TY - THES A1 - Hanio, Simon T1 - The impact of bile on intestinal permeability of drug substances T1 - Der Einfluss der Galle auf die intestinale Permeabilität von Arzneimittelwirkstoffen N2 - Most medicines are taken orally. To enter the systemic circulation, they dissolve in the intestinal fluid, cross the epithelial barrier, and pass through the liver. Intestinal absorption is driven by the unique features of the gastrointestinal tract, including the bile colloids formed in the lumen and the mucus layer covering the intestinal epithelium. Neglecting this multifaceted environment can lead to poor drug development decisions, especially for poorly water-soluble drugs that interact with bile and mucus. However, there is a lack of a rationale nexus of molecular interactions between oral medicines and gastrointestinal components with drug bioavailability. Against this background, this thesis aims to develop biopharmaceutical strategies to optimize the presentation of oral therapeutics to the intestinal epithelial barrier. In Chapter 1, the dynamics of bile colloids upon solubilization of the poorly-water soluble drug Perphenazine was studied. Perphenazine impacted molecular arrangement, structure, binding thermodynamics, and induced a morphological transition from vesicles to worm-like micelles. Despite these dynamics, the bile colloids ensured stable relative amounts of free drug substance. The chapter was published in Langmuir. Chapter 2 examined the impact of pharmaceutical polymeric excipients on bile-mediated drug solubilization. Perphenazine and Imatinib were introduced as model compounds interacting with bile, whereas Metoprolol did not. Some polymers altered the arrangement and geometry of bile colloids, thereby affecting the molecularly soluble amount of those drugs interacting with bile. These insights into the bile-drug-excipient interplay provide a blueprint to optimizing formulations leveraging bile solubilization. The chapter was published in Journal of Controlled Release. Chapter 3 deals with the impact of bile on porcine intestinal mucus. Mucus exposed to bile solution changed transiently, it stiffened, and the overall diffusion rate increased. The bile-induced changes eased the transport of the bile-interacting drug substance Fluphenazine, whereas Metoprolol was unaffected. This dichotomous pattern was linked to bioavailability in rats and generalized based on two previously published data sets. The outcomes point to a bile-mucus interaction relevant to drug delivery. The chapter is submitted. The Appendix provides a guide for biopharmaceutical characterization of drug substances by nuclear magnetic resonance spectroscopy aiming at establishing a predictive algorithm. In summary, this thesis deciphers bile-driven mechanisms shaping intestinal drug absorption. Based on these molecular insights, pharmaceuticals can be developed along a biopharmaceutical optimization, ultimately leading to better oral drugs of tomorrow. N2 - Die meisten Arzneimittel werden oral eingenommen. Um in den Blutkreislauf zu gelangen, liegen sie in der Darmflüssigkeit gelöst vor, überwinden die Epithelbarriere und passieren die Leber. Die intestinale Absorption wird durch die einzigartigen Eigenschaften des Magen-Darm-Trakts, einschließlich der im Lumen gebildeten Gallenkolloide und der Schleimschicht, die das Darmepithel bedeckt, bestimmt. Die Vernachlässigung dieser facettenreichen Umgebung kann zu schlechten Entscheidungen bei der Arzneimittelentwicklung führen, insbesondere bei schlecht wasserlöslich Wirkstoffen, die mit Galle und Schleim interagieren. Es fehlt jedoch eine rationale Verknüpfung der molekularen Wechselwirkungen zwischen oralen Arzneimitteln und gastrointestinalen Komponenten mit der Bioverfügbarkeit von Arzneimitteln. Vor diesem Hintergrund zielt diese Arbeit darauf ab, biopharmazeutische Strategien zur Optimierung der Präsentation von oralen Therapeutika an der intestinalen Epithelbarriere zu entwickeln. In Kapitel 1 wurde die Dynamik von Gallenkolloiden bei der Solubilisierung des schwer wasserlöslichen