Etablierung eines kompetitiven ELSIA für den Nachweis von Gliotoxin

Lindenhahn, Jakob

07 June 2022

Gliotoxin ist ein ubiquitär vorkommendes Mykotoxin und wird unter anderem von Aspergillus sp. gebildet. Das Gliotoxin ist toxisch und stellt für Mensch und Tier ein gesundheitliches Risiko dar. Über die Aufnahme von kontaminierten Futtermitteln (FM) kann es in tierische Produkte und anschließend in die Nahrungsmittelkette gelangen. Dem Mykotoxin werden starke immunmodulatorische Eigenschaften zugeschrieben. Gliotoxin gilt als eine sehr reaktive Verbindung, die in der Umwelt schnell zu bis(methylthio)Gliotoxin (bmGliotoxin) umgesetzt werden kann. Dieser Metabolit ist sowohl atoxisch als auch biologisch inaktiv und wird aufgrund seiner Stabilität als ein wichtiger und zuverlässiger Diagnostikmarker beschrieben. In der Mykotoxinanalytik werden Konzentrationsbestimmungen primär durch chromato-graphische Verfahren durchgeführt. Mit diesen Verfahren konnten bereits Gliotoxin-Konzentrationen in verschiedensten FM bestimmt werden. Im Gegensatz zu anderen prominenten Mykotoxinen gibt es für das Gliotoxin kein Nachweisverfahren für routinemäßige Kontrolluntersuchungen. Daher war das Ziel der Dissertationsarbeit die Entwicklung eines ELISA, mit dem Gliotoxin in FM einfach und schnell bestimmt werden kann. Es wurden zunächst geeignete Protein-Gliotoxin-Konjugate für die Anti-Gliotoxin-Immunisierung hergestellt. Kaninchen wurden nach einem festgelegten Protokoll mit diesen Hapten-Konjugaten immunisiert (Kurzzeit- bzw. Langzeitimmunisierung). Anschließend erfolgte die Titerbestimmung in den Antiseren und die Überprüfung der Paratophemmbarkeit durch freies Gliotoxin. Aus dem Antiserum mit der höchsten IgG-anti-Gliotoxin-Konzentration wurden die Antikörper antigenaffinitäts-chromatografisch aufgereinigt. Zusätzlich wurde für den kompetitiven ELISA ein geeignetes Gliotoxin-Peroxidase-Konjugat hergestellt. Alle Testkomponenten wurden vorab geprüft und danach der kompetitive Gliotoxin-ELISA validiert. Mit dem optimierten kompetitiven Testsystem wurden die Gliotoxin-Konzentrationen in Schimmelpilz-Kulturüberständen (Aspergillus sp.) gemessen. Anschließend erfolgte die Untersuchung von Futtermittelproben (Silagen) auf Gliotoxin. Nach der entsprechenden Probenaufbereitung der FM wurde das Gliotoxin im kompetitiven ELISA ebenfalls quantitativ bestimmt. Die hier gemessenen Gliotoxin-Konzentrationen wurden mit Ergebnissen aus parallel durchgeführten Untersuchungen mit der LC-MS/MS verglichen. Mit dem entwickelten kompetitiven ELISA sind quantitative Aussagen zu erhöhten Gliotoxin-Konzentrationen in verschiedenen Probenmaterialien möglich. Das Mykotoxin kann sowohl frei in seiner nativen Form, gebunden an Proteine oder metabolisiert als bis(methylthio)gliotoxin detektiert werden. Mit dem Testsystem kann die quantitative Produktion von Gliotoxin durch verschiedene Schimmelpilzarten beurteilt werden. Die untersuchten FM (Silageproben) konnten im entwickelten ELISA alle erfolgreich gemessen und beurteilt werden.:1 Einleitung 1 2 Literaturübersicht 2 2.1 Schimmelpilze 2 2.1.1 Definition und Zuordnung 2 2.1.2 Vorkommen in der Umwelt 4 2.1.3 Bedeutung und Nutzen 5 2.1.4 Schadwirkung für Mensch und Tier 7 2.2 Mykotoxine 9 2.3 Gliotoxin 10 2.3.1 Allgemeine Merkmale 10 2.3.2 Bis(methylthio)Gliotoxin 16 2.3.3 Ausgewählte Pathogenitätsmechanismen 17 2.3.3.1 Redox-Zirkel und ROS-Produktion 17 2.3.3.2 Verschiebung des TH1/ TH2-Gleichgewichtes 18 2.3.3.3 Inhibition des Transkriptionsfaktors NF-κB 19 2.3.3.4 Einleitung von Apoptose und Nekrose 20 2.3.3.5 Inhibition von Mastzellen 21 2.3.4 Nachweisverfahren 22 2.3.4.1 Chromatographie 22 2.3.4.2 Enzyme-linked Immunosorbent Assay (ELISA) 23 2.3.5 Quantitative Mengenbestimmungen in Proben 25 2.3.5.1 Klinisches Probenmaterial 25 2.3.5.2 Belastete Futtermittelproben 27 2.3.5.3 Belastete Lebensmittelproben 33 3 Material und Methoden 34 3.1 Gliotoxin, Chemikalien und ausgewählte Laborgeräte 34 3.2 Gliotoxin-Hapten für die Immunisierung 35 3.3 Immunisierung 37 3.4 Untersuchung der Anti-Gliotoxin-Antiseren 37 3.4.1 Protein-Gliotoxin-Konjugate für ELISA 37 3.4.2 ELISA für Antiserumuntersuchung 39 3.4.3 ELISA für die Bestimmung der IgG-Konzentrationen anti-Gliotoxin 40 3.5 Etablierung des kompetitiven Gliotoxin-ELISA 42 3.5.1 Isolierung der IgG-anti-Gliotoxin 42 3.5.2 Herstellung des Gliotoxin-HRP-Konjugates 43 3.5.3 Prüfung der Testkomponenten 44 3.5.4 Validierung des kompetitiven Gliotoxin-ELISA 45 3.6 Untersuchung von Kreuzreaktionen 45 3.7 Untersuchung von Pilzkulturen auf Gliotoxin 45 3.8 Untersuchung von Futtermitteln auf Gliotoxin 47 3.8.1 Untersuchung von dotiertem Futtermittel 47 3.8.2 Futtermitteluntersuchung mit dem Gliotoxin-ELISA 48 3.8.3 Futtermitteluntersuchung mit der LC-MS/MS 49 3.9 Datenauswertung 49 4 Ergebnisse 50 4.1 Hapten für die Immunisierung 50 4.2 Untersuchung der Anti-Gliotoxin-Antiseren 50 4.2.1 Titerbestimmung 50 4.2.2 Bestimmung der Hemmungsrate durch freies Gliotoxin 51 4.2.3 IgG-anti-Gliotoxin-Konzentration in den Antiseren 53 4.3 Untersuchung der Antiseren 55 4.3.1 Isolierung des IgG-anti-Gliotoxin 55 4.3.2 Voruntersuchungen für die Etablierung des kompetitiven Gliotoxin-ELISA 57 4.3.3 Validierung des kompetitiven Gliotoxin-ELISA 60 4.4 Untersuchung von Kreuzreaktionen 64 4.5 Untersuchung von Pilzkulturen auf Gliotoxin 65 4.6 Untersuchung von Futtermitteln auf Gliotoxin 68 4.6.1 Untersuchung mit Gliotoxin dotierter Futtermittel 68 4.6.2 Futtermitteluntersuchung mit Gliotoxin-ELISA und LC-MS/MS 71 4.7 Auswertung und Bewertung 73 5 Diskussion 78 5.1 Bewertung der Gliotoxin-Antigen Entwicklung 78 5.2 Bewertung der Antiseren nach Immunisierung (28d- und 91d-Protokoll) 79 5.3 Etablierung des kompetitiven ELISA 83 5.4 Bewertung der Pilze und der Kulturüberstände 85 5.5 Bewertung der Futtermittel 88 6 Zusammenfassung 96 7 Summary 98 8 Literaturverzeichnis 100 9 Anhang 116

