@article{WernerChenRoweetal.2018, author = {Werner, Rudolf A. and Chen, Xinyu and Rowe, Steven P. and Lapa, Constantin and Javadi, Mehrbod S. and Higuchi, Takahiro}, title = {Moving into the Next Era of PET Myocardial Perfusion Imaging - Introduction of Novel \(^{18}\)F-labeled Tracers}, series = {The International Journal of Cardiovascular Imaging}, journal = {The International Journal of Cardiovascular Imaging}, issn = {1569-5794}, doi = {10.1007/s10554-018-1469-z}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169134}, year = {2018}, abstract = {The heart failure (HF) epidemic continues to rise with coronary artery disease (CAD) as one of its main causes. Novel concepts for risk stratification to guide the referring cardiologist towards revascularization procedures are of significant value. Myocardial perfusion imaging (MPI) using single-photon emission computed tomography (SPECT) agents has demonstrated high accuracy for the detection of clinically relevant stenoses. With positron emission tomography (PET) becoming more widely available, mainly due to its diagnostic performance in oncology, perfusion imaging with that modality is more practical than in the past and overcomes existing limitations of SPECT MPI. Advantages of PET include more reliable quantification of absolute myocardial blood flow, the routine use of computed tomography for attenuation correction, a higher spatiotemporal resolution and a higher count sensitivity. Current PET radiotracers such as rubidium-82 (half-life, 76 sec), oxygen-15 water (2 min) or nitrogen-13 ammonia (10 min) are labeled with radionuclides with very short half-lives, necessitating that stress imaging is performed under pharmacological vasodilator stress instead of exercise testing. However, with the introduction of novel 18F-labeled MPI PET radiotracers (half-life, 110 min), the intrinsic advantages of PET can be combined with exercise testing. Additional advantages of those radiotracers include, but are not limited to: potentially improved cost-effectiveness due to the use of pre-existing delivery systems and superior imaging qualities, mainly due to the shortest positron range among available PET MPI probes. In the present review, widely used PET MPI radiotracers will be reviewed and potential novel 18F-labeled perfusion radiotracers will be discussed.}, subject = {Positronenemissionstomografie}, language = {en} } @article{Werner2018, author = {Werner, Rudolf A.}, title = {Editorial: Cardiac Innervation Imaging as a Risk Stratification Tool for Potential Device Therapy Candidates}, series = {Journal of Nuclear Cardiology}, journal = {Journal of Nuclear Cardiology}, issn = {1071-3581}, doi = {10.1007/s12350-018-01475-0}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-168465}, year = {2018}, abstract = {As a scintigraphic approach evaluating cardiac nerve integrity, \(^{123}\)I-metaiodobenzylguanidine (123I-mIBG) has been recently Food and Drug Administration approved. A great deal of progress has been made by the prospective ADMIRE-HF trial, which primarily demonstrated the association of denervated myocardium assessed by \(^{123}\)I-mIBG and cardiac events. However, apart from risk stratification, myocardial nerve function evaluated by molecular imaging should also be expanded to other clinical contexts, in particular to guide the referring cardiologist in selecting appropriate candidates for specific therapeutic interventions. In the present issue of the Journal of Nuclear Cardiology, the use of 123I-mIBG for identifying cardiomyopathy patients, which would most likely not benefit from ICD due low risk of arrhythmias, is described. If we aim to deliver on the promise of cardiac innervation imaging as a powerful tool for risk stratification in a manner similar to nuclear oncology, studies such as the one reviewed here may imply an important step to lay the proper groundwork for a more widespread adoption in clinical practice.}, subject = {SPECT}, language = {en} } @phdthesis{Rehman2018, author = {Rehman, Saba}, title = {Identification of accessible and closed substrate binding sites in the outward open cleft of rat Organic Cation Transporter 1 (rOCT1)}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169992}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {The present study was conducted on the rOCT1, a member of SLC22 family. Structurally, it consists of 12 membrane spanning α-helices with both N- and C-termini intracellular. Studies done so far, through tracer uptake and inhibition, reconstitution of rOCT1 in nanodiscs and proteoliposomes and voltage-clamp fluorometry, have identified the main amino acids in the cleft of rOCT1 that interact in a critical manner with the substrates/inhibitors either directly or indirectly. Homology modeling studies have also supported these observations. In the present study we aimed at measuring the binding of substrates MPP+ and TEA+ to rOCT1 at 0oC in order to establish the amino acids in the cleft region that interact with the substrate when the transporter is frozen in the outward-open conformation. Previously identified crucial amino acids (Asp475, Phe160, Leu447, Arg440, Trp218 and Tyr222) were selected for the study. rOCT1 wild-type and its mutants were stably expressed in HEK293 cells and these cells were used for the binding measurements with the radioactive substrate (MPP+ or TEA+) at 0°C in Mg-Ca-PBS buffer as described in "Materials and Methods" section in detail. rOCT1 wild-type revealed for MPP+-binding a KD which was not significantly different from the corresponding Km value. Also, after addition of 10 nM non-radioactive MPP+, an initial increase of about 20\% in bound MPP+ was observed. The results indicate that the Km for transport is dependent on the binding of MPP+ to the outward-open conformation and hints at the possibility of allosteric interaction between the binding sites. Mutations at position Trp218, Phe160 and Asp475 resulted in a change in the KD value. Trp218 mutations also showed an allosteric increase similar to the rOCT1 wild-type. This study suggests that these amino acids are located at a critical position in the outward-open conformation for MPP+ transport. TEA+-binding could not be observed in rOCT1 wild-type, indicating that the binding site is perhaps inaccessible for TEA+ in frozen outward-open state. The mutants D475E, F160A, L447F, R440K and Y222F showed a very low affinity binding with a very high KD value as compared to the corresponding Km values indicating that the transporter might have different affinities for extra-cellular binding alone and for the complete transport process especially if temperature is the limiting factor. Substrate inhibition studies done using both MPP+ and TEA+ have confirmed the existence of overlapping binding sites for these two ligands. This study has confirmed the direct interaction of Trp218, Phe160, Asp475 with MPP+ and Phe160, Asp475, Leu447, Arg440 and Tyr222 with TEA+ in the outward-open conformation.}, subject = {Kation}, language = {en} } @phdthesis{Chowdhury2018, author = {Chowdhury, Suvagata Roy}, title = {The Role of MicroRNAs in \(Chlamydia\) Infection}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-155866}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {The obligate intracellular pathogen Chlamydia trachomatis is the causative agent of trachoma related blindness and the sexually transmitted pelvic inflammatory disease. Being an obligate intracellular pathogen, C. trachomatis has an intricate dependency on the survival of the host cell. This relationship is indispensible owing to the fact that the pathogen spends a considerable fraction of its biphasic lifecycle within a cytoplasmic vacuole inside the host cell, the so-called chlamydial inclusion. The cellular apoptotic-signalling network is governed by several finely tuned regulatory cascades composed of pro- and anti-apoptotic proteins that respond to changes in the cellular homeostasis. In order to facilitate its intracellular survival, Chlamydia has been known to inhibit the premature apoptosis of the host cell via the stabilization of several host anti-apoptotic proteins such as cIAP2 and Mcl-1. While the pro- and anti-apoptotic proteins are the major regulators of the host apoptotic signalling network, a class of the small non-coding RNAs called microRNAs (miRNAs) has increasingly gained focus as a new level of regulatory control over apoptosis. This work investigates the changes in the host miRNA expression profile post Chlamydia infection using a high throughput miRNA deep sequencing approach. Several miRNAs previously associated with the modulation for apoptotic signalling were differentially expressed upon Chlamydia infection in human endothelial cells. Of the differentially regulated miRNAs, miR-30c-5p was of particular interest since it had been previously shown to target the tumor suppressor protein p53. Our lab and others have previously demonstrated that Chlamydia can downregulate the levels of p53 by promoting its proteasomal degradation. This work demonstrates that Chlamydia infection promotes p53 downregulation by increasing the abundance of miR-30c-5p and a successful infection cycle is hindered by a loss of miR-30c-5p. Over the last decade, dedicated research aimed towards a better understanding of apoptotic stimuli has greatly improved our grasp on the subject. While extrinsic stress, deprivation of survival signals and DNA damage are regarded as major proponents of apoptotic induction, a significant responsibility lies with the mitochondrial network of the cell. Mitochondrial function and dynamics are crucial to cell fate determination and dysregulation of either is decisive for cell survival and pathogenesis of several diseases. The ability of the mitochondrial network to perform its essential tasks that include ATP synthesis, anti-oxidant defense, and calcium homeostasis amongst numerous other processes critical to cellular equilibrium is tied closely to the fission and fusion of individual mitochondrial fragments. It is, thus, 8 unsurprising that mitochondrial dynamics is closely linked to apoptosis. In fact, many of the proteins involved regulation of mitochondrial dynamics are also involved in apoptotic signalling. The mitochondrial fission regulator, Drp1 has previously been shown to be transcriptionally regulated by p53 and is negatively affected by a miR- 30c mediated inhibition of p53. Our investigation reveals a significant alteration in the mitochondrial dynamics of Chlamydia infected cells affected by the loss of Drp1. We show that loss of Drp1 upon chlamydial infection is mediated by the miR-30c-5p induced depletion of p53 and results in a hyper-fused architecture of the mitochondrial network. While it is widely accepted that Chlamydia depends on the host cell metabolism for its intracellular growth and development, the role of mitochondria in an infected cell, particularly with respect to its dynamic nature, has not been thoroughly investigated. This work attempts to illustrate the dependence of Chlamydia on miR-30c-5p induced changes in the mitochondrial architecture and highlight the importance of these modulations for chlamydial growth and development.