Wirkstoffes Perphenazin untersucht. Perphenazin beeinflusste die molekulare Anordnung, die Struktur sowie die Bindungsthermodynamik und führte zu einem morphologischen Übergang von Vesikeln hin zu wurmartigen Mizellen. Trotz dieser Dynamik sorgten die Gallenkolloide für stabile relative Mengen an freiem Arzneistoff. Dieses Kapitel wurde in Langmuir veröffentlicht. In Kapitel 2 wurde der Einfluss von pharmazeutischen polymeren Hilfsstoffen auf die Solubilisierung von Wirkstoffen durch Galle untersucht. Perphenazin und Imatinib wurden als Modellverbindungen eingeführt, die mit der Galle interagieren, während Metoprolol dies nicht tat. Einige Polymere veränderten die Anordnung und Geometrie der Gallenkolloide und beeinflussten somit die molekular lösliche Menge von solchen Wirkstoffen, die mit der Galle wechselwirken. Diese Einblicke in das Zusammenspiel von Galle und Arzneistoffen bieten einen Ansatz zur Optimierung von Formulierungen, die die Solubilisierung in der Galle nutzen. Dieses Kapitel wurde in Journal of Controlled Release veröffentlicht. Kapitel 3 befasst sich mit den Auswirkungen von Galle auf den Dünndarmschleim von Schweinen. Schleim, der Gallenlösung ausgesetzt war, veränderte sich vorübergehend, versteifte sich und die Gesamtdiffusionsrate nahm zu. Die durch die Galle hervorgerufenen Veränderungen erleichterten den Transport des mit der Galle interagierenden Wirkstoffs Fluphenazin, während Metoprolol unbeeinflusst blieb. Dieses dichotome Muster konnte mit der Bioverfügbarkeit bei Ratten verknüpft werden und durch zwei zuvor veröffentlichte Datensätze mit insgesamt 50 Verbindungen verallgemeinert werden. Die Ergebnisse deuten auf eine Wechselwirkung zwischen Galle und Schleim hin, die für die Verabreichung von Medikamenten relevant ist. Dieses Kapitel ist eingereicht. Der Anhang bietet einen Leitfaden für die biopharmazeutische Charakterisierung von Arzneimittelsubstanzen durch kernmagnetische Resonanzspektroskopie mit dem Ziel des Aufstellens von prädiktiven Algorithmen. Zusammenfassend entschlüsselt diese Arbeit die von der Galle gesteuerten Mechanismen, die die Aufnahme von Arzneimitteln im Darm beeinflussen. Auf der Grundlage dieser molekularen Erkenntnisse können Arzneimittel entlang einer biopharmazeutischen Optimierung entwickelt werden, was letztendlich zu besseren oralen Arzneimitteln führt. KW - Solubilisation KW - Galle KW - Bioverfügbarkeit KW - Pharmazeutischer Hilfsstoff KW - drug delivery KW - absorption KW - intestinal permeability KW - poor water-soluble drugs KW - intestinal mucus KW - pig KW - drug formulation KW - molecular biopharmaceutics KW - mucin KW - Schleim KW - Bile KW - Mucus Y1 - 2024 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-348906 ER - TY - JOUR A1 - Weissenseel, Sebastian A1 - Gottscholl, Andreas A1 - Bönnighausen, Rebecca A1 - Dyakonov, Vladimir A1 - Sperlich, Andreas T1 - Long-lived spin-polarized intermolecular exciplex states in thermally activated delayed fluorescence-based organic light-emitting diodes JF - Science Advances N2 - Spin-spin interactions in organic light-emitting diodes (OLEDs) based on thermally activated delayed fluorescence (TADF) are pivotal because radiative recombination is largely determined by triplet-to-singlet conversion, also called reverse intersystem crossing (RISC). To explore the underlying process, we apply a spin-resonance spectral hole-burning technique to probe electroluminescence. We find that the triplet exciplex states in OLEDs are highly spin-polarized and show that these states can be decoupled from the heterogeneous nuclear environment as a source of spin dephasing and can even be coherently manipulated on a spin-spin relaxation time scale T-2* of 30 ns. Crucially, we obtain the characteristic triplet exciplex spin-lattice relaxation time T-1 in the range of 50 mu s, which far exceeds the RISC time. We conclude that slow spin relaxation rather than RISC is an efficiency-limiting step for intermolecular donor:acceptor systems. Finding TADF emitters with faster spin relaxation will benefit this type of