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Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01

Bacillus mycoides SeITE01 is an environmental isolate that transforms the oxyanion selenite ([Formula: see text]) into the less bioavailable elemental selenium (Se(0)) forming biogenic selenium nanoparticles (Bio-SeNPs). In the present study, the reduction of sodium selenite (Na(2)SeO(3)) by SeITE01...

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Autores principales: Baggio, Greta, Groves, Ryan A., Chignola, Roberto, Piacenza, Elena, Presentato, Alessandro, Lewis, Ian A., Lampis, Silvia, Vallini, Giovanni, Turner, Raymond J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8481872/
https://www.ncbi.nlm.nih.gov/pubmed/34603239
http://dx.doi.org/10.3389/fmicb.2021.711000
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author Baggio, Greta
Groves, Ryan A.
Chignola, Roberto
Piacenza, Elena
Presentato, Alessandro
Lewis, Ian A.
Lampis, Silvia
Vallini, Giovanni
Turner, Raymond J.
author_facet Baggio, Greta
Groves, Ryan A.
Chignola, Roberto
Piacenza, Elena
Presentato, Alessandro
Lewis, Ian A.
Lampis, Silvia
Vallini, Giovanni
Turner, Raymond J.
author_sort Baggio, Greta
collection PubMed
description Bacillus mycoides SeITE01 is an environmental isolate that transforms the oxyanion selenite ([Formula: see text]) into the less bioavailable elemental selenium (Se(0)) forming biogenic selenium nanoparticles (Bio-SeNPs). In the present study, the reduction of sodium selenite (Na(2)SeO(3)) by SeITE01 strain and the effect of [Formula: see text] exposure on the bacterial cells was examined through untargeted metabolomics. A time-course approach was used to monitor both cell pellet and cell free spent medium (referred as intracellular and extracellular, respectively) metabolites in SeITE01 cells treated or not with [Formula: see text]. The results show substantial biochemical changes in SeITE01 cells when exposed to [Formula: see text]. The initial uptake of [Formula: see text] by SeITE01 cells (3h after inoculation) shows both an increase in intracellular levels of 4-hydroxybenzoate and indole-3-acetic acid, and an extracellular accumulation of guanosine, which are metabolites involved in general stress response adapting strategies. Proactive and defensive mechanisms against [Formula: see text] are observed between the end of lag (12h) and beginning of exponential (18h) phases. Glutathione and N-acetyl-L-cysteine are thiol compounds that would be mainly involved in Painter-type reaction for the reduction and detoxification of [Formula: see text] to Se(0). In these growth stages, thiol metabolites perform a dual role, both acting against the toxic and harmful presence of the oxyanion and as substrate or reducing sources to scavenge ROS production. Moreover, detection of the amino acids L-threonine and ornithine suggests changes in membrane lipids. Starting from stationary phase (24 and 48h), metabolites related to the formation and release of SeNPs in the extracellular environment begin to be observed. 5-hydroxyindole acetate, D-[+]-glucosamine, 4-methyl-2-oxo pentanoic acid, and ethanolamine phosphate may represent signaling strategies following SeNPs release from the cytoplasmic compartment, with consequent damage to SeITE01 cell membranes. This is also accompanied by intracellular accumulation of trans-4-hydroxyproline and L-proline, which likely represent osmoprotectant activity. The identification of these metabolites suggests the activation of signaling strategies that would protect the bacterial cells from [Formula: see text] toxicity while it is converting into SeNPs.
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spelling pubmed-84818722021-10-01 Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01 Baggio, Greta Groves, Ryan A. Chignola, Roberto Piacenza, Elena Presentato, Alessandro Lewis, Ian A. Lampis, Silvia Vallini, Giovanni Turner, Raymond J. Front Microbiol Microbiology Bacillus mycoides SeITE01 is an environmental isolate that transforms the oxyanion selenite ([Formula: see text]) into the less bioavailable elemental selenium (Se(0)) forming biogenic selenium nanoparticles (Bio-SeNPs). In the present study, the reduction of sodium selenite (Na(2)SeO(3)) by SeITE01 strain and the effect of [Formula: see text] exposure on the bacterial cells was examined through untargeted metabolomics. A time-course approach was used to monitor both cell pellet and cell free spent medium (referred as intracellular and extracellular, respectively) metabolites in SeITE01 cells treated or not with [Formula: see text]. The results show substantial biochemical changes in SeITE01 cells when exposed to [Formula: see text]. The initial uptake of [Formula: see text] by SeITE01 cells (3h after inoculation) shows both an increase in intracellular levels of 4-hydroxybenzoate and indole-3-acetic acid, and an extracellular accumulation of guanosine, which are metabolites involved in general stress response adapting strategies. Proactive and defensive mechanisms against [Formula: see text] are observed between the end of lag (12h) and beginning of exponential (18h) phases. Glutathione and N-acetyl-L-cysteine are thiol compounds that would be mainly involved in Painter-type reaction for the reduction and detoxification of [Formula: see text] to Se(0). In these growth stages, thiol metabolites perform a dual role, both acting against the toxic and harmful presence of the oxyanion and as substrate or reducing sources to scavenge ROS production. Moreover, detection of the amino acids L-threonine and ornithine suggests changes in membrane lipids. Starting from stationary phase (24 and 48h), metabolites related to the formation and release of SeNPs in the extracellular environment begin to be observed. 5-hydroxyindole acetate, D-[+]-glucosamine, 4-methyl-2-oxo pentanoic acid, and ethanolamine phosphate may represent signaling strategies following SeNPs release from the cytoplasmic compartment, with consequent damage to SeITE01 cell membranes. This is also accompanied by intracellular accumulation of trans-4-hydroxyproline and L-proline, which likely represent osmoprotectant activity. The identification of these metabolites suggests the activation of signaling strategies that would protect the bacterial cells from [Formula: see text] toxicity while it is converting into SeNPs. Frontiers Media S.A. 2021-09-16 /pmc/articles/PMC8481872/ /pubmed/34603239 http://dx.doi.org/10.3389/fmicb.2021.711000 Text en Copyright © 2021 Baggio, Groves, Chignola, Piacenza, Presentato, Lewis, Lampis, Vallini and Turner. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Baggio, Greta
Groves, Ryan A.
Chignola, Roberto
Piacenza, Elena
Presentato, Alessandro
Lewis, Ian A.
Lampis, Silvia
Vallini, Giovanni
Turner, Raymond J.
Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01
title Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01
title_full Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01
title_fullStr Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01
title_full_unstemmed Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01
title_short Untargeted Metabolomics Investigation on Selenite Reduction to Elemental Selenium by Bacillus mycoides SeITE01
title_sort untargeted metabolomics investigation on selenite reduction to elemental selenium by bacillus mycoides seite01
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8481872/
https://www.ncbi.nlm.nih.gov/pubmed/34603239
http://dx.doi.org/10.3389/fmicb.2021.711000
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