}, subject = {Chlamydienkrankheit}, language = {en} } @phdthesis{Sieck2018, author = {Sieck, Carolin}, title = {Synthesis and Photophysical Properties of Luminescent Rhodacyclopentadienes and Rhodium 2,2'-Biphenyl Complexes}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-154844}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {The photochemistry and photophysics of transition metal complexes are of great interest, since such materials can be exploited for a wide range of applications such as in photocatalysis, sensing and imaging, multiphoton-absorption materials and the fabrication of OLEDs. A full understanding of the excited state behavior of transition metal compounds is therefore important for the design of new materials for the applications mentioned above. In principle, the luminescence properties of this class of compounds can be tuned by changing the metal or subtle changes in the ligand environment. Furthermore, transition-metal complexes continue to play a major role in modern synthetic chemistry. In particular, they can realize selective transformations that would either be difficult or impossible by conventional organic chemistry. For example, they enable the efficient and selective formation of carbon-carbon bonds. One famous example of these types of transformations are metal-catalyzed cyclization reactions. Herein, metallacyclopentadiene complexes are considered as key intermediates in a number of metal-mediated or -catalyzed cyclization reactions, i.e. the [2+2+2] cyclotrimerization of alkynes. Recent research has focused on the synthesis and characterization of these metallacyclic intermediates such as MC4 ring systems. Metallacyclopentadienes are structurally related to main group EC4 systems such as boroles, siloles, thiophenes and phospholes. Overall, this group of compounds (EC4 analogues) is well known and has attracted significant attention due to their electron-transport and optical properties. Unlike transition metal analogues, however, these EC4 systems show no phosphorescence, which is due to inefficient SOC compared to 2nd and 3rd row transition metals, which promoted us to explore the phosphorescence potential of metallacyclopentadienes. In 2001, Marder et al. developed a one-pot high-yield synthesis of luminescent 2,5 bis(arylethynyl)rhodacyclopentadienes by reductive coupling of 1,4-diarylbuta-1,3-diynes at a suitable rhodium(I) precursor. Over the past years, a variety of ligands (e.g. TMSA, S,S' diethyldithiocarbamate, etc.) and 1,4-bis(p-R-phenyl)-1,3-butadiynes or linked , bis(p-R-arylethynyl)alkanes (R = electron withdrawing or donating groups) were investigated and always provided a selective formation of 2,5 bis(arylethynyl)rhodacyclopentadienes, which were reported to be fluorescent despite presence of the heavy atom. To examine the influence of the ligand sphere around the rhodium center on the intersystem-crossing (ISC) processes in the above-mentioned fluorescent rhodacyclopentadienes and to increase the metal character in the frontier orbitals by destabilizing the Rh filled d-orbitals, a -electron donating group was introduced, namely acetylacetonato (acac). Interestingly, in 2010 Tay reacted [Rh(κ2-O,O-acac)(PMe3)2] with ,-bis(p-R-arylbutadiynyl)alkanes and observed not only the fluorescent 2,5 bis(arylethynyl)rhodacyclopentadienes, but also rhodium 2,2'-bph complexes as products, which were reported to be phosphorescent in preliminary photophysical studies. In this work, the reaction behavior of [Rh(κ2-O,O-acac)(L)2] (L = PMe3, P(p-tolyl)3) with different ,-bis(p-R-arylbutadiynyl)alkanes was established. Furthermore, the separation of the two isomers 2,5-bis(arylethynyl)rhodacyclopentadienes (A) and rhodium 2,2'-bph complexes (B), and the photophysical properties of those were explored in order to clarify their fundamentally different excited state behaviors. Reactions of [Rh(κ2-O,O-acac)(P(p-tolyl3)2)] with ,-bis(arylbutadiynyl)alkanes gives exclusively weakly fluorescent 2,5-bis(arylethynyl)rhodacyclopentadienes. Changing the phosphine ligands to PMe3, reactions of [Rh(κ2-O,O-acac)(PMe3)2] and , bis(arylbutadiynyl)alkanes afford two isomeric types of MC4 metallacycles with very different photophysical properties, as mentioned before. As a result of a normal [2+2] reductive coupling at rhodium, 2,5 bis(arylethynyl)rhodacyclopentadienes (A) are formed, which display intense fluorescence. Rhodium 2,2'-bph complexes (B), which show phosphorescence, have been isolated as a second isomer originating from an unusual [4+2] cycloaddition reaction and a subsequent -H-shift. Control of the isomer distribution, of 2,5-bis(arylethynyl)rhodacyclopentadienes (A) and rhodium biphenyl complexes (B), is achieved by modification of the linked , bis(arylbutadiynyl)alkane. Changing the linker length from four CH2 to three CH2 groups, dramatically favors the formation of the rhodium biphenyl isomer B, providing a fundamentally new route to access photoactive metal biphenyl compounds in good yields. This is very exciting as the photophysical properties of only a limited number of bph complexes of Ir, Pd and Pt had been explored. The lack of photophysical reports in the literature is presumably due to the limited synthetic access to various substituted 2,2'-bph transition metal complexes. On the other hand, as the reaction of [Rh(κ2-O,O-acac)(P(p-tolyl)3)2] with , bis(arylbutadiynyl)alkanes provides a selective reaction to give weakly fluorescent 2,5 bis(arylethynyl)rhodacyclopentadiene complexes with P(p-tolyl)3 as phosphine ligands, a different synthetic access to 2,5-bis(arylethynyl)rhodacyclopentadiene complexes with PMe3 as phosphine ligands was developed, preventing the time-consuming separation of the isomers. The weak rhodium-phosphorus bonds of 2,5-bis(arylethynyl)rhodacyclopentadiene complexes bearing P(p tolyl)3 as phosphine ligands, relative to those of related PMe3 complexes, allowed for facile ligand exchange reactions. In the presence of an excess of PMe3, a stepwise reaction was observed, giving first the mono-substituted, mixed-phosphine rhodacyclopentadiene intermediates and, subsequently, full conversion to the highly fluorescent 2,5 bis(arylethynyl)-rhodacyclopentadienes bearing only PMe3 ligands (by increasing the reaction temperature). With spectroscopically pure 2,5-bis(arylethynyl)rhodacyclopentadiene complexes A (bearing PMe3 as phosphine ligands) and rhodium 2,2-bph complexes B in hand, photophysical studies were conducted. The 2,5-bis(arylethynyl)rhodacyclopentadienes (A) are highly fluorescent with high quantum yields up to 54\% and very short lifetimes (τ = 0.2 - 2.5 ns) in solution at room temperature. Even at 77 K in glass matrices, no additional phosphorescence is observed which is in line with previous observations made by Steffen et al., who showed that SOC mediated by the heavy metal atom in 2,5-bis(arylethynyl)rhodacyclopentadienes and 2,5 bis(arylethynyl)iridacyclopentadienes is negligible. The origin of this fluorescence lies in the pure intra-ligand (IL) nature of the excited states S1 and T1. The HOMO and the LUMO are nearly pure  and * ligand orbitals, respectively, and the HOMO is energetically well separated from the filled rhodium d orbitals. The absence of phosphorescence in transition metal complexes due to mainly IL character of the excited states is not unusual, even for heavier homologues than rhodium with greater SOC, resulting in residual S1 emission (fluorescence) despite ISC S1→Tn being sufficiently fast for population of T1 states. However, there are very few complexes that exhibit fluorescence with the efficiency displayed by our rhodacyclopentadienes, which involves exceptionally slow S1→Tn ISC on the timescale of nanoseconds rather than a few picoseconds or faster. In stark contrast, the 2,2'-bph rhodium complexes B are exclusively phosphorescent, as expected for 2nd-row transition metal complexes, and show long-lived (hundreds of s) phosphorescence (Ф = 0.01 - 0.33) at room temperature in solution. As no fluorescence is detected even at low temperature, it can be assumed that S1→Tn ISC must be faster than both fluorescence and non-radiative decay from the S1 state. This contrasts with the behavior of the isomeric 2,5-bis(arylethynyl)rhodacyclopentadienes for which unusually slow ISC occurs on a timescale that is competitive with fluorescence (vide supra). The very small values for the radiative rate constants, however, indicate that the nature of the T1 state is purely 3IL with weak SOC mediated by the Rh atom. The phosphorescence efficiency of these complexes in solution at room temperature is even more impressive, as non-radiative coupling of the excited state with the ground state typically inhibits phosphorescence. Instead, the rigidity of the organic -system allows the ligand-based excited triplet state to exist in solution for up to 646 s and to emit with high quantum yields for biphenyl complexes. The exceptionally long lifetimes and small radiative rate constants of the rhodium biphenyl complexes are presumably a result of the large conjugated -system of the organic ligand. According to TD DFT studies, the T1 state involves charge-transfer from the biphenyl ligand into the arylethynyl