TADF OLEDs. KW - detected magnetic-resonance KW - population oscillations KW - polaron delocalization KW - charge separation KW - hole KW - phosphorescence KW - singlet KW - absorption KW - tryptophan KW - emission Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-265508 VL - 7 IS - 47 ER - TY - JOUR A1 - Shukla, A. A1 - Mannheim, K. T1 - Gamma-ray flares from relativistic magnetic reconnection in the jet of the quasar 3C 279 JF - Nature Communications N2 - Spinning black holes in the centres of galaxies can release powerful magnetised jets. When the jets are observed at angles of less than a few degrees to the line-of-sight, they are called blazars, showing variable non-thermal emission across the electromagnetic spectrum from radio waves to gamma rays. It is commonly believed that shock waves are responsible for this dissipation of jet energy. Here we show that gamma-ray observations of the blazar 3C 279 with the space-borne telescope Fermi-LAT reveal a characteristic peak-in-peak variability pattern on time scales of minutes expected if the particle acceleration is instead due to relativistic magnetic reconnection. The absence of gamma-ray pair attenuation shows that particle acceleration takes place at a distance of ten thousand gravitational radii from the black hole where the fluid dynamical kink instability drives plasma turbulence. KW - kink instability KW - energy KW - radiation KW - blazars KW - variability KW - absorption KW - telescope KW - shocks Y1 - 2020 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-231328 VL - 11 ER - TY - JOUR A1 - Lohse, Christian A1 - Bock, Andreas A1 - Maiellaro, Isabella A1 - Hannawacker, Annette A1 - Schad, Lothar R. A1 - Lohse, Martin J. A1 - Bauer, Wolfgang R. T1 - Experimental and mathematical analysis of cAMP nanodomains JF - PLoS ONE N2 - In their role as second messengers, cyclic nucleotides such as cAMP have a variety of intracellular effects. These complex tasks demand a highly organized orchestration of spatially and temporally confined cAMP action which should be best achieved by compartmentalization of the latter. A great body of evidence suggests that cAMP compartments may be established and maintained by cAMP degrading enzymes, e.g. phosphodiesterases (PDEs). However, the molecular and biophysical details of how PDEs can orchestrate cAMP gradients are entirely unclear. In this paper, using fusion proteins of cAMP FRET-sensors and PDEs in living cells, we provide direct experimental evidence that the cAMP concentration in the vicinity of an individual PDE molecule is below the detection limit of our FRET sensors (<100nM). This cAMP gradient persists in crude cytosol preparations. We developed mathematical models based on diffusion-reaction equations which describe the creation of nanocompartments around a single PDE molecule and more complex spatial PDE arrangements. The analytically solvable equations derived here explicitly determine how the capability of a single PDE, or PDE complexes, to create a nanocompartment depend on the cAMP degradation rate, the diffusive mobility of cAMP, and geometrical and topological parameters. We apply these generic models to our experimental data and determine the diffusive mobility and degradation rate of cAMP. The results obtained for these parameters differ by far from data in literature for free soluble cAMP interacting with PDE. Hence, restricted cAMP diffusion in the vincinity of PDE is necessary to create cAMP nanocompartments in cells. KW - fluorescence resonance energy transfer KW - yellow fluorescent protein KW - radii KW - adenylyl cyclase signaling cascade KW - cell fusion KW - cytosol KW - isoproterenol KW - absorption KW - cyclic nucleotides such as cyclic adenosine monophosphate Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-170972 VL - 12 IS - 4 ER - TY - JOUR A1 - Sauer, C A1 - Wießner, M A1 - Schöll, A A1 - Reinert, F T1 - Observation of a molecule-metal interface charge transfer related feature by resonant photoelectron spectroscopy JF - New Journal of Physics N2 - We report the discovery