info:eu-repo/classification/ddc/636.089

ddc:636.089

info:eu-repo/classification/ddc/630

ddc:630

Česká masmédia a Bezpečnostní informační služba: mediální obraz výroční zprávy BIS / Czech mass media and Security information Service: media perspective on the annual reports of the BIS

Primasová, Rachel

January 2021

The diploma thesis Czech mass media and Security Information Service: media perspective of the annual report of BIS focuses on the image of the annual report published by the Security Information Service (often used acronym "BIS") in selected mass media: servers Parlamentni listy, Aktualne, and daily newspaper Lidove noviny. The author is looking to answer the research question Do Czech mass media present the annual report of the BIS differently? If yes, why? The author follows the hypothesis that Czech mass media contribute a different image of BIS. The reason for these contrasting opinions lies both in the internal and external factors, such as changes in ownership structures, other relationships with the BIS, or various attributes of readers. Firstly, the author describes existing literature, theory and its application, and methodology. Concerning media theory is explained and linked to the idea of social constructivism. At the example of selected foreign information services, the author highlights the Security Information Service and mass media relationship complexity. In the empirical part, the diploma thesis continues with applying quantitative content analysis in the selected time range of 1996-2019. The author explains the different media coverage, frequency of media communication, and various...

Friedensdenken und Friedensbewegung in Symbiose: Abschlussveranstaltung Dresdener Studiengemeinschaft Sicherheitspolitik, Oktober 2015

Bald, Detlef, Bialas, Volker, Böhme, Rainer, Hagena, Hermann, Haueis, Eberhard, Hoffmann, Theodor, Kiss, Endre, Schreiber, Wilfried, Schröter, Lothar

15 January 2019

Dokumentation der Abschließenden Veranstaltung der Dresdener Studiengemeinschaft Sicherheitspolitik e. V. am 15. Oktober 2015, im Volkshaus Dresden-Laubegast.:Vorbemerkung. Redebeiträge: 25-jähriger Entwicklungsweg der Dresdener Studiengemeinschaft Sicherheitspolitik. - Rainer Böhme, Eberhard Haueis, Eine eindrucksvolle Power-Point-Präsentation (60 min). Zusammenfassender Bericht. - Wolfgang Scheler, Vom Geist, der uns getragen hat. Beiträge der Kooperationspartner und Vereinsmitglieder: - Detlev Bald, Es wird fehlen, was aus Dresden kam. - Theodor Hoffmann, Hochachtung und Dank für das Geleistete. - Hermann Hagena, 25 Jahre DSS – ein Blick zurück. - Volker Bialas, Grußadresse. - Endre Kiss, Gedanken zum Abschied. - Siegfried Schönherr, DSS-Arbeitspapiere – eine zufriedenstellende Bilanz. - Lothar Schröter, Konsequentes und couragiertes friedenspolitisches Denken. - Wifried Schreiber, Symbiose von Friedensforschung und Friedensbewegung.

info:eu-repo/classification/ddc/355

ddc:355

A study on positive electrode materials for sodium secondary batteries utilizing ionic liquids as electrolytes / イオン液体を電解質として用いるナトリウム二次電池の正極材料に関する研究

Chen, Chih-Yao

24 September 2014

京都大学 / 0048 / 新制・課程博士 / 博士(エネルギー科学) / 甲第18607号 / エネ博第303号 / 新制||エネ||62(附属図書館) / 31507 / 京都大学大学院エネルギー科学研究科エネルギー基礎科学専攻 / (主査)教授 萩原 理加, 教授 佐川 尚, 教授 平藤 哲司 / 学位規則第4条第1項該当 / Doctor of Energy Science / Kyoto University / DFAM

Sodium secondary battery

Positive electrode material

Sodium chromium oxide

Sodium iron pyrophosphate

Sodium manganese silicate

Ionic liquid

Bis(fluorosulfonyl)amide

501

Studies on the Reactivity of a Bis–Mesityl Imidazolyl Carbene Intermediate toward Carbon Dioxide and Stability of the Resulting Carboxylate

Ka, Seon Young

23 August 2019

No description available.

Analytical Chemistry

Chemistry

Climate Change

Bis-mesityl imidazolyl carbene

Imidazolium-2-carboxylate synthesis

CO2 adduct

Hydrolytic stability

Reductive conversion of CO2

CO2 reduction

Gold Nanoparticles as Boron Carriers for Boron Neutron Capture Therapy: Synthesis, Radiolabelling and In Vivo Evaluation

Pulagam, Krishna R., Gona, Kiran B., Gómez-Vallejo, Vanessa, Meijer, Jan, Zilberfain, Carolin, Estrela-Lopis, Irina, Baz, Zuriñe, Cossío, Unai, Llop, Jordi

