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On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling

Cold atmospheric plasmas (CAPs) are promising medical tools and are currently applied in dermatology and epithelial cancers. While understanding of the biomedical effects is already substantial, knowledge on the contribution of individual ROS and RNS and the mode of activation of biochemical pathway...

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Autores principales: Wende, Kristian, Bruno, Giuliana, Lalk, Michael, Weltmann, Klaus-Dieter, von Woedtke, Thomas, Bekeschus, Sander, Lackmann, Jan-Wilm
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9051657/
https://www.ncbi.nlm.nih.gov/pubmed/35496584
http://dx.doi.org/10.1039/c9ra08745a
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author Wende, Kristian
Bruno, Giuliana
Lalk, Michael
Weltmann, Klaus-Dieter
von Woedtke, Thomas
Bekeschus, Sander
Lackmann, Jan-Wilm
author_facet Wende, Kristian
Bruno, Giuliana
Lalk, Michael
Weltmann, Klaus-Dieter
von Woedtke, Thomas
Bekeschus, Sander
Lackmann, Jan-Wilm
author_sort Wende, Kristian
collection PubMed
description Cold atmospheric plasmas (CAPs) are promising medical tools and are currently applied in dermatology and epithelial cancers. While understanding of the biomedical effects is already substantial, knowledge on the contribution of individual ROS and RNS and the mode of activation of biochemical pathways is insufficient. Especially the formation and transport of short-lived reactive species in liquids remain elusive, a situation shared with other approaches involving redox processes such as photodynamic therapy. Here, the contribution of plasma-generated reactive oxygen species (ROS) in plasma liquid chemistry was determined by labeling these via admixing heavy oxygen (18)O(2) to the feed gas or by using heavy water H(2)(18)O as a solvent for the bait molecule. The inclusion of heavy or light oxygen atoms by the labeled ROS into the different cysteine products was determined by mass spectrometry. While products like cysteine sulfonic acid incorporated nearly exclusively gas phase-derived oxygen species (atomic oxygen and/or singlet oxygen), a significant contribution of liquid phase-derived species (OH radicals) was observed for cysteine-S-sulfonate. The role, origin, and reaction mechanisms of short-lived species, namely hydroxyl radicals, singlet oxygen, and atomic oxygen, are discussed. Interactions of these species both with the target cysteine molecule as well as the interphase and the liquid bulk are taken into consideration to shed light onto several reaction pathways resulting in observed isotopic oxygen incorporation. These studies give valuable insight into underlying plasma–liquid interaction processes and are a first step to understand these interaction processes between the gas and liquid phase on a molecular level.
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spelling pubmed-90516572022-04-29 On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling Wende, Kristian Bruno, Giuliana Lalk, Michael Weltmann, Klaus-Dieter von Woedtke, Thomas Bekeschus, Sander Lackmann, Jan-Wilm RSC Adv Chemistry Cold atmospheric plasmas (CAPs) are promising medical tools and are currently applied in dermatology and epithelial cancers. While understanding of the biomedical effects is already substantial, knowledge on the contribution of individual ROS and RNS and the mode of activation of biochemical pathways is insufficient. Especially the formation and transport of short-lived reactive species in liquids remain elusive, a situation shared with other approaches involving redox processes such as photodynamic therapy. Here, the contribution of plasma-generated reactive oxygen species (ROS) in plasma liquid chemistry was determined by labeling these via admixing heavy oxygen (18)O(2) to the feed gas or by using heavy water H(2)(18)O as a solvent for the bait molecule. The inclusion of heavy or light oxygen atoms by the labeled ROS into the different cysteine products was determined by mass spectrometry. While products like cysteine sulfonic acid incorporated nearly exclusively gas phase-derived oxygen species (atomic oxygen and/or singlet oxygen), a significant contribution of liquid phase-derived species (OH radicals) was observed for cysteine-S-sulfonate. The role, origin, and reaction mechanisms of short-lived species, namely hydroxyl radicals, singlet oxygen, and atomic oxygen, are discussed. Interactions of these species both with the target cysteine molecule as well as the interphase and the liquid bulk are taken into consideration to shed light onto several reaction pathways resulting in observed isotopic oxygen incorporation. These studies give valuable insight into underlying plasma–liquid interaction processes and are a first step to understand these interaction processes between the gas and liquid phase on a molecular level. The Royal Society of Chemistry 2020-03-17 /pmc/articles/PMC9051657/ /pubmed/35496584 http://dx.doi.org/10.1039/c9ra08745a Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Wende, Kristian
Bruno, Giuliana
Lalk, Michael
Weltmann, Klaus-Dieter
von Woedtke, Thomas
Bekeschus, Sander
Lackmann, Jan-Wilm
On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
title On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
title_full On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
title_fullStr On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
title_full_unstemmed On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
title_short On a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
title_sort on a heavy path – determining cold plasma-derived short-lived species chemistry using isotopic labelling
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9051657/
https://www.ncbi.nlm.nih.gov/pubmed/35496584
http://dx.doi.org/10.1039/c9ra08745a
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