of a charge transfer (CT) related low binding energy feature at a molecule-metal interface by the application of resonant photoelectron spectroscopy (RPES). This interface feature is neither present for molecular bulk samples nor for the clean substrate. A detailed analysis of the spectroscopic signature of the low binding energy feature shows characteristics of electronic interaction not found in other electron spectroscopic techniques. Within a cluster model description this feature is assigned to a particular eigenstate of the photoionized system that is invisible in direct photoelectron spectroscopy but revealed in RPES through a relative resonant enhancement. Interpretations based on considering only the predominant character of the eigenstates explain the low binding energy feature by an occupied lowest unoccupied molecular orbital, which is either realized through CT in the ground or in the intermediate state. This reveals that molecule-metal CT is responsible for this feature. Consequently, our study demonstrates the sensitivity of RPES to electronic interactions and constitutes a new way to investigate CT at molecule-metal interfaces. KW - transfer dynamics KW - photoemission KW - states KW - interface KW - charge transfer KW - organic thin films KW - resonant photoelectron spectroscopy KW - energy KW - model calculation KW - NEXAFS spectroscopy KW - ce compounds KW - absorption Y1 - 2015 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-148672 VL - 17 IS - 043016 ER - TY - JOUR A1 - Sung, Jooyoung A1 - Kim, Pyosang A1 - Fimmel, Benjamin A1 - Würthner, Frank A1 - Kim, Dongho T1 - Direct observation of ultrafast coherent exciton dynamics in helical π-stacks of self-assembled perylene bisimides JF - Nature Communications N2 - Ever since the discovery of dye self-assemblies in nature, there have been tremendous efforts to exploit biomimetic supramolecular assemblies for tailored artificial photon processing materials. This feature necessarily has resulted in an increasing demand for understanding exciton dynamics in the dye self-assemblies. In a sharp contrast with pi-type aggregates, however, the detailed observation of exciton dynamics in H-type aggregates has remained challenging. In this study, as we succeed in measuring transient fluorescence from Frenkel state of π-stacked perylene tetracarboxylic acid bisimide dimer and oligomer aggregates, we present an experimental demonstration on Frenkel exciton dynamics of archetypal columnar π-π stacks of dyes. The analysis of the vibronic peak ratio of the transient fluorescence spectra reveals that unlike the simple π-stacked dimer, the photoexcitation energy in the columnar π-stacked oligomer aggregates is initially delocalized over at least three molecular units and moves coherently along the chain in tens of femtoseconds, preceding excimer formation process. KW - systems KW - molecules KW - J-aggregate behavior KW - absorption KW - spectroscopy KW - photoluminescence KW - diffusion KW - fluorescence KW - excimer formation KW - organic semiconductors Y1 - 2015 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-148157 VL - 6 IS - 8646 ER - TY - THES A1 - Gräfe, Eva Ulrike T1 - Relative systemische Verfügbarkeit und Pharmakokinetik von Quercetin und Quercetinglykosiden (Quercetin-4'-0-glucosid und Quercetin-3-0-rutinosid) im Menschen T1 - Relative bioavailability and pharmacokinetics of the flavonol quercetin and quercetin glycosides (quercetin-4'-0-glucoside and quercetin-3-0-rutinoside) in humans N2 - Aufgrund seiner potentiell gesundheitsfoerdernden Wirkung wurde das Falvonol Quercetin in den letzten Jahren intensiv untersucht. Daten zur Bioverfuegbarkeit nach oraler Applikation sind jedoch selten und widerspruechlich. Fruehere Untersuchungen deuteten darauf hin, dass die Disposition von Quercetin von der Zuckerkomponente des Glykosids oder der Pflanzenmatrix abhaengen koennte. Um den Einfluss der Zuckerkomponente oder der Matrix auf die Resorption von Quercetin festzustellen, wurden zwei isolierte Quercetinglykoside sowie zwei Pflanzenextrakte