moiety away from the rhodium atom. This reduces the SOC of the metal center that would be necessary for fast phosphorescence. These results show that the π-chromophoric ligand can gain control over the photophysical excited state behavior to such an extent that even heavy transition metal atoms like rhodium participate in increasing the fluorescence such as main-group analogues do. Furthermore, in the 2,2'-bph rhodium complexes, the rigidity of the organic -system allows the ligand-based excited triplet state to exist in solution for up to hundreds of s and to emit with exceptional quantum yields. Therefore, investigations of the influence of the ligand sphere around the rhodium center have been made to modify the photophysical properties and furthermore to explore the reaction behavior of these rhodium complexes. Bearing in mind that the P(p-tolyl)3 ligands can easily be replaced by the stronger -donating PMe3 ligands, ligand exchange reactions with N heterocyclic carbenes (NHCs) as even stronger -donors was investigated. Addition of two equivalents of NHCs at room temperature led to the release of one equivalent of P(p-tolyl3) and formation of the mono-substituted NHC rhodium complex. The reaction of isolated mono-NHC complex with another equivalent of NHC at room temperature did not result in the exchange of the second phosphine ligand. Moderate heating of the reaction to 60 °C, however, resulted in the formation of tetra-substituted NHC rhodium complex [Rh(nPr2Im)4]+[acac]-. To circumvent the loss of the other ligands in the experiments described above, a different approach was investigated to access rhodacyclopentadienes with NHC instead of phosphine ligands. Reaction of the bis-NHC complex [Rh(κ2-O,O-acac)(nPr2Im)2] with , bis(arylbutadiynyl)alkanes at room temperature resulted 2,5-bis(arylethynyl)-rhodacyclopentadienes with the NHC ligands being cis or trans to each other as indicated by NMR spectroscopic measurements and single-crystal X-ray diffraction analysis. Isolation of clean material and a fundamental photophysical study could not be finished for reasons of time within the scope of this work. Furthermore, shortening of the well conjugated -system of the chromophoric ligand (changing from tetraynes to diynes) was another strategy to examine the reaction behavior of theses ligands with rhodium(I) complexes and to modify the excited state behavior of the formed rhodacyclopentadienes. The reaction of [Rh(κ2-O,O-acac)(PMe3)2] with 1,7 diaryl 1,6-heptadiynes (diynes) leads to the selective formation of 2,5 bis(aryl)rhodacyclopentadienes. These compounds, however, are very weakly fluorescent with quantum yields ФPL < 1, and very short emission lifetimes in toluene at room temperature. Presumably, vibrational modes of the bis(phenyl)butadiene backbone leads to a higher rate constant for non-radiative decay and is thus responsible for the low quantum yields compared to their corresponding PMe3 complexes with the bis(phenylethynyl)butadiene backbone at room temperature. No additional phosphorescence, even at 77 K in the glass matrix is observed. Chancing the phosphine ligands to P(p-tolyl)3, reactions of [Rh(κ2-O,O-acac)(P(p-tolyl3)2)] with 1,7-diaryl-1,6-heptadiynes, however, resulted in a metal-mediated or -catalyzed cycloaddition reaction of alkynes and leads to full conversion to dimerization and trimerization products and recovery of the rhodium(I) starting material. This is intuitive, considering that P(Ar)3 (Ar = aryl) ligands are considered weaker -donor ligands and therefore have a higher tendency to dissociate. Therefore, rhodium(I) complexes with aryl phosphines as ligands have an increasing tendency to promote catalytic reactions, while the stronger -donating ligands (PMe3 or NHCs) promote the formation of stable rhodium complexes. Finally, in Chapter 4, the findings of the work conducted on N-heterocyclic carbenes (NHCs) and cyclic (alkyl)(amino)carbenes (CAACs) is presented. These compounds have unique electronic and steric properties and are therefore of great interest as ligands and organo-catalysts. In this work, studies of substitution reactions involving novel carbonyl complexes of rhodium and nickel are reported. For characterization and comparison of CAACmethyl with the large amount of data available for NHC and sterically more demanding CAAC ligands, an overview on physicochemical data (electronics, sterics and bond strength) is provided. The reaction of [Rh(-Cl)(CO)2]2 with 2 equivalents of CAACmethyl at low temperature afforded the mononuclear complex cis-[(RhCl(CO)2(CAACmethyl)]. However, reacting [Rh( Cl)(CO)2]2 with CAACmethyl at room temperature afforded a mixture of complexes. The mononuclear complex [(RhCl(CO)(CAACmethyl)2], the chloro-bridged complexes [(Rh2( Cl)2(CO)3(CAACmethyl)], [Rh(-Cl)(CO)(CAACmethyl)]2 and a carbon monoxide activation product were formed. The carbon monoxide activation product is presumably formed via the reaction of two equivalents of the CAAC with CO to give the bis-carbene adduct of CO, and subsequent rearrangement via migration of the Dipp moiety. While classical N-heterocyclic carbenes are not electrophilic enough to react with CO, related diamidocarbenes and alkyl(amino)carbenes undergo addition reactions with CO to give the corresponding ketenes. Consequently, to obtain the CAAC-disubstituted mononuclear complex selectively, 8 equivalents of CAACmethyl were reacted with 1 equivalent of [Rh(-Cl)(CO)2]2. For the evaluation of TEP values, [Ni(CO)3(CAAC)] was synthesized in collaboration with the group of Radius. With the complexes [(RhCl(CO)(CAACmethyl)2] and [Ni(CO)3(CAAC)] in hand, it was furthermore possible to examine the electronic and steric parameters of CAACmethyl. Like its bulkier congeners CAACmenthyl and CAACcy, the methyl-substituted CAAC is proposed to be a notably stronger -donor than common NHCs. While it has a very similar TEP value of 2046 cm-1, it additionally possess superior -acceptor properties (P = 67.2 ppm of phosphinidene adduct). CAACs appear to be very effective in the isolation of a variety of otherwise unstable main group and transition metal diamagnetic and paramagnetic species. This is due to their low-lying LUMO and the small singlet-triplet gap. These electronic properties also allow free CAACs to activate small molecules with strong bonds. They also bind strongly to transition metal centers, which enables their use under harsh conditions. One recent development is the use of CAACs as ligands in transition metal complexes, which previously were only postulated as short-lived catalytic intermediates.[292,345] The availability of these reactive species allows for a better understanding of known catalytic reactions and the design of new catalysts and, moreover, new applications. For example Radius et al.[320] prepared a CAAC complex of cobalt as a precursor for thin-film deposition and Steffen et al.[346] reported a CAAC complex of copper with very high photoluminescent properties, which could be used in LED devices. With the development of cheap and facile synthetic methods for the preparation of CAACs and their corresponding transition metals complexes, as well as the knowledge of their electronic properties, it is safe to predict that applications in and around this field of chemistry will continue to increase.}, subject = {{\"U}bergangsmetallkomplexe}, language = {en} } @phdthesis{Hofmann2018, author = {Hofmann, Lukas}, title = {The α-galactosidase A deficient mouse as a model for Fabry disease and the effect of Gb3 depositions on peripheral nociceptive ion channel function}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-158513}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Fabry disease (FD) is an X-linked lysosomal storage disorder with intracellular accumulation of globotriaosylceramide (Gb3) due to α-galactosidase A deficiency. We studied α-galactosidase A knockout mice (GLA KO) as a model for sensory disturbance and pain in FD. Pain associated behavior of young (3 months) and old (≥18 months) GLA KO mice and wildtype (WT) littermates in an inflammatory and a neuropathic pain model was investigated. Furthermore, affective and cognitive behavior was assessed in the na{\"i}ve state and in an inflammatory pain model. Gene and protein expression of pain associated ion channels and Gb3 accumulation in dorsal root ganglion (DRG) neurons was determined. We also performed patch clamp analysis on cultivated DRG neurons and human embryonic kidney 293 (HEK) cells expressing voltage-gated-sodium channel 1.7 (Nav1.7) as an in vitro model of FD. Intracellular Gb3 deposits were modulated using shRNA silencing of α-galactosidase A. After intraplantar injection of complete Freund`s adjuvant (CFA) and chronic constriction injury (CCI) of the right sciatic nerve, old GLA KO mice did not develop heat and mechanical hypersensitivity in contrast to young GLA KO and old WT mice. Additionally, we found no relevant differences between genotypes and age-groups in affective and cognitive behavior in the na{\"i}ve state and after CFA injection. Gene and protein expression analysis provided no explanation for the observed sensory impairment. However, cultured DRG neurons of old GLA KO mice revealed a marked decrease of sodium and Ih-currents compared to young GLA KO and old WT mice. DRG neurons of old GLA KO mice displayed substantial intracellular accumulation of Gb3 compared to young GLA KO and old WT mice. Similar to cultured neurons, sodium currents were also decreased in HEK cells treated with shRNA and consecutively increased intracellular Gb3 deposits compared to the control condition, but could be rescued by treatment with agalsidase-alpha. Our study unveils that, similar to patients with FD, GLA KO mice display age-dependent sensory deficits. However, contrary to patients, GLA KO mice are also protected from hypersensitivity induced by inflammation and nerve lesion due to Gb3-dependent and reversible reduction of neuronal sodium- and Ih-currents. Our data provide evidence for direct Gb3-dependent ion channel impairment in sensory DRG neurons as a potential contributor to sensory dysfunction and pain in FD.