11 April 2023

Background: Boron Neutron Capture Therapy (BNCT) is a binary approach to cancer therapy that requires accumulation of boron atoms preferentially in tumour cells. This can be achieved by using nanoparticles as boron carriers and taking advantage of the enhanced permeability and retention (EPR) effect. Here, we present the preparation and characterization of size and shape-tuned gold NPs (AuNPs) stabilised with polyethylene glycol (PEG) and functionalized with the boron-rich anion cobalt bis(dicarbollide), commonly known as COSAN. The resulting NPs were radiolabelled with 124I both at the core and the shell, and were evaluated in vivo in a mouse model of human fibrosarcoma (HT1080 cells) using positron emission tomography (PET). Methods: The thiolated COSAN derivatives for subsequent attachment to the gold surface were synthesized by reaction of COSAN with tetrahydropyran (THP) followed by ring opening using potassium thioacetate (KSAc). Iodination on one of the boron atoms of the cluster was also carried out to enable subsequent radiolabelling of the boron cage. AuNPs grafted with mPEG-SH (5 Kda) and thiolated COSAN were prepared by ligand displacement. Radiolabelling was carried out both at the shell (isotopic exchange) and at the core (anionic absorption) of the NPs using 124I to enable PET imaging. Results: Stable gold nanoparticles simultaneously functionalised with PEG and COSAN (PEG-AuNPs@[4]) with hydrodynamic diameter of 37.8 0.5 nm, core diameter of 19.2 1.4 nm and -potential of 18.0 0.7 mV were obtained. The presence of the COSAN on the surface of the NPs was confirmed by Raman Spectroscopy and UV-Vis spectrophotometry. PEG-AuNPs@[4] could be efficiently labelled with 124I both at the core and the shell. Biodistribution studies in a xenograft mouse model of human fibrosarcoma showed major accumulation in liver, lungs and spleen, and poor accumulation in the tumour. The dual labelling approach confirmed the in vivo stability of the PEG-AuNPs@[4]. Conclusions: PEG stabilized, COSAN-functionalised AuNPs could be synthesized, radiolabelled and evaluated in vivo using PET. The low tumour accumulation in the animal model assayed points to the need of tuning the size and geometry of the gold core for future studies.

info:eu-repo/classification/ddc/540

ddc:540

Structure and Exciton Coupling in Jet-Cooled Bichromophores

Hamza, Abdulhamid

23 March 2008

No description available.

Chemistry

spectroscopy

exciton coupling

supersonic jet

dimer

excited states

deuterated

1,2-diphenylethane

1,2-bis(4-methylphenyl)ethane

1,2-diphenylcyclopropane

2-phenylindane

2-(4-fluorophenyl)indane

BUSINESS INTELLIGENCE AND LEARNING, DRIVERS OF QUALITY AND COMPETITIVE PERFORMANCE

Joseph, Woodside M.

10 May 2011

No description available.

Business Administration

Computer Science

Health Care

Health Care Management

Information Systems

Information Technology

BI

BIS

Business Intelligence

Healthcare

Quality

Learning

Competitive Performance

Bis(trimethylstannyl)benzopinacolate Promoted Radical Carbon-Carbon Bond Forming Reactions and Related Studies

Seely, Franklin Lee

16 December 2010

No description available.

Chemistry

organic free radical

non-chain

radical conjugate addition

intermolecular radical

bis(trimethylstannyl)benzopinacolate

free radical

stable free radical

radical one carbon homologation

free radical homologation

Siloxane-Based Reinforcement of Polysiloxanes: from Supramolecular Interactions to Nanoparticles

