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- International Max Planck Research School Molecular Biology, University of Göttingen, Germany (2)
- Agricultural Center, BASF SE, 67117 Limburgerhof, Germany (1)
- Center for Computational and Theoretical Biology (CCTB), Universität Würzburg (1)
- Center for Nanoscale Microscopy and Molecular Physiology of the Brain (CNMPB), Göttingen, Germany (1)
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- Center for Nanosystems Chemistry (CNC), University of Würzburg (1)
- Center for Nanosystems Chemistry (CNC), Universität Würzburg, Am Hubland, 97074 Würzburg, Germany (1)
- Charles University, Faculty of Mathematics and Physics, Ke Karlovu 5, 121 16 Prague, Czech Republic (1)
- Chemical Biology Laboratory, National Cancer Institue, Frederick (USA) (1)
- Cluster of Excellence "Multiscale Bioimaging: from Molecular Machines to Networks of Excitable Cells, Göttingen (1)
The aim of the thesis was to develop water soluble poly(2-oxazoline) (POx) copolymers with new side group functionalities, which can be used for the formation of hydrogels in biomedical applications and for the development of peptide-polymer conjugates.
First, random copolymers of the monomer MeOx or EtOx with ButEnOx and EtOx with DecEnOx were synthesized and characterized. The vinyl functionality brought into the copolymer by the monomers ButEnOx and DecEnOx would later serve for post-polymerization functionalization. The synthesized copolymers were further functionalized with thiols via post-polymerization functionalization using a newly developed synthesis protocol or with a protected catechol molecule for hydrogel formation. For the formation of peptide-polymer conjugates, a cyclic thioester, namely thiolactone acrylamide and an azlactone precursor, whose synthesis was newly developed, were attached to the side chain of P(EtOx-co-ButEnOx) copolymers.
The application of the functionalized thiol copolymers as hydrogels using thiol-ene chemistry for cross-linking was demonstrated. The swelling behavior and mechanical properties were characterized. The hydrophilicity of the network as well as the cross-linking density strongly influenced the swelling behavior and the mechanical strength of the hydrogels. All hydrogels showed good cell viability results.
The hydrogel networks based on MeOx and EtOx were loaded with two dyes, fluorescein and methylene blue. It was observed that the uptake of the more hydrophilic dye fluorescein depended more on the ability of the hydrogel to swell. In contrast, the uptake of the more hydrophobic dye methylene blue was less dependent on the swelling degree, but much more on the hydrophilicity of the network.
For the potential application as cartilage glue, (biohybrid) hydrogels were synthesized based on the catechol-functionalized copolymers, with and without additional fibrinogen, using sodium periodate as the oxidizing agent. The system allowed for degradation due to the incorporated ester linkages at the cross-linking points. The swelling behavior as well as the mechanical properties were characterized. As expected, hydrogels with higher degrees of cross-linking showed less swelling and higher elastic modulus. The addition of fibrinogen however increased the elasticity of the network, which can be favorable for the intended application as a cartilage glue. Biological evaluation clearly demonstrated the advantage of degradable ester links in the hydrogel network, where chondrocytes were able to bridge the artificial gap in contrast to hydrogels without any ester motifs.
Lastly, different ways to form peptide-polymer conjugates were presented. Peptides were attached with the thiol of the terminal cysteine group to the vinyl side chain of P(EtOx-co-ButEnOx) copolymers by radical thiol-ene chemistry. Another approach was to use a cyclic thioester, thiolactone, or an azlactone functionality to bind a model peptide via native chemical ligation. The two latter named strategies to bind peptides to POx side chains are especially interesting as one and in the case of thiolactone two free thiols are still present at the binding site after the reaction, which can, for example, be used for further thiol-ene cross-linking to form POx hydrogels.
In summary, side functional poly(oxazoline) copolymers show great potential for numerous biomedical applications. The various side chain functionalities can be introduced by an appropriate monomer or by post-polymerization functionalization, as demonstrated. By their multi-functionality, hydrogel characteristics, such as cross-linking degree and mechanical strength, can be fine-tuned and adjusted depending on the application in the human body. In addition, the presented chemoselective and orthogonal reaction strategies can be used in the future to synthesize polymer conjugates, which can, for example, be used in drug delivery or in tissue regeneration.