}, subject = {Fabry-Krankheit}, language = {en} } @phdthesis{Aulbach2018, author = {Aulbach, Julian}, title = {Gold-Induced Atomic Wires on Terraced Silicon Surfaces: Formation and Interactions of Silicon Spin Chains}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169347}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Atomic nanowires formed by self-assembled growth on semiconducting surfaces represent a feasible physical realization of quasi-1D electron systems and can be used to study fascinating 1D quantum phenomena. The system in the focus of this thesis, Si(553)-Au, is generated by Au adsorption onto a stepped silicon surface. It features two different chain types, interspersed with each other: A Au chain on the terrace, and a honeycomb chain of graphitic silicon located at the step edge. The silicon atoms at the exposed edges of the latter are predicted to be spin-polarized and charge-ordered [1], leading to an ordered array of local magnetic moments referred to as ``spin chains''. The present thesis puts this spin chain proposal to an experimental test. A detailed scanning tunneling microscopy (STM) and scanning tunneling spectroscopy (STS) scrutiny reveals a distinct unoccupied density of states (DOS) feature localized at every third Si step-edge atom, which aligns perfectly with the density functional theory (DFT) prediction. This finding provides strong evidence for the formation of spin chains at the Si(553)-Au step edges, and simultaneously rules out the interpretation of previous studies which attributed the x3 step-edge superstructure to a Peierls instability. To study the formation of spin chains in further detail, an additional member of the so-called Si(hhk)-Au family -- Si(775)-Au -- is analyzed. Based on DFT modeling (performed by S.C. Erwin, Naval Research Laboratory, USA) and detailed STM and STS experiments, a new structure model for this surface is developed, and the absence of spin chains at the Si(775)-Au step edges is demonstrated. The different step-edge charge distributions of all known Si(hhk)-Au surfaces are traced back to an electron transfer between the terrace and the step edge. Accordingly, an unintentional structure defect should create a localized spin at the Si(775)-Au step edge. This prediction is verified experimentally, and suggest that surface chemistry can be used to create and destroy Si spin chains. Having clarified why spin chains form on some Si(hhk)-Au surfaces but not on others, various interaction effects of the Si(553)-Au spin chains are inspected. A collaborative analysis by SPA-LEED (M. Horn-von Hoegen group, University of Duisburg-Essen, Germany), DFT (S.C. Erwin), and STM reveals strong lateral coupling between adjacent spin chains, bearing interesting implications for their magnetic ordering. The centered geometry uncovered leads to magnetic frustration, and may stabilize a 2D quantum spin liquid. Moreover, a complex interplay between neighboring Au and Si chains is detected. Specifically, the interaction is found effectively ``one-way'', i.e., the Si step edges respond to the Au chains but not vice versa. This unidirectional effect breaks the parity of the Si chains, and creates two different configurations of step edges with opposite directionality. In addition to the static properties of the Si(553)-Au surface mentioned above, the occurrence of solitons in both wire types is witnessed in real space by means of high-resolution STM imaging. The solitons are found to interact with one another such that both move in a coupled fashion along the chains. Likewise, STM experiments as a function of the tunneling current suggest an excitation of solitons along the step edge by the STM tunneling tip. Solitons are also found to play an essential role in the temperature-dependent behavior of the Si(553)-Au step edges. It is an accepted fact that the distinct x3 superstructure of the Si(553)-Au step edges vanishes upon heating to room temperature. As a first step in exploring this transition in detail over a large temperature range, a previously undetected, occupied electronic state associated with the localized step-edge spins is identified by means of angle-resolved photoemission spectroscopy (ARPES). A tracking of this state as a function of temperature reveals an order-disorder-type transition. Complementary STM experiments attribute the origin of this transition to local, thermally activated spin site hops, which correspond to soliton-anitsoliton pairs. Finally, a manipulation of the Si(553)-Au atomic wire array is achieved by the stepwise adsorption of potassium atoms. This does not only increase the filling of the Au-induced surface bands culminating in a metal-insulator transition (MIT), but also modifies the Si step-edge charge distribution, as indicated by STM and ARPES experiments. [1] S. C. Erwin and F. Himpsel, Intrinsic magnetism at silicon surfaces, Nat. Commun. 1, 58 (2010).}, subject = {Rastertunnelmikroskopie}, language = {en} } @phdthesis{Klotzky2018, author = {Klotzky, Jens}, title = {Well-posedness of a fluid-particle interaction model}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169009}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {This thesis considers a model of a scalar partial differential equation in the presence of a singular source term, modeling the interaction between an inviscid fluid represented by the Burgers equation and an arbitrary, finite amount of particles moving inside the fluid, each one acting as a point-wise drag force with a particle related friction constant. \begin{align*} \partial_t u + \partial_x (u^2/2) \&= \sum_{i \in N(t)} \lambda_i \Big(h_i'(t)-u(t,h_i(t)\Big)\delta(x-h_i(t)) \end{align*} The model was introduced for the case of a single particle by Lagouti{\`e}re, Seguin and Takahashi, is a first step towards a better understanding of interaction between fluids and solids on the level of partial differential equations and has the unique property of considering entropy admissible solutions and the interaction with shockwaves. The model is extended to an arbitrary, finite number of particles and interactions like merging, splitting and crossing of particle paths are considered. The theory of entropy admissibility is revisited for the cases of interfaces and discontinuous flux conservation laws, existing results are summarized and compared, and adapted for regions of particle interactions. To this goal, the theory of germs introduced by Andreianov, Karlsen and Risebro is extended to this case of non-conservative interface coupling. Exact solutions for the Riemann Problem of particles drifting apart are computed and analysis on the behavior of entropy solutions across the particle related interfaces is used to determine physically relevant and consistent behavior for merging and splitting of particles. Well-posedness of entropy solutions to the Cauchy problem is proven, using an explicit construction method, L-infinity bounds, an approximation of the particle paths and compactness arguments to obtain existence of entropy solutions. Uniqueness is shown in the class of weak entropy solutions using almost classical Kruzkov-type analysis and the notion of L1-dissipative germs. Necessary fundamentals of hyperbolic conservation laws, including weak solutions, shocks and rarefaction waves and the Rankine-Hugoniot condition are briefly recapitulated.}, subject = {Hyperbolische Differentialgleichung}, language = {en} } @phdthesis{NguyenNgoc2018, author = {Nguyen-Ngoc, Anh}, title = {On Performance Assessment of Control Mechanisms and Virtual Components in SDN-based Networks}, issn = {1432-8801}, doi = {10.25972/OPUS-16932}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169328}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {This dissertation focuses on the performance evaluation of all components of Software Defined Networking (SDN) networks and covers whole their architecture. First, the isolation between virtual networks sharing the same physical resources is investigated with SDN switches of several vendors. Then, influence factors on the isolation are identified and evaluated. Second, the impact of control mechanisms on the performance of the data plane is examined through the flow rule installation time of SDN switches with different controllers. It is shown that both hardware-specific and controller instance have a specific influence on the installation time. Finally, several traffic flow monitoring methods of an SDN controller are investigated and a new monitoring approach is developed and evaluated. It is confirmed that the proposed method allows monitoring of particular flows as well as consumes fewer resources than the standard approach. Based on findings in this thesis, on the one hand, controller developers can refer to the work related to the control plane, such as flow monitoring or flow rule installation, to improve the performance of their applications. On the other hand, network administrators can apply the presented methods to select a suitable combination of controller and switches in their SDN networks, based on their performance requirements}, subject = {Leistungsbewertung}, language = {en} } @phdthesis{Hetterich2018, author = {Hetterich, Daniel Marcus}, title = {Localization within disordered systems of star-like topology}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169318}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {This Thesis investigates the interplay of a central degree of freedom with an environment. Thereby, the environment is prepared in a localized phase of matter. The long-term aim of this setup is to store quantum information on the central degree of freedom while exploiting the advantages of localized systems. These many-body localized systems fail to equilibrate under the description of thermodynamics, mostly due to disorder. Doing so, they form the most prominent phase of matter that violates the eigenstate thermalization hypothesis. Thus, many-body localized systems preserve information about an initial state until infinite times without the necessity to isolate the system. This unique feature clearly suggests to store quantum information within localized environments, whenever isolation is impracticable. After an introduction to the relevant