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Featured researches published by Anja Eichner.


PLOS ONE | 2014

Fast and Effective Photodynamic Inactivation of Multiresistant Bacteria by Cationic Riboflavin Derivatives

Tim Maisch; Anja Eichner; Andreas Späth; Anita Gollmer; Burkhard König; Johannes Regensburger; Wolfgang Bäumler

Photodynamic inactivation of bacteria (PIB) proves to be an additional method to kill pathogenic bacteria. PIB requires photosensitizer molecules that effectively generate reactive oxygen species like singlet oxygen when exposed to visible light. To allow a broad application in medicine, photosensitizers should be safe when applied in humans. Substances like vitamin B2, which are most likely safe, are known to produce singlet oxygen upon irradiation. In the present study, we added positive charges to flavin derivatives to enable attachment of these molecules to the negatively charged surface of bacteria. Two of the synthesized flavin derivatives showed a high quantum yield of singlet oxygen of approximately 75%. Multidrug resistant bacteria like MRSA (Methicillin resistant Staphylococcus aureus), EHEC (enterohemorrhagic Escherichia coli), Pseudomonas aeruginosa, and Acinetobacter baumannii were incubated with these flavin derivatives in vitro and were subsequently irradiated with visible light for seconds only. Singlet oxygen production in bacteria was proved by detecting its luminescence at 1270 nm. After irradiation, the number of viable bacteria decreased up to 6 log10 steps depending on the concentration of the flavin derivatives and the light dosimetry. The bactericidal effect of PIB was independent of the bacterial type and the corresponding antibiotic resistance pattern. In contrast, the photosensitizer concentration and light parameters used for bacteria killing did not affect cell viability of human keratinocytes (therapeutic window). Multiresistant bacteria can be safely and effectively killed by a combination of modified vitamin B2 molecules, oxygen and visible light, whereas normal skin cells survive. Further work will include these new photosensitizers for topical application to decolonize bacteria from skin and mucosa.


Photochemistry and Photobiology | 2018

A Closer Look at Dark Toxicity of the Photosensitizer TMPyP in Bacteria

Daniel B. Eckl; Linda Dengler; Marina Nemmert; Anja Eichner; Wolfgang Bäumler; Harald Huber

Photodynamic inactivation of bacteria (PIB) is based on photosensitizers which absorb light and generate reactive oxygen species (ROS), killing cells via oxidation. PIB is evaluated by comparing viability with and without irradiation, where reduction of viability in the presence of the photosensitizer without irradiation is considered as dark toxicity. This effect is controversially discussed for photosensitizers like TMPyP (5,10,15,20‐Tetrakis(1‐methyl‐4‐pyridinio)porphyrin tetra(p‐toluensulfonate). TMPyP shows a high absorption coefficient for blue light and a high yield of ROS production, especially singlet oxygen. Escherichia coli and Bacillus atrophaeus were incubated with TMPyP and irradiated with different light sources at low radiant exposures (μW per cm²), reflecting laboratory conditions of dark toxicity evaluation. Inactivation of E. coli occurs for blue light, while no effect was detectable for wavelengths >450 nm. Being more susceptible toward PIB, growth of B. atrophaeus is even reduced for light with emission >450 nm. Decreasing the light intensities to nW per cm² for B. atrophaeus, application of TMPyP still caused bacterial killing. Toxic effects of TMPyP disappeared after addition of histidine, quenching residual ROS. Our experiments demonstrate that the evaluation of dark toxicity of a powerful photosensitizer like TMPyP requires low light intensities and if necessary additional application of substances quenching any residual ROS.


The Journal of Infectious Diseases | 2009

Dynamics of Adaptive Microevolution of Hypermutable Pseudomonas aeruginosa during Chronic Pulmonary Infection in Patients with Cystic Fibrosis

Christina Hoboth; Reinhard Hoffmann; Anja Eichner; Christine Henke; Sabine Schmoldt; Axel Imhof; Jürgen Heesemann; Michael Hogardt


Photochemical and Photobiological Sciences | 2013

Dirty hands: photodynamic killing of human pathogens like EHEC, MRSA and Candida within seconds

Anja Eichner; Fernanda Pereira Gonzales; Ariane Felgenträger; Johannes Regensburger; Thomas Holzmann; Wulf Schneider-Brachert; Wolfgang Bäumler; Tim Maisch


Photochemical and Photobiological Sciences | 2015

Fast and effective inactivation of Bacillus atrophaeus endospores using light-activated derivatives of vitamin B2

Anja Eichner; Anita Gollmer; Andreas Späth; Wolfgang Bäumler; Johannes Regensburger; Burkhard König; Tim Maisch


International Journal of Medical Microbiology | 2015

Corrigendum to “Marker genes for the metabolic adaptation of Pseudomonas aeruginosa to the hypoxic cystic fibrosis lung environment” [Int. J. Med. Microbiol. 304 (2014) 1050–1061]

Anja Eichner; Nicole Günther; Martin Arnold; Max Schobert; Jürgen Heesemann; Michael Hogardt


Archive | 2017

1,7-DIARYL-1,6-HEPTADIEN-3,5-DION DERIVATIVES, METHODS OF MAKING AND USING THE SAME

Andreas Späth; Kristjan Plätzer; Tim Maisch; Anja Eichner


Archive | 2016

1,7-diaryl-1,6-heptadiene-3,5-dione derivatives, methods for the prodcution and use thereof

Andreas Späth; Kristjan Plätzer; Tim Maisch; Anja Eichner


Archive | 2016

1,7-diaryl-1,6-heptadien-3,5-dion-derivative, methoden zur herstellung und verwendung derselben

Andreas Späth; Kristjan Plätzer; Tim Maisch; Anja Eichner


PLOS ONE | 2014

Antimicrobial photodynamic efficacy of FLASH-01a.

Tim Maisch; Anja Eichner; Andreas Späth; Anita Gollmer; Burkhard König; Johannes Regensburger; Wolfgang Bäumler

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Tim Maisch

University of Regensburg

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Andreas Späth

University of Regensburg

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Anita Gollmer

University of Regensburg

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Michael Hogardt

Goethe University Frankfurt

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Daniel B. Eckl

University of Regensburg

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