191 research outputs found
The kINPen—a review on physics and chemistry of the atmospheric pressure plasma jet and its applications
The kINPen® plasma jet was developed from laboratory prototype to commercially available non-equilibrium cold plasma jet for various applications in materials research, surface treatment and medicine. It has proven to be a valuable plasma source for industry as well as research and commercial use in plasma medicine, leading to very successful therapeutic results and its certification as a medical device. This topical review presents the different kINPen plasma sources available. Diagnostic techniques applied to the kINPen are introduced. The review summarizes the extensive studies of the physics and plasma chemistry of the kINPen performed by research groups across the world, and closes with a brief overview of the main application fields
Using a dual plasma process to produce cobalt--polypyrrole catalysts for the oxygen reduction reaction in fuel cells -- part II: analysing the chemical structure of the films
The chemical structure of cobalt--polypyrrole -- produced by a dual plasma
process -- is analysed by means of X-ray photoelectron spectroscopy (XPS), near
edge X-ray absorption spectroscopy (NEXAFS), X-ray diffraction (XRD),
energy-dispersive X-Ray spectroscopy (EDX) and extended x-ray absorption
spectroscopy (EXAFS).It is shown that only nanoparticles of a size of 3\,nm
with the low temperature crystal structure of cobalt are present within the
compound. Besides that, cobalt--nitrogen and carbon--oxygen structures are
observed. Furthermore, more and more cobalt--nitrogen structures are produced
when increasing the magnetron power. Linking the information on the chemical
structure to the results about the catalytic activity of the films -- which are
presented in part I of this contribution -- it is concluded that the
cobalt--nitrogen structures are the probable catalytically active sites. The
cobalt--nitrogen bond length is calculated as 2.09\,\AA\ and the
carbon--nitrogen bond length as 1.38\,\AA
Towards a Machine-Learned Poisson Solver for Low-Temperature Plasma Simulations in Complex Geometries
Poisson's equation plays an important role in modeling many physical systems.
In electrostatic self-consistent low-temperature plasma (LTP) simulations,
Poisson's equation is solved at each simulation time step, which can amount to
a significant computational cost for the entire simulation. In this paper, we
describe the development of a generic machine-learned Poisson solver
specifically designed for the requirements of LTP simulations in complex 2D
reactor geometries on structured Cartesian grids. Here, the reactor geometries
can consist of inner electrodes and dielectric materials as often found in LTP
simulations. The approach leverages a hybrid CNN-transformer network
architecture in combination with a weighted multiterm loss function. We train
the network using highly-randomized synthetic data to ensure the
generalizability of the learned solver to unseen reactor geometries. The
results demonstrate that the learned solver is able to produce quantitatively
and qualitatively accurate solutions. Furthermore, it generalizes well on new
reactor geometries such as reference geometries found in the literature. To
increase the numerical accuracy of the solutions required in LTP simulations,
we employ a conventional iterative solver to refine the raw predictions,
especially to recover the high-frequency features not resolved by the initial
prediction. With this, the proposed learned Poisson solver provides the
required accuracy and is potentially faster than a pure GPU-based conventional
iterative solver. This opens up new possibilities for developing a generic and
high-performing learned Poisson solver for LTP systems in complex geometries
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Quantification of the ozone and singlet delta oxygen produced in gas and liquid phases by a non-thermal atmospheric plasma with relevance for medical treatment
In the field of plasma medicine, the identification of relevant reactive species in the liquid phase is highly important. To design the plasma generated species composition for a targeted therapeutic application, the point of origin of those species needs to be known. The dominant reactive oxygen species generated by the plasma used in this study are atomic oxygen, ozone, and singlet delta oxygen. The species density changes with the distance to the active plasma zone, and, hence, the oxidizing potential of this species cocktail can be tuned by altering the treatment distance. In both phases (gas and liquid), independent techniques have been used to determine the species concentration as a function of the distance. The surrounding gas composition and ambient conditions were controlled between pure nitrogen and air-like by using a curtain gas device. In the gas phase, in contrast to the ozone density, the singlet delta oxygen density showed to be more sensitive to the distance. Additionally, by changing the surrounding gas, admixing or not molecular oxygen, the dynamics of ozone and singlet delta oxygen behave differently. Through an analysis of the reactive species development for the varied experimental parameters, the importance of several reaction pathways for the proceeding reactions was evaluated and some were eventually excluded