concepts, this Thesis examines to which extent a localized phase of matter may exist at all if a central degree of freedom dismantles the notion of locality in the first place. To this end, a central spin is coupled to the disordered Heisenberg spin chain, which shows many-body localization. Furthermore, a noninteracting analog describing free fermions is discussed. Therein, an impurity is coupled to an Anderson localized environment. It is found that in both cases, the presence of the central degree of freedom manifests in many properties of the localized environment. However, for a sufficiently weak coupling, quantum chaos, and thus, thermalization is absent. In fact, it is shown that the critical disorder, at which the metal-insulator transition of its environment occurs in the absence of the central degree of freedom, is modified by the coupling strength of the central degree of freedom. To demonstrate this, a phase diagram is derived. Within the localized phase, logarithmic growth of entanglement entropy, a typical signature of many-body localized systems, is increased by the coupling to the central spin. This property is traced back to resonantly coupling spins within the localized Heisenberg chain and analytically derived in the absence of interactions. Thus, the studied model of free fermions is the first model without interactions that mimics the logarithmic spreading of entanglement entropy known from many-body localized systems. Eventually, it is demonstrated that observables regarding the central spin significantly break the eigenstate thermalization hypothesis within the localized phase. Therefore, it is demonstrated how a central spin can be employed as a detector of many-body localization.}, subject = {Quanteninformatik}, language = {en} } @phdthesis{Muehlemann2018, author = {M{\"u}hlemann, Markus}, title = {Intestinal stem cells and the Na\(^+\)-D-Glucose Transporter SGLT1: potential targets regarding future therapeutic strategies for diabetes}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169266}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {The pancreas and the small intestine are pivotal organs acting in close synergism to regulate glucose metabolism. After absorption and processing of dietary glucose within the small intestine, insulin and glucagon are released from pancreatic islet cells to maintain blood glucose homeostasis. Malfunctions affecting either individual, organ-specific functions or the sophisticated interplay of both organs can result in massive complications and pathologic conditions. One of the most serious metabolic diseases of our society is diabetes mellitus (DM) that is hallmarked by a disturbance of blood glucose homeostasis. Type 1 (T1DM) and type 2 (T2DM) are the main forms of the disease and both are characterized by chronic hyperglycemia, a condition that evokes severe comorbidities in the long-term. In the past, several standard treatment options allowed a more or less adequate therapy for diabetic patients. Albeit there is much effort to develop new therapeutic interventions to treat diabetic patients in a more efficient way, no cure is available so far. In view of the urgent need for alternative treatment options, a more systemic look on whole organ systems, their biological relation and complex interplay is needed when developing new therapeutic strategies for DM. T1DM is hallmarked by an autoimmune-mediated destruction of the pancreatic β-cell mass resulting in a complete lack of insulin that is in most patients restored by applying a life-long recombinant insulin therapy. Therefore, novel regenerative medicine-based concepts focus on the derivation of bioartificial β-like cells from diverse stem cell sources in vitro that survive and sustain to secrete insulin after implantation in vivo. In this context, the first part of this thesis analyzed multipotent intestinal stem cells (ISCs) as alternative cell source to derive bioartificial, pancreatic β-like cells in vitro. From a translational perspective, intestinal stem cells pose a particularly attractive cell source since intestinal donor tissues could be obtained via minimal invasive endoscopy in an autologous way. Furthermore, intestinal and pancreatic cells both derive from the same developmental origin, the endodermal gut tube, favoring the differentiation process towards functional β-like cells. In this study, pancreas-specific differentiation of ISCs was induced by the ectopic expression of the pancreatic transcription factor 1 alpha (Ptf1a), a pioneer transcriptional regulator of pancreatic fate. Furthermore, pancreatic lineage-specific culture media were applied to support the differentiation process. In general, ISCs grow in vitro in a 3D Matrigel®-based environment. Therefore, a 2D culture platform for ISCs was established to allow delivery and ectopic expression of Ptf1a with high efficiency. Next, several molecular tools were applied and compared with each other to identify the most suitable technology for Ptf1a delivery and expression within ISCs as well as their survival under the new established 2D conditions. Success of differentiation was investigated by monitoring changes in cellular morphology and induction of pancreatic differentiation-specific gene expression profiles. In summary, the data of this project part suggest that Ptf1a harbors the potential to induce pancreatic differentiation of ISCs when applying an adequate differentiation media. However, gene expression analysis indicated rather an acinar lineage-determination than a pancreatic β-cell-like specification. Nevertheless, this study proved ISCs not only as interesting stem cell source for the generation of pancreatic cell types with a potential use in the treatment of T1DM but alsoPtf1a as pioneer factor for pancreatic differentiation of ISCs in general. Compared to T1DM, T2DM patients suffer from hyperglycemia due to insulin resistance. In T2DM management, the maintenance of blood glucose homeostasis has highest priority and can be achieved by drugs affecting the stabilization of blood glucose levels. Recent therapeutic concepts are aiming at the inhibition of the intestinal glucose transporter Na+-D-Glucose cotransporter 1 (SGLT1). Pharmacological inhibition of SGLT1 results in reduced postprandial blood glucose levels combined with a sustained and increased Glucagon-like peptide 1 (GLP-1) secretion. So far, systemic side effects of this medication have not been addressed in detail. Of note, besides intestinal localization, SGLT1 is also expressed in various other tissues including the pancreas. In context of having a closer look also on the interplay of organs when developing new therapeutic approaches for DM, the second part of this thesis addressed the effects on pancreatic islet integrity after loss of SGLT1. The analyses comprised the investigation of pancreatic islet size, cytomorphology and function by the use of a global SGLT1 knockout (SGLT1-/-) mouse model. As SGLT1-/- mice develop the glucose-galactose malabsorption syndrome when fed a standard laboratory chow, these animals derived a glucose-deficient, fat-enriched (GDFE) diet. Wildtype mice on either standard chow (WTSC) or GDFE (WTDC) allowed the discrimination between diet- and knockout-dependent effects. Notably, GDFE fed mice showed decreased expression and function of intestinal SGLT1, while pancreatic SGLT1 mRNA levels were unaffected. Further, the findings revealed increased isled sizes, reduced proliferation- and apoptosis rates as well as an increased α-cell and reduced β-cell proportion accompanied by a disturbed cytomorphology in islets when SGLT1 function is lost or impaired. In addition, pancreatic islets were dysfunctional in terms of insulin- and glucagon-secretion. Moreover, the release of intestinal GLP-1, an incretin hormone that stimulates insulin-secretion in the islet, was abnormal after glucose stimulatory conditions. In summary, these data show that intestinal SGLT1 expression and function is nutrient dependent. The data obtained from the islet studies revealed an additional and new role of SGLT1 for maintaining pancreatic islet integrity in the context of structural, cytomorphological and functional aspects. With special emphasis on SGLT1 inhibition in diabetic patients, the data of this project indicate an urgent need for analyzing systemic side effects in other relevant organs to prove pharmacological SGLT1 inhibition as beneficial and safe. Altogether, the findings of both project parts of this thesis demonstrate that focusing on the molecular and cellular relationship and interplay of the small intestine and the pancreas could be of high importance in context of developing new therapeutic strategies for future applications in DM patients.