Cashman, Mark Francis

01 October 2020

Polysiloxanes represent a unique class of synthetic polymers, employing a completely inorganic backbone structure comprised of repeating –(Si–O)n– 'siloxane' main chain linkages. This results in an assortment of diverse properties exclusive to the siloxane bond that clearly distinguish them from the –(C–C)n– backbone of purely organic polymers. Previous work has elucidated a methodology for fabricating flexible and elastic crosslinked poly(dimethyl siloxane) (PDMS) constructs with high Mc through a simultaneous crosslinking and chain-extension methodology. However, these constructs suffer the poor mechanical properties typical of lower molecular weight crosslinked siloxanes (e.g. modulus, tear strength, and strain at break). Filled PDMS networks represent another important class of elastomers in which fillers, namely silica and siloxane-based fillers, impart improved mechanical properties to otherwise weak PDMS networks. This work demonstrates that proper silicon-based reinforcing agent selection (e.g. siloxane-based MQ copolymer nanoparticles) and incorporation provides a synergistic enhancement to mechanical properties, whilst maintaining a low viscosity liquid composition, at high loading content, without the use of co-solvents or heating. Rheological analysis evaluates the viscosity while photorheology and photocalorimetry measurements evaluate rate and extent of curing of the various MQ-loaded formulations, demonstrating theoretical printability up to 40 wt% MQ copolymer nanoparticle incorporation. Dynamic mechanical analysis (DMA) and tensile testing evaluated thermomechanical and mechanical properties of the cured nanocomposites as a function of MQ loading content, demonstrating a 3-fold increase in ultimate stress at 50 wt% MQ copolymer nanoparticle incorporation. VP AM of the 40 wt% MQ-loaded, photo-active PDMS formulation demonstrates facile amenability of photo-active PDMS formulations with high MQ-loading content to 3D printing processes with promising results. PDMS polyureas represent an important class of elastomers with unique properties derived from the synergy between the nonpolar nature, unusual flexibility, and low glass transition temperature (Tg) afforded by the backbone siloxane linkages (-Si-O)n- of PDMS and the exceptional hydrogen bond ordering and strength evoked by the bidentate hydrogen bonding of urea. The work herein presents an improved melt polycondensation synthetic methodology, which strategically harnesses the spontaneous pyrolytic degradation of urea to afford a series of PDMS polyureas via reactions at high temperatures in the presence of telechelic amine-terminated oligomeric poly(dimethyl siloxane) (PDMS1.6k-NH2) and optional 1,3-bis(3-aminopropyl)tetramethyldisiloxane (BATS) chain extender. This melt polycondensation approach uniquely circumvents the accustomed prerequisite of isocyanate monomer, solvent, and metal catalysts to afford isocyanate-free PDMS polyureas using bio-derived urea with the only reaction byproduct being ammonia, a fundamental raw ingredient for agricultural and industrial products. As professed above, reinforcement of polysiloxane materials is ascertained via the incorporation of reinforcing fillers or nanoparticles (typically fumed silica) or blocky or segmented development of polymer chains eliciting microphase separation, in order to cajole the elongation potential of polysiloxanes. Herein, a facile approach is detailed towards the synergistic fortification of PDMS-based materials through a collaborative effort between both primary methods of polysiloxane reinforcement. A novel one-pot methodology towards the facile, in situ incorporation of siloxane-based MQ copolymer nanoparticles into segmented PDMS polyureas to afford MQ-loaded thermoplastic and thermoplastic elastomer PDMS polyureas is detailed. The isocyanate-free melt polycondensation achieves visible melt dispersibility of MQ copolymer nanoparticles (good optical clarity) and affords segmented PDMS polyureas while in the presence of MQ nanoparticles, up to 40 wt% MQ, avoiding post-polymerization solvent based mixing, the only other reported alternative. Incorporation of MQ copolymer nanoparticles into segmented PDMS polyureas provides significant enhancements to modulus and ultimate stress properties: results resemble traditional filler effects and are contrary to previous studies and works discussed in Chapter 2 implementing MQ copolymer nanoparticles into chemically-crosslinked PDMS networks. In situ MQ-loaded, isocyanate-free, segmented PDMS polyureas remain compression moldable, affording transparent, free-standing films. / Master of Science / Polysiloxanes, also referred to as 'silicones' encompass a unique and important class of polymers harboring an inorganic backbone. Polysiloxanes, especially poly(dimethyl siloxane) (PDMS) the flagship polymer of the family, observe widespread utilization throughout industry and academia thanks to a plethora of desirable properties such as their incredible elongation potential, stability to irradiation, and facile chemical tunability. A major complication with the utilization of polysiloxanes for mechanical purposes is their poor resistance to defect propagation and material failure. As a result polysiloxane materials ubiquitously observe reinforcement in some fashion: reinforcement is achieved either through the physical or chemical incorporation of a reinforcing agent, such as fumed silica, or through the implementation of a chemical functionality that facilitates reinforcement via phase separation and strong associative properties, such as hydrogen bonding. This research tackles polysiloxane reinforcement via both of these strategies. Facile chemical modification permits the construction PDMS polymer chains that incorporate hydrogen bonding motifs, which phase separate to afford hydrogen bond-reinforced phases that instill vast improvements to elastic behavior, mechanical and elongation properties, and upper-use temperature. Novel nanocomposite formulation through the incorporation of MQ nanoparticles (which observe widespread usage in cosmetics) facilitate further routes toward improved mechanical and elongation properties. Furthermore, with growing interest in additive manufacturing strategies, which permit the construction of complex geometries via an additive approach (as opposed to conventional manufacturing processes, which require subtractive approaches and are limited in geometric complexity), great interest lies in the capability to additively manufacture polysiloxane-based materials. This work also illustrates the development of an MQ-reinforced polysiloxane system that is amenable to conventional vat photopolymerization additive manufacturing: chemical modification of PDMS polymer chains permits the installation of UV-activatable crosslinking motifs, allowing solid geometries to be constructed from a liquid precursor formulation.

Siloxane

polysiloxane

poly(dimethyl siloxane) (PDMS)

MQ copolymer nanoparticle

vat photopolymerization (VP)

additive manufacturing (AM)

3D printing (3DP)

chain extender

microphase separation