in einer vierarmigen, randomisierten cross-over Studie an 12 gesunden Probanden getestet. Jeder Proband erhielt eine Zwiebelzubereitung oder Quercetin-4'-O-glucosid, jeweils entsprechend 100 mg Quercetinaglykon, sowie Quercetin-3-O-rutinosid oder Buchweizenkrauttee entsprechend 200 mg Quercetinaglykon. Die Proben wurden mittels HPLC und Coulometrischer Arraydetektion analysiert. Im Plasma wurden ausschliesslich Quercetinglucuronide detektiert. Freies Quercetin und die Glykoside waren nicht nachweisbar. Die Bioverfuegbarkeit und Pharmakokinetik nach Applikation von Zwiebeln und Quercetin-4'-glucosid zeigte keine signifikanten Unterschiede. Maximale Plasmakonzentrationen von 2.3±1.5 µg·mL-1 and 2.1±1.6 µg·mL-1 (MW±SD) wurden nach 0.7±0.2 h und 0.7±0.3 h erreicht. Nach Einnahme von Buchweizenkraut und Rutin wurden maximale Plasmakonzentrationen (trotz der doppelten Dosis) von nur 0.6±0.7 µg·mL-1 und 0.3±0.3 µg·mL-1 nach 4.3±1.8 h bzw. 7.0±2.9 h erreicht. Die terminale Halbwertszeit lag bei ca. 11 h fuer alle vier Pruefpraeparate. Die Disposition von Quercetin ist daher primaer von der Zuckerkomponente abhaengig. Zu einem geringern Anteil beeinflusst die Pflanzenmatrix im Falle von Buchweizenkrauttee sowohl Geschwindigkeit als auch Ausmass der Resorption. Der Resorptionsort scheint fuer Quercetin-4‘-O-glucoside und Quercetin-3-O-rutinoside unterschiedlich zu sein. Die bedeutung spezifischer carrier fuer die Resorption von Quercetinglykosiden sowie von intestinalen ß-Glucosidasen muss in weiteren Untersuchungen geklaert werden. N2 - Due to its potentially beneficial impact on human health the polyphenol quercetin has come into the focus of medicinal interest. However, data on the bioavailability of quercetin after oral intake are scarce and contradictory. Previous investigations indicate that the disposition of quercetin may depend on the sugar moiety of the glycoside or the plant matrix. In order to determine the influence of the sugar moiety or matrix on the absorption of quercetin, two isolated quercetin glycosides and two plant extracts were administered to 12 healthy volunteers in a four-way cross-over study. Each subject received an onion supplement or quercetin-4‘-O-glucoside both equivalent to 100 mg quercetin, as well as quercetin-3-O-rutinoside and buckwheat tea both equivalent to 200 mg quercetin. Samples were analyzed by HPLC with a 12-channel coulometric array detector. In human plasma only quercetin glucuronides, but no free quercetin, could be detected. There was no significant difference in the bioavailability and pharmacokinetic parameters between the onion supplement and quercetin-4‘-O-glucoside. Peak plasma concentrations were 2.3±1.5 µg·mL-1 and 2.1±1.6 µg·mL-1 (mean±SD) and were reached after 0.7±0.2 h and 0.7±0.3 h, respectively. After administration of buckwheat tea and rutin, however, peak plasma levels were (despite the higher dose) only 0.6±0.7 µg·mL-1 and 0.3±0.3 µg·mL-1, respectively. Peak concentrations were reached 4.3±1.8 h after administration of buckwheat tea and 7.0±2.9 h after ingestion of rutin. The terminal elimination half life was about 11 h for all treatments. Thus, the disposition of quercetin in humans is primarily depending on the sugar moiety. To a minor extent, the plant matrix influences both rate and extent of absorption in the case of buckwheat tea administration compared to the isolated compound. The site of absorption seems to be different for quercetin-4‘-O-glucoside and quercetin-3-O-rutinoside. The significance of specific carriers on the absorption of quercetin glycosides as well as specific intestinal ß-glucosidases needs to be further evaluated. KW - Mensch KW - Stoffwechsel KW - Quercetin KW - Pharmakokinetik KW - Flavonoide KW - Quercetin KW - Zwiebel KW - Buchweizenkraut KW - Bioverfügbarkeit KW - Pharmakokinetik KW - Metabolismus KW - Resorption KW - flavonoids KW - quercetin KW - bioavailibility KW - pharmacokinetics KW - absorption KW - metabolism KW - onion KW - buckwheat Y1 - 2001 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-1333 ER -