}, subject = {Stammzelle}, language = {en} } @phdthesis{Glogger2018, author = {Glogger, Marius}, title = {Single-molecule fluorescence microscopy in live \(Trypanosoma\) \(brucei\) and model membranes}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169222}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Der eukaryotische Parasit Trypanosoma brucei hat komplexe Strategien entwickelt um der Immunantwort eines Wirtes zu entkommen und eine persistente Infektion innerhalb dessen aufrechtzuerhalten. Ein zentrales Element seiner Verteidigungsstrategie st{\"u}tzt sich auf die Schutzfunktion seines Proteinmantels auf der Zelloberfl{\"a}che. Dieser Mantel besteht aus einer dichten Schicht aus identischen, Glykosylphosphatidylinositol (GPI)-verankerten variablen Oberfl{\"a}chenglykoproteinen (VSG). Der VSG Mantel verhindert die Erkennung der darunterliegenden, invarianten Epitope durch das Immunsystem. Obwohl es notwendig ist die Funktionsweise des VSG Mantels zu verstehen, vor allem um ihn als m{\"o}gliches Angriffsziel gegen den Parasiten zu verwenden, sind seine biophysikalischen Eigenschaften bisher nur unzureichend verstanden. Dies ist vor allem der Tatsache geschuldet, dass die hohe Motilit{\"a}t der Parasiten mikroskopische Studien in lebenden Zellen bisher weitestgehend verhinderten. In der vorliegenden Arbeit wird nun hochmoderne Einzelmolek{\"u}l-Fluoreszenzmikroskopie (EMFM) als M{\"o}glichkeit f{\"u}r mikroskopische Untersuchungen im Forschungsbereich der Trypanosomen vorgestellt. Die Arbeit umfasst Untersuchungen der VSG Dynamik unter definierten Bedingungen k{\"u}nstlicher Membransysteme. Es wurde zuerst der Einfluss der lateralen Proteindichte auf die VSG Diffusion untersucht. Experimente mittels Fluoreszenz- Wiederkehr nach irreversiblem Photobleichen und komplement{\"a}re Einzelmolek{\"u}l- Verfolgungs Experimente offenbarten, dass ein molekularer Diffusionsschwellenwert existiert. {\"U}ber diesem Schwellenwert wurde eine dichteabh{\"a}nige Reduzierung des Diffusionskoeffizienten gemessen. Eine relative Quantifizierung der rekonstituierten VSGs verdeutlichte, dass der Oberfl{\"a}chenmantel der Trypanosomen sehr nahe an diesem Schwellenwert agiert. Der VSG Mantel ist optimiert um eine hohe Proteindichte bei gleichzeitiger hoher Mobilit{\"a}t der VSGs zu gew{\"a}hrleisten. Des Weiteren wurde der Einfluss der VSG N-Glykosylierung auf die Diffusion des Proteins quantitativ untersucht. Die Messungen ergaben, dass die N-Glykosylierung dazu beitr{\"a}gt eine hohe Mobilit{\"a}t bei hohen Proteindichten aufrechtzuerhalten. Eine detaillierte Analyse von VSG Trajektorien offenbarte, dass zwei unterschiedliche Populationen frei diffundierender VSGs in der k{\"u}nstlichen Membran vorlagen. K{\"u}rzlich wurde entdeckt, dass VSGs zwei strukturell unterschiedliche Konformationen annehmen k{\"o}nnen. Die Messungen in der Arbeit stimmen mit diesen Beschreibungen {\"u}berein. Die Ergebnisse der EMFM in k{\"u}nstlichen Membranen wurden durch VSG Einzelmolek{\"u}l- Verfolgungs Experimente auf lebenden Zellen erg{\"a}nzt. Es wurde eine hohe Mobilit{\"a}t und Dynamik einzelner VSGs gemessen, was die allgemein dynamische Natur des VSG Mantels verdeutlicht. Dies f{\"u}hrte zu der Schlussfolgerung, dass der VSG Mantel auf lebenden Trypanosomen ein dichter und dennoch dynamischer Schutzmantel ist. Die F{\"a}higkeit der VSGs ihre Konformation flexibel anzupassen, unterst{\"u}tzt das Erhalten der Fluidit{\"a}t bei variablen Dichten. Diese Eigenschaften des VSG Mantels sind elementar f{\"u}r die Aufrechterhaltung einer presistenden Infektion eines Wirtes. In dieser Arbeit werden des Weiteren verschiedene, auf Hydrogel basierende Einbettungsmethoden vorgestellt. Diese erm{\"o}glichten die Zellimmobilisierung und erlaubten EMFM in lebenden Trypanosomen. Die Hydrogele wiesen eine hohe Zytokompatibilit{\"a}t auf. Die Zellen {\"u}berlebten in den Gelen f{\"u}r eine Stunde nach Beginn der Immobilisierung. Die Hydrogele erf{\"u}llten die Anforderungen der Superresolution Mikroskopie (SRM) da sie eine geringe Autofluoreszenz im Spektralbereich der verwendeten Fluorophore besaßen. Mittels SRM konnte nachgewiesen werden, dass die Hydrogele die Zellen effizient immobilisierten. Als erstes Anwendungsbeispiel der Methode wurde die Organisation der Plasmamembran in lebenden Trypanosomen untersucht. Die Untersuchung eines fluoreszenten Tracers in der inneren Membranschicht ergab, dass dessen Verteilung nicht homogen war. Es wurden spezifische Membrandom{\"a}nen gefunden, in denen das Molek{\"u}l entweder vermehrt oder vermindert auftrat. Dies f{\"u}hrte zu der Schlussfolgerung, dass diese Verteilung durch eine Interaktion des Tracers mit Proteinen des zellul{\"a}ren Zytoskeletts zustande kam. Die in dieser Arbeit pr{\"a}sentierten Ergebnisse zeigen, dass EMFM erfolgreich f{\"u}r verschiedene biologische Untersuchungen im Forschungsfeld der Trypanosomen angewendet werden kann. Dies gilt zum Beispiel f{\"u}r die Untersuchung von der VSG Dynamik in k{\"u}nstlichen Membransystemen, aber auch f{\"u}r Studien in lebenden Zellen unter Verwendung der auf Hydrogelen basierenden Zelleinbettung.}, subject = {Trypanosoma brucei}, language = {en} } @phdthesis{Mao2018, author = {Mao, Lujia}, title = {Transition Metal-Catalyzed Construction of Benzyl/Allyl sp\(^3\) and Vinyl/Allenyl sp\(^2\) C-B Bonds}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-154022}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Organoboron compounds, such as benzyl-, allyl-, allenyl-, vinyl-, and 2-boryl allyl-boronates, have been synthesized via metal-catalyzed borylations of sp3 C-O and C-H bonds. Thus, Cu-catalyzed borylations of alcohols and their derivatives provide benzyl-, allyl-, allenyl-, vinyl-, and 2-boryl allyl-boronates via nucleophilic substitution. The employment of Ti(OiPr)4 turns the OH moiety into a good leaving group ('OTi'). The products of Pd-catalyzed oxidative borylations of allylic C-H bonds of alkenes were isolated and purified, and their application in the one-pot synthesis of stereodefined homoallyl alcohols was also investigated. Chapter 2 presents a copper-catalyzed synthesis of benzyl-, allyl-, and allenyl-boronates from benzylic, allylic, and propargylic alcohols, respectively, employing a commercially available catalyst precursor, [Cu(CH3CN)4]2+[BF4-]2, and Xantphos as the ligand. The borylation of benzylic alcohols was carried out at 100 oC with 5-10 mol \% [Cu(CH3CN)4]2+[BF4-]2, which afforded benzylic boronates in 32\%-95\% yields. With 10 mol \% [Cu(CH3CN)4]2+[BF4-]2, allylic boronates were provided in 53\%-89\% yields from the borylation of allylic alcohols at 60 or 100 oC. Secondary allylboronates were prepared in 72\%-84\% yields from the borylation of primary allylic alcohols, which also suggests that a nucleophilic substitution pathway is involved in this reaction. Allenylboronates were also synthesized in 72\%-89\% yields from the borylation of propargylic alcohols at 40 or 60 oC. This methodology can be extended to borylation of benzylic and allylic acetates. This protocol exhibits broad reaction scope (40 examples) and high efficiency (up to 95\% yield) under mild conditions, including the preparation of secondary allylic boronates. Preliminary mechanistic studies suggest that nucleophilic substitution is involved in this reaction. Chapter 3 reports an efficient methodology for the synthesis of vinyl-, allyl-, and (E)-2-boryl allylboronates from propargylic alcohols via copper-catalyzed borylation reactions under mild conditions. In the presence of a commercially available catalyst precursor (Cu(OAc)2 or Cu(acac)2) and ligand (Xantphos), the reaction affords the desired products in up to 92\% yield with a broad substrate scope (43 examples). Vinylboronates were synthesized in 50\%-83\% yields via Cu-catalyzed hydroboration of mono-substituted propargylic alcohols. With 1,1-disubstituted propargylic alcohols as the starting materials and Cu(OAc)2 as the catalyst precursor, a variety of allylboronates were synthesized in 44\%-83\% yields. The (E)-2-boryl allylboronates were synthesized in 54\%-92\% yields via the Cu-catalyzed diboration of propargylic alcohols. The stereoselectivity is different from the Pd(dba)2-catalyzed diboration of allenes that provided (Z)-2-boryl allylboronates predominantly. The isolation of an allenyl boronate as the reaction intermediate suggests that an SN2'-type reaction, followed by borylcupration, is involved in the mechanism of the diboration of propargylic alcohols. In chapter 4, a Pd-catalyzed allylic C-H borylation of alkenes is reported. The transformation exhibits high regioselectivity with a variety of linear alkenes, employing a Pd-pincer complex as the catalyst precursor, and the allylic boronate products were isolated and purified. This protocol can also be extended to one-pot carbonyl allylation reactions to provide homoallyl alcohols efficiently. An interesting mechanistic feature is that the reaction proceeds via a Pd(II)/Pd(IV) catalytic cycle. Formation of the Pd(IV) intermediate occurs by a unique combination of an NCNpincer complex and application of F-TEDA-BF4 as the oxidant. An important novelty of the present C-H borylation reaction is that all allyl-Bpin products can be isolated with usually high yields. This is probably a consequence of the application of the NCN-pincer complex as catalyst, which selectively catalyzes C-B bond formation avoiding subsequent C-B bond cleavage based side-reactions}, subject = {{\"U}bergangsmetall}, language = {en} } @phdthesis{DinhXuan2018, author = {Dinh-Xuan, Lam}, title = {Quality of Experience Assessment of Cloud Applications and Performance Evaluation of VNF-Based QoE Monitoring}, issn = {1432-8801}, doi = {10.25972/OPUS-16918}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169182}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {In this thesis various aspects of Quality of Experience (QoE) research are examined. The work is divided into three major blocks: QoE Assessment, QoE Monitoring, and VNF Performance Evaluation. First, prominent cloud applications such as Google Docs and a cloud-based photo album are explored. The QoE is characterized and the influence of packet loss and delay is studied. Afterwards, objective QoE monitoring for HTTP Adaptive Video Streaming (HAS) in the cloud is investigated. Additionally, by using a Virtual Network Function (VNF) for QoE monitoring in the cloud, the feasibility of an interworking of Network Function Virtualization (NFV) and cloud paradigm is evaluated. To this end, a VNF that exploits deep packet inspection technique was used to parse the video traffic. An algorithm is then designed accordingly to estimate video quality and QoE based on network and application layer parameters. To assess the accuracy of the estimation, the VNF is measured in different scenarios under different network QoS and the virtual environment of the cloud architecture. The insights show that the different geographical deployments of the VNF influence the accuracy of the video quality and QoE estimation. Various Service Function Chain (SFC) placement algorithms have been proposed and compared in the context of edge cloud networks. On the one hand, this research is aimed at cloud service providers by providing methods for evaluating QoE for cloud applications. On the other hand, network operators can learn the pitfalls and disadvantages of using the NFV paradigm for such a QoE monitoring mechanism.