. This investigation also provides strong evidence that the NaHCO(3)-responsive phenotype in MRSA may involve NaHCO(3)-mediated increases in both initial cell surface β-lactam binding, as well as ultimate PBP2a binding of β-lactams. MDPI 2022-03-30 /pmc/articles/PMC9028190/ /pubmed/35453214 http://dx.doi.org/10.3390/antibiotics11040462 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ersoy, Selvi C.
Chan, Liana C.
Yeaman, Michael R.
Chambers, Henry F.
Proctor, Richard A.
Ludwig, Kevin C.
Schneider, Tanja
Manna, Adhar C.
Cheung, Ambrose
Bayer, Arnold S.
Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes
title Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes
title_full Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes
title_fullStr Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes
title_full_unstemmed Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes
title_short Impacts of NaHCO(3) on β-Lactam Binding to PBP2a Protein Variants Associated with the NaHCO(3)-Responsive versus NaHCO(3)-Non-Responsive Phenotypes
title_sort impacts of nahco(3) on β-lactam binding to pbp2a protein variants associated with the nahco(3)-responsive versus nahco(3)-non-responsive phenotypes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9028190/
https://www.ncbi.nlm.nih.gov/pubmed/35453214
http://dx.doi.org/10.3390/antibiotics11040462
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