A unique series of six biaryl natural products displaying four different coupling types (5,10 , 7,10 , 7,80 , and 5,80) were isolated from the roots of the West African liana Ancistrocladus abbreviatus (Ancistrocladaceae). Although at first sight structurally diverse, these secondary metabolites all have in common that they belong to the rare group of naphthylisoquinoline alkaloids with a fully dehydrogenated isoquinoline portion. Among the African Ancistrocladus species, A. abbreviatus is so far only the second one that was found to produce compounds with such a molecular entity. Here, we report on four new representatives, named ancistrobreveines A–D (12–14, and 6). They were identified along with the two known alkaloids 6-O-methylhamateine (4) and entdioncophylleine A (10). The two latter naphthylisoquinolines had so far only been detected in Ancistrocladus species from Southeast Asia. All of these fully dehydrogenated alkaloids have in common being optically active despite the absence of stereogenic centers, due to the presence of the rotationally hindered biaryl axis as the only element of chirality. Except for ent-dioncophylleine A (10), which lacks an oxygen function at C-6, the ancistrobreveines A–D (12–14, and 6) and 6-O-methylhamateine (4) are 6-oxygenated alkaloids, and are, thus, typical ‘Ancistrocladaceae-type’ compounds. Ancistrobreveine C (14), is the first – and so far only – example of a 7,80-linked fully dehydrogenated naphthylisoquinoline discovered in nature that is configurationally stable at the biaryl axis. The stereostructures of the new alkaloids were established by spectroscopic (in particular HRESIMS, 1D and 2D NMR) and chiroptical (electronic circular dichroism) methods. Ancistrobreveine C (14) and 6-O-methylhamateine (4) exhibited strong antiproliferative activities against drug-sensitive acute lymphoblastic CCRF-CEM leukemia cells and their multidrugresistant subline, CEM/ADR5000.
From the leaves of a botanically and phytochemically as yet unexplored Ancistrocladus liana discovered in the rainforests of the Central region of the Democratic Republic of the Congo in the vicinity of the town of Ikela, six new naphthylisoquinoline alkaloids were isolated, viz., two constitutionally unsymmetric dimers, the mbandakamines B\(_3\) (3) and B\(_4\) (4), and four related 5,8′-linked monomeric alkaloids, named ikelacongolines A–D (5a, 5b, 6, and 7). The dimers 3 and 4 are structurally unusual quateraryls comprising two 5,8′-coupled monomers linked via a sterically strongly constrained 6′,1′′-connection between their naphthalene units. These compounds contain seven elements of chirality, four stereogenic centers and three consecutive chiral axes. They were identified along with two known related compounds, the mbandakamines A (1) and B\(_2\) (2), which had so far only been detected in two Ancistrocladus species indigenous to the Northwestern Congo Basin. In addition, five known monomeric alkaloids, previously found in related Central African Ancistrocladus species, were isolated from the here investigated Congolese liana, three of them belonging to the subclass of 5,8′-coupled naphthylisoquinoline alkaloids, whereas two compounds exhibited a less frequently occurring 7,8′-biaryl linkage. The stereostructures of the new alkaloids were established by spectroscopic (in particular HRESIMS, 1D and 2D NMR), chemical (oxidative degradation), and chiroptical (electronic circular dichroism) methods. The mbandakamines B\(_3\) (3) and B\(_4\) (4) displayed pronounced activities in vitro against the malaria parasite Plasmodium falciparum and the pathogen of African sleeping sickness, Trypanosoma brucei rhodesiense.
A series of seven unusual dimeric naphthylisoquinoline alkaloids was isolated from the leaves of the tropical liana Ancistrocladus ealaensis J. Léonard, named cyclombandakamine A (1), 1-epi-cyclombandakamine A (2), and cyclombandakamines A3–7 (3–7). These alkaloids have a chemically thrilling structural array consisting of a twisted dihydrofuran-cyclohexenone-isochromene system. The 1′″-epimer of 4, cyclombandakamine A1 (8), had previously been discovered in an unidentified Ancistrocladus species related to A. ealaensis. Both lianas produce the potential parent precursor, mbandakamine A (9), but only A. ealaensis synthesizes the corresponding cyclized form, along with a broad series of slightly modified analogs. The challenging isolation required, besides multi-dimensional chromatography, the use of a pentafluorophenyl stationary phase. Featuring up to six stereocenters and two types of chiral axes, their structures were elucidated by means of 1D and 2D NMR, HRESIMS, in combination with oxidative chemical degradation experiments as well as chiroptical (electronic circular dichroism spectroscopy) and quantum chemical calculations. Compared to the ‘open-chain’ parent compound 9, these dimers displayed rather moderate antiplasmodial activities.