}, subject = {Quality of Experience}, language = {en} } @phdthesis{Poerner2018, author = {P{\"o}rner, Frank}, title = {Regularization Methods for Ill-Posed Optimal Control Problems}, edition = {1. Auflage}, publisher = {W{\"u}rzburg University Press}, address = {W{\"u}rzburg}, isbn = {978-3-95826-086-3 (Print)}, doi = {10.25972/WUP-978-3-95826-087-0}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-163153}, school = {W{\"u}rzburg University Press}, pages = {xiii, 166}, year = {2018}, abstract = {This thesis deals with the construction and analysis of solution methods for a class of ill-posed optimal control problems involving elliptic partial differential equations as well as inequality constraints for the control and state variables. The objective functional is of tracking type, without any additional \(L^2\)-regularization terms. This makes the problem ill-posed and numerically challenging. We split this thesis in two parts. The first part deals with linear elliptic partial differential equations. In this case, the resulting solution operator of the partial differential equation is linear, making the objective functional linear-quadratic. To cope with additional control constraints we introduce and analyse an iterative regularization method based on Bregman distances. This method reduces to the proximal point method for a specific choice of the regularization functional. It turns out that this is an efficient method for the solution of ill-posed optimal control problems. We derive regularization error estimates under a regularity assumption which is a combination of a source condition and a structural assumption on the active sets. If additional state constraints are present we combine an augmented Lagrange approach with a Tikhonov regularization scheme to solve this problem. The second part deals with non-linear elliptic partial differential equations. This significantly increases the complexity of the optimal control as the associated solution operator of the partial differential equation is now non-linear. In order to regularize and solve this problem we apply a Tikhonov regularization method and analyse this problem with the help of a suitable second order condition. Regularization error estimates are again derived under a regularity assumption. These results are then extended to a sparsity promoting objective functional.}, subject = {Optimale Steuerung}, language = {en} } @phdthesis{MeiningergebChrist2018, author = {Meininger [geb. Christ], Susanne}, title = {Processing of calcium and magnesium phosphate cements for bone substitution}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169126}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {The main focus of this thesis was the processing of different calcium and magnesium phosphate cements together with an optimization of mechanical and biological properties. Therefore, different manufacturing techniques like 3D powder printing and centrifugally casting were employed for the fabrication of reinforced or biomedically improved implants. One of the main problems during 3D powder printing is the low green strength of many materials, especially when they are only physically bonded and do not undergo a setting reaction. Such materials need post-treatments like sintering to exhibit their full mechanical performance. However, the green bodies have to be removed from the printer requiring a certain stability. With the help of fiber reinforcement, the green strength of printed gypsum samples could be increased by the addition of polymeric and glass fibers within the printing process. The results showed that fiber reinforcement during 3D powder printing is possible and opens up diverse opportunities to enhance the damage tolerance of green bodies as well as directly printed samples. The transfer to biomedically relevant materials like calcium and magnesium phosphate cements and biocompatible fibers would be the next step towards reinforced patient-specific implants. In a second approach, centrifugally casting derived from construction industries was established for the fabrication of hollow bioceramic cylinders. The aim was the replacement of the diaphysis of long bones, which exhibit a tubular structure with a high density of cortical bone on the fringe. By centrifugation, cement slurries with and without additives could be fabricated to tubes. As a first establishment, the processing parameters regarding the material (e.g. cement composition) as well as the set-up (e.g. rotation times) had to be optimized for each system. In respect of mechanics, such tubes can keep up with 3D powder printed tubes, although the mechanical performance of 3D printed tubes is strongly dependent on printing directions. Additionally, some material compositions like dual setting systems cannot be fabricated by 3D powder printing. Therefore, a transfer of such techniques to centrifugally casting enabled the fabrication of tubular structures with an extremely high damage tolerance due to high deformation ability. A similar effect was achieved by fiber (mesh) addition, as already shown for 3D powder printing. Another possibility of centrifugally casting is the combination of different materials resulting in graded structures to adjust implant degradation or bone formation. This became especially apparent for the incorporation of the antibiotic vancomycin, which is used for the treatment of bacterial implant infections. A long-term release could be achieved by the entrapment of the drug between magnesium phosphate cement layers. Therefore, the release of the drug could be regulated by the degradation of the outer shell, which supports the release into an acidic bacterial environment. The centrifugally casting technique exhibited to be a versatile tool for numerous materials and applications including the fabrication of non-centrosymmetric patient-specific implants for the reconstruction of human long bones. The third project aimed to manufacture strontium-substituted magnesium phosphate implants with improved biological behavior by 3D powder printing. As the promoting effect of strontium on bone formation and the inhibitory impact on bone resorption is already well investigated, the incorporation of strontium into a degradable magnesium phosphate cement promised a fast integration and replacement of the implant. Porous structures were obtained with a high pore interconnectivity that is favorable for cell invasion and bone ingrowth. Despite the porosity, the mechanical performance was comparable to pure magnesium phosphate cement with a high reliability of the printed samples as quantitatively determined by Weibull statistics. However, the biological testing was impeded by the high degradation rate and the relating ion release. The high release of phosphate ions into surrounding media and the detachment of cement particles from the surface inhibited osteoblast growth and activity. To distinguish those two effects, a direct and indirect cell seeding is always required for degradable materials. Furthermore, the high phosphate release compared to the strontium release has to be managed during degradation such that the adverse effect of phosphate ions does not overwhelm the bone promoting effect of the strontium ions. The manufacturing techniques presented in this thesis together with the material property improvement offer a diverse tool box for the fabrication of patient-specific implants. This includes not just the individual implant shape but also the application like bone growth promotion, damage tolerance and local drug delivery. Therefore, this can act as the basis for further research on specific medical indications.}, subject = {Calciumphosphate}, language = {en} } @phdthesis{Braun2018, author = {Braun, Alexandra Carolin}, title = {Bioresponsive delivery of anticatabolic and anabolic agents for muscle regeneration using bioinspired strategies}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-169047}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Progressive loss of skeletal muscle mass, strength and function poses a major threat to independence and quality of life, particularly in the elderly. To date, sarcopenia therapy consists of resistance exercise training in combination with protein supplementation due to the limited efficacy of available pharmacological options in counteracting the effects of muscle wasting. Therapeutic intervention with growth factors including insulin-like growth factor I (IGF-I) or inhibitors of myostatin  a potent suppressor of myogenesis  hold potential to rebalance the altered activity of anabolic and catabolic cytokines. However, dosing limitations due to acute side effects and disruptions of the homeostasis have so far precluded clinical application. Intending to provide a therapy with a superior safety and efficacy profile by directing drug release to inflamed tissue and minimizing off-target activity, we designed bioresponsive delivery systems for an anti-catabolic peptide and anabolic IGF-I responding to local flares of muscle wasting. In Chapter I, current concepts for bioorthogonal conjugation methods are discussed and evaluated based on various drug delivery applications. With a focus on protein delivery, challenges and potential pitfalls of each chemical and enzymatic conjugation strategy are analyzed and opportunities regarding their use for coupling of biomolecules are given. Based on various studies conjugating proteins to polymers, particles and biomaterials using different site-directed approaches, the chapter summarizes available strategies and highlights certain aspects requiring particular consideration when applied to biomolecules. Finally, a decision process for selection of an optimum conjugation strategy is exemplarily presented. Three of these bioorthogonal coupling reactions are applied in Chapter II detailing the potential of site-directed conjugation in the development of novel, homogenous drug delivery systems. The chapter describes the design of a delivery system of a myostatin inhibitor (MI) for controlled and local release counteracting myositis flares. MI release from the carrier is driven by increased matrix metalloproteinase (MMP) levels in compromised muscle tissues cleaving the interposed linker, thereby releasing the peptide inhibitor from the particulate carrier. Release experiments were performed to assess the response towards various MMP isoforms (MMP-1, -8, -9 and -13) - as upregulated during skeletal muscle myopathies - and the release pattern of the MI in case of disease progression was analyzed. By selection of the protease-sensitive linker (PSL) showing variable susceptibilities to proteases, release rates of the MI can be controlled and adapted. Immobilized MI as well as released MI as response to MMP upregulation was able to antagonize the effects of myostatin on cell signalling and myoblast differentiation. The approach of designing bioresponsive protein delivery systems was also applied to the anabolic growth factor IGF-I, as described in Chapter III. Numerous studies of PEGylated proteins or peptides reveal, that successful therapy is challenged by safety and efficacy issues, as polymer attachment considerably alters the properties of the biologic, thereby jeopardizing clinical efficacy. To this end, a novel promising approach is presented, intending to exploit beneficial effects of PEGylation on pharmacokinetics, but addressing the pharmacodynamic challenges by releasing the protein upon entering the target tissue. This was realized by integration of a PSL between the PEG moiety and the protein. The soluble polymer conjugate was produced by site-directed, enzymatic conjugation of IGF-I to the PSL, followed by attachment of a 30 kDa-PEG using Strain-promoted azide-alkyne cycloaddition (SPAAC). This strategy illustrates the potential of bioorthogonal conjugation (as described in Chapter I) for generation of homogenous protein-polymer conjugates with reproducible outcome, but also emphasizes the altered protein properties resulting from permanent polymer conjugation. As compared to wild type IGF-I, the PEGylated protein showed considerable changes in pharmacologic effects - such as impaired insulin-like growth factor binding protein (IGFBPs) interactions, submaximal proliferative activity and altered endocytosis patterns. In contrast, IGF-I characteristics were fully restored upon local disintegration of the conjugate triggered by MMP upregulation and release of the natural growth factor. For successful formulation development for the proteins and conjugates, the careful selection of suitable excipients is crucial for a safe and reliable therapy. Chapter IV addresses one aspect by highlighting the chemical heterogeneity of excipients and associated differences in performance. Polysorbate 80 (PS80) is a surfactant frequently used in protein formulations to prevent aggregation and surface adsorption. Despite being widely deployed as a standard excipient, heterogeneous composition and performance entails the risk of eliciting degradation and adverse effects on protein stability. Based on a comprehensive study using different batches of various suppliers, the PS80 products were characterized regarding chemical composition and physicochemical properties, facilitating the assessment of excipient performance in a formulation. Noticeable deviations were recorded between different suppliers as well as between batches of the same suppliers. Correlation of all parameters revealed, that functionality related characteristics (FRCs) could be reliably predicted based on chemical composition alone or by a combination of chemical and physicochemical properties, respectively. In summary, this thesis describes and evaluates novel strategies for the targeted delivery and controlled release of biologics intended to counteract the imbalance of anabolic and catabolic proteins observed during aging and musculoskeletal diseases. Two delivery platforms were developed and characterized in vitro - (i) using anti-catabolic peptides immobilized on a carrier for local delivery and (ii) using soluble IGF-I polymer conjugates for systemic application. Both approaches were implemented by bioorthogonal coupling strategies, which were carefully selected in consideration of limitations, side reactions and efficiency aspects. Bioresponsive release of the active biomolecules following increased protease activity could be successfully realized. The therapeutic potential of these approaches was demonstrated using various cell-based potency assays. The systems allow targeted and controlled release of the growth factor IGF-I and anti-catabolic peptides thereby overcoming safety concerns of current growth factor therapy and thus positively impacting the benefit-risk profile of potent therapeutics. Taking potential heterogeneity and by-product concerns into account, comprehensive excipient characterization was performed and a predictive algorithm for FRCs developed, in order to facilitate formulation design and guarantee a safe and efficient therapy from start to finish.}, subject = {Muskelatrophie}, language = {en} } @techreport{Greubel2018, type = {Working Paper}, author = {Greubel, Johannes}, title = {Towards a Profound European Asylum System? On EU Governance during the Refugee Crisis}, edition = {1. Auflage}, issn = {2625-6193}, doi = {10.25972/OPUS-16879}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-168797}, pages = {43}, year = {2018}, abstract = {The refugee crisis has developed as one of the major challenges for EU governance in recent years. From 2013 onwards, the crisis determined the political agenda and public discourse within European politics. During that time, the numbers of asylum seekers reaching Europe increased dramatically, with more than one million people applying for asylum at the crisis peak in 2015. This paper deals with the efforts taken by the EU and its member states to mitigate and overcome the refugee crisis. How exactly has the EU reacted to the refugee crisis and how and to what extend have the EU and its governance changed throughout the crisis? These research questions are approached through a reconstructive analysis of the whole period of crisis. This approach provides for a comprehensive examination of the refugee crisis that includes all issues, measures and processes of the EU's policy reaction at the same time. It will be argued that due to severe shortcomings of the Dublin regulation and the Common European Asylum System, a crisis in the EU's refugee policy was already predestined. This was the case from 2013 onwards. The EU approached the crisis in three stages - neglect and non-solidarity leading to unilateral approaches by affected states, supranational short-term emergency measures during the peak of crisis and enhanced cooperation with third countries, especially with Turkey, the Western Balkans states and African states - until the crisis lost traction in 2017. Yet, the asylum system's shortcomings are still not eliminated as the lasting measures of the EU's crisis management between 2013 and 2018 mainly focused on border security and externalisation. EU governance changed towards more intergovernmental, informal and regional action. Further, the crisis led to serious rows between member states, leading to the fragmentation of the EU into two blocs. With decreasing numbers of asylum seeker in the last few years, what remains is an incomplete asylum system and a political crisis among member states.}, subject = {Europ{\"a}ische Union}, language = {en} } @phdthesis{Heinrichs2018, author = {Heinrichs, Susanne Margarete}, title = {Myocardial B-cell infiltration following occlusion of the left anterior descending artery in mice is driven by CXCL13}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-168554}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Myocardial B-cell infiltration after LAD occlusion in mice is driven by CXCL13 After myocardial infarction, the immune system is activated and regulates wound healing and remodeling processes in the heart. While the role of T cells has been elucidated already, the function of B cells in myocardial infarction remained relatively unclear until now. It is, however, already known that B cells are of importance in healing processes in other tissues, for example in the skin. Our studies therefore addressed the role and function of B cells in healing and early remodeling processes in the myocardium after infarction. Under physiological conditions, only few B cells can be found in the heart. After myocardial infarction, however, which we modelled with a permanent ligation of the left anterior descending artery (LAD) in C57BL/6J mice, we could demonstrate that B lymphocytes accumulate in the early phase after tissue injury (days one to seven) in the myocardium. To detect B cells, we performed immunofluorescence stainings on cryosections of infarcted hearts using an anti-B220 antibody. Quantitative analysis of tissue infiltration revealed that B cells peaked at day seven. In flow cytometry, we further characterized the B cells infiltrating infarcted tissue. We found that most of them were mature B cells (IgM+, IgD+). Next, we wanted to outline a potential mechanism responsible for B-cell infiltration to the site of tissue injury. We therefore performed ELISA experiments revealing that CXCL13 was upregulated in scar tissue. Antibody-mediated neutralization of CXCL13 verifiably attenuated B-cell infiltration. Treated mice also showed - in the tendency - smaller infarct sizes and an improved survival. In conclusion, we could show that B lymphocytes infiltrate the myocardium after MI in mice following a local CXCL13 gradient and that it is, most likely, beneficial to inhibit this process.}, subject = {Maus}, language = {en} } @phdthesis{Botrel2018, author = {Botrel, Loic}, title = {Brain-computer interfaces (BCIs) based on sensorimotor rhythms - Evaluating practical interventions to improve their performance and reduce BCI inefficiency}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-168110}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2018}, abstract = {Brain computer interfaces based on sensorimotor rhythms modulation (SMR-BCIs) allow people to emit commands to an interface by imagining right hand, left hand or feet movements. The neurophysiological activation associated with those specific mental imageries can be measured by electroencephalography and detected by machine learning algorithms. Improvements for SMR-BCI accuracy in the last 30 years seem to have reached a limit. The currrent main issue with SMR-BCIs is that between 15