Non-steroidal anti-inflammatory drugs: recent advances in the use of synthetic COX-2 inhibitors
Cyclooxygenase (COX) enzymes comprise COX-1 and COX-2 isoforms and are responsible for prostaglandin production. Prostaglandins have critical roles in the inflammation pathway and must be controlled by administration of selective nonsteroidal anti-inflammatory drugs (NSAIDs). Selective COX-2 inhibitors have been among the most used NSAIDs during the ongoing coronavirus 2019 pandemic because they reduce pain and protect against inflammation-related diseases. In this framework, the mechanism of action of both COX isoforms (particularly COX-2) as inflammation mediators must be reviewed. Moreover, proinflammatory cytokines such as tumor necrosis factor-α and interleukin (IL)-6, IL-1β, and IL-8 must be highlighted due to their major participation in upregulation of the inflammatory reaction. Structural and functional analyses of selective COX-2 inhibitors within the active-site cavity of COXs could enable introduction of lead structures with higher selectivity and potency against inflammation with fewer adverse effects. This review focuses on the biological activity of recently discovered synthetic COX-2, dual COX-2/lipoxygenase, and COX-2/soluble epoxide hydrolase hybrid inhibitors based primarily on the active motifs of related US Food and Drug Administration-approved drugs. These new agents could provide several advantages with regard to anti-inflammatory activity, gastrointestinal protection, and a safer profile compared with those of the NSAIDs celecoxib, valdecoxib, and rofecoxib
The kINPen—a review on physics and chemistry of the atmospheric pressure plasma jet and its applications
ABSTRACT: The kINPen® plasma jet was developed from laboratory prototype to commercially available non-equilibrium cold plasma jet for various applications in materials research, surface treatment and medicine. It has proven to be a valuable plasma source for industry as well as research and commercial use in plasma medicine, leading to very successful therapeutic results and its certification as a medical device. This topical review presents the different kINPen plasma sources available. Diagnostic techniques applied to the kINPen are introduced. The review summarizes the extensive studies of the physics and plasma chemistry of the kINPen performed by research groups across the world, and closes with a brief overview of the main application fields
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Non-touching plasma–liquid interaction – where is aqueous nitric oxide generated?
Mass transport through graphene is receiving increasing attention due to the potential for molecular sieving. Experimental studies are mostly limited to the translocation of protons, ions, and water molecules, and results for larger molecules through graphene are rare. Here, we perform controlled radical polymerization with surface-anchored self-assembled initiator monolayer in a monomer solution with single-layer graphene separating the initiator from the monomer. We demonstrate that neutral monomers are able to pass through the graphene (via native defects) and increase the graphene defects ratio (Raman ID/IG) from ca. 0.09 to 0.22. The translocations of anionic and cationic monomers through graphene are significantly slower due to chemical interactions of monomers with the graphene defects. Interestingly, if micropatterned initiator-monolayers are used, the translocations of anionic monomers apparently cut the graphene sheet into congruent microscopic structures. The varied interactions between monomers and graphene defects are further investigated by quantum molecular dynamics simulations
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A Comparison of Floating-Electrode DBD and kINPen Jet: Plasma Parameters to Achieve Similar Growth Reduction in Colon Cancer Cells Under Standardized Conditions
A comparative study of two plasma sources (floating-electrode dielectric barrier discharge, DBD, Drexel University; atmospheric pressure argon plasma jet, kINPen, INP Greifswald) on cancer cell toxicity was performed. Cell culture protocols, cytotoxicity assays, and procedures for assessment of hydrogen peroxide (H2O2) were standardized between both labs. The inhibitory concentration 50 (IC50) and its corresponding H2O2 deposition was determined for both devices. For the DBD, IC50 and H2O2 generation were largely dependent on the total energy input but not pulsing frequency, treatment time, or total number of cells. DBD cytotoxicity could not be replicated by addition of H2O2 alone and was inhibited by larger amounts of liquid present during the treatment. Jet plasma toxicity depended on peroxide generation as well as total cell number and amount of liquid. Thus, the amount of liquid present during plasma treatment in vitro is key in attenuating short-lived species or other physical effects from plasmas. These in vitro results suggest a role of liquids in or on tissues during plasma treatment in a clinical setting. Additionally, we provide a platform for correlation between different plasma sources for a predefined cellular response
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