The initial goal was the conversion of Bifidobacterium adolescentis Sucrose Phosphorylase (BaSP) into a polyphenol glucosidase by structure based enzyme engineering. BaSP was chosen because of its ability to utilize sucrose, an economically viable and sustainable donor substrate, and transfer the glucosyl moiety to various acceptor substrates. The introduction of aromatic residues into the active site was considered a viable way to render it more suitable for aromatic acceptor compounds by reducing its polarity and potentially introducing π-π-interactions with the polyphenols. An investigation of the active site revealed Gln345 as a suitable mutagenesis target. As a proof of concept BaSP Q345F was employed in the glycosylation of (+)-catechin, (-)-epicatechin and resveratrol. The variant was selective for the aromatic acceptor substrates and the glucose disaccharide side reaction was only observed after almost quantitative conversion of the aromatic substrates. A crystal structure of BaSP Q345F in complex with glucose was obtained and it displayed an unexpected shift of an entire domain by 3.3 Å. A crystal structure of BaSP D192N-Q345F, an inactive variant in complex with resveratrol-3-α-D-glucosid, the glucosylation product of resveratrol, synthesized by BaSP Q345F was solved. It proved that the domain shift is in fact responsible for the ability of the variant to glycosylate aromatic compounds. Simultaneously a ligand free crystal structure of BaSP Q345F disproved an induced fit effect as the cause of the domain shift. The missing link, a crystal structure of BaSP Q345F in the F-conformation is obtained. This does not feature the domain shift, but is in outstanding agreement with the wildtype structure. The domain shift is therefore not static but rather a step in a dynamic process. It is further conceivable that the domain shifted conformation of BaSP Q345F resembles the open conformation of the wild type and that an adjustment of a conformational equilibrium as a result of the Q345F point mutation is observed. An investigation into the background reaction, the formation of glucose-glucose disaccharides of BaSP Q345F and three further variants that addressed the same region (L341C, D316C-L341C and D316C-N340C) revealed the formation of nigerose by BaSP Q345F.
RNA aptamers form compact tertiary structures and bind their ligands in specific binding sites. Fluorescence-based strategies reveal information on structure and dynamics of RNA aptamers. Here we report the incorporation of the universal emissive nucleobase analog 4-cyanoindole into the fluorogenic RNA aptamer Chili, and its application as a donor for supramolecular FRET to bound ligands DMHBI+ or DMHBO+. The photophysical properties of the new nucleobase-ligand-FRET pair revealed structural restraints for the overall RNA aptamer organization and identified nucleotide positions suitable for FRET-based readout of ligand binding. This strategy is generally suitable for binding site mapping and may also be applied for responsive aptamer devices.
In this work the catalytic activity of nanodiamond particles with different dopants and surface terminations and of diamond nanomaterials funtionalized with ruthenium-based photocatalysts was investigated, illustrating materials application in photoredox chemistry and the photo(electro)catalytic reduction of CO2. Regarding the application of diamond nanomaterials in photocatalysis, methods to fabricate and characterize several (un)doped nanoparticles with different surface termination were successfully developed. Various photocatalysts, attached to nanodiamond particles via linker systems, were tested in photoredox catalysis and the photo(electro)catalytic reduction of CO2.
In T cells, as in all other cells of the body, sphingolipids form important structural components of membranes. Due to metabolic modifications, sphingolipids additionally play an active part in the signaling of cell surface receptors of T cells like the T cell receptor or the co-stimulatory molecule CD28. Moreover, the sphingolipid composition of their membranes crucially affects the integrity and function of subcellular compartments such as the lysosome. Previously, studying sphingolipid metabolism has been severely hampered by the limited number of analytical methods/model systems available. Besides well-established high resolution mass spectrometry new tools are now available like novel minimally modified sphingolipid subspecies for click chemistry as well as recently generated mouse mutants with deficiencies/overexpression of sphingolipid-modifying enzymes. Making use of these tools we and others discovered that the sphingolipid sphingomyelin is metabolized to ceramide to different degrees in distinct T cell subpopulations of mice and humans. This knowledge has already been translated into novel immunomodulatory approaches in mice and will in the future hopefully also be applicable to humans. In this paper we are, thus, summarizing the most recent findings on the impact of sphingolipid metabolism on T cell activation, differentiation, and effector functions. Moreover, we are discussing the therapeutic concepts arising from these insights and drugs or drug candidates which are already in clinical use or could be developed for clinical use in patients with diseases as distant as major depression and chronic viral infection.
Die photolytische Stickstoffabspaltung aus Azoalkanen vom DBH-Typ verläuft stereoselektiv unter bevorzugter Bildung des invertierten Hausans. Bei cyclopentenannelierten DBH-Derivaten kann die Selektivität in Abhängigkeit von den Brückenkopfsubstituenten auch umgekehrt sein. Bei der Photolyse von Azoalkan DBH-d2 zeigt sich, dass das Verhältnis von Inversions- zu von der Viskosität des Lösungsmittels abhängig ist. Die Viskosität wird sowohl durch Verwendung einer Serie von Alkoholen verschiedener Viskosität als auch durch Variation der Temperatur in n-Butanol geändert. Der Wert für die Photolyse in Acetonitril fügt sich in die Reihe der alkoholischen Solventien ein, womit eine Beteiligung von Wasserstoffbrücken ausgeschlossen ist. Der Viskositätseffekt ist mit einem schrittweisen Mechanismus der Stickstoffabspaltung vereinbar, der über ein unsymmetrisches Singulettdiazenyldiradikal verläuft. Die Abweichung der Viskositätprofile des kinv/kret-Verhältnisses für die Viskositätsänderung durch Lösungsmittel- und Temperaturvariation lässt einen kleinen aber messbaren Unterschied in der Aktivierungsenergie für den Inversions- und Retentionsprozess ableiten. Das kinv/kret-Verhältnis bei der Photolyse von DBH-d2 wird auch in Abhängigkeit vom Druck in superkritischem Ethan und Kohlendioxid untersucht, wofür zunächst eine spezielle Apparatur aufgebaut werden musste. Die Analyse der beobachteten Druckabhängigkeit im Hinblick auf Stoß- (Selbstdiffusionskoeffi-zient) und Reibungseffekte (Viskosität) lässt schließen, dass eine Behinderung des Inversionsprozesses durch Reibung mit Mediummolekülen die experimentellen Beobachtungen am besten erklärt. Dies entspricht den Beobachtungen in flüssiger Phase und bestätigt den Mechanismus. In einer vergleichenden Untersuchung der Photolyse (bei + 25 °C) von Azaolkan Ib und der thermischen (bei +25 °C) syn-zu-anti-Isomerisierung des entsprechenden Hausans IIb wird festgestellt, dass die kinv/kret-Verhältnisse bei der Photolyse des Azoalkans in einer Serie von Alkoholen und die Geschwindigkeitskonstanten kiso der Isomerisierung in der gleichen Reihe von Lösungsmitteln einer sehr ähnlichen Viskositätsabhängigkeit gehorchen. Daraus wird geschlossen, dass die Bewegung bei der Gerüstinversion in beiden Fällen durch Reibung mit Lösungsmittelmolekülen gehemmt und damit die Stereoselektivität bestimmt wird. Die Photolyse von DBH-d2 in Isooctan/Nujol-Gemischen zeigt die gleiche Viskositätsabhängigkeit des kinv/kret-Verhältnisses wie die in alkoholischen Medien. Aus dem Unterschied der absoluten kinv/kret-Werte der beiden Serien und durch die Verwendung weite-rer aprotischer Lösungsmittel wird eine Beeinflussung der Selektivität durch die "bulk" Polarität des Mediums festgestellt. Fazit: Durch die Untersuchung des Einflusses der Viskosität und Polarität des Lösungsmittels auf die Stereoselektivität bei der Photolyse von bicyclischen Azoalkanen und die thermi-sche Isomerisierung der entsprechenden Hausane wird das Auftreten eines Diazenyldiradi-kals als Schlüsselintermediat bestätigt und dynamische Effekte werden ausgeschlossen. Bei der Photolyse der cyclopentenannelierten Azoalkane Ic,d mit n-Propyl- und Acetoxy-methylsubstituenten an den Brückenkopfpositionen (Schema IV) entstehen unter Singulettbedingungen (direkte Photolyse bei höherer Temperatur) unter Retention hauptsächlich die anti-IIc,d Hausane. Unter Triplettbedingungen (direkte Photolyse bei tiefer Temperatur oder sensibilisierte Photolyse) wird das Inversionsprodukt syn-IIc,d bevorzugt. Die favorisierte Inversion beim Triplettweg wird mit der unsymmetrischen Natur der Brückenkopfsubstituenten nPropyl und Acetoxymethyl bei der Rotation um die Brückenkopfposition des planaren Cyclopentan-1,3-diyltriplettdiradikal erklärt. Die rotationsunsymmetrischen Brückenkopfsubstituenten stehen in ihrer Konformation niedrigster Energie (AM1-Rechnungen) auf der gegenüberliegenden Seite des Diylrings als der annelierte Cyclopentenring. Nach ISC führt der Ringschluss aufgrund sterischer Wechselwirkungen zwischen den Brückenkopfsubstituenten und der gem-dimethylsubstituierten Methylenbrücke bevorzugt zum syn-Hausan. Beim Vergleich des Verhältnisses von Inversion zu Retention bei der Photolyse des ungesät-tigten und gesättigten Azoalkans Ie und If (Schema IV) zeigt sich, dass bei beiden Derivaten unter Singulettbedingungen das syn-Hausan in etwa gleichem Ausmaß entsteht. Unter Triplettbedingungen führt die Photolyse zum Retentionsprodukt anti-IIe,f als Hauptdiastereomer, aber mit einem beträchtlichen Unterschied im syn/anti-Hausan-Verhältnis für Ie (38 : 62) und If (6 : 94). Dieser signifikante Unterschied der anti-Stereoselektivität im Triplettweg wird mechanistisch durch weitreichende sterische Wechselwirkungen zwischen dem annelierten Ring und der gem-dimethylsubstituierten Methylenbrücke während des Ringschlusses nach ISC des planaren Cyclopentan-1,3-diyltriplettdiradikals gedeutet. Im Gegensatz dazu ist die Denitrogenierung des intermediären Diazenyldiradikals Ie,f-1DZ (analog zu Ia-1DZ) im SH2-Prozess (Inversion) des Singulettwegs relativ unempfindlich gegenüber solchen sterischen Effekten zwischen den entfernten Substituenten. Fazit: Bei der Photolyse von fünfringannelierten Azoalkanen wirken sich kleinere strukturelle Variationen (rotationsunsymmetrische Brückenkopfsubstituenten oder die Hydrierung der Doppelbindung im annelierten Ring) vor allem im Triplettweg über sterische Wechselwirkungen im planaren Cyclopentan-1,3-diyltriplettdiradikal auf das Verhältnis der entstehenden syn/anti-Hausane aus. Der SH2-Prozess im Singulettweg ist relativ unempfindlich gegenüber solchen sterischen Effekten.
The aim of this work was the selective functionalisation of tribenzotriquinacene (TBTQ) in order to extend the aromatic system and tune the electronic properties. The synthesised molecules could be starting materials for a model system of a defective graphene fragment. The “triple cyclisation pathway” by Hopf et al. was adapted and fluorinated tribenzotriquinacenes were synthesised for the first time.
Phenanthrene groups were also introduced in other model systems and the crystal structures of phenanthrene functionalised TBTQs were compared with the parent molecules.
In addition, the arrangement of TBTQ and centro methyl functionalised TBTQ was investigated on a Ag(111) surface for the first time using scanning transmission microscopy (STM). Different arrangements were observed, depending on the coverage of the surface.
The insights gained about the interaction between TBTQs as well as their synthesis provide a foundation for further work and potential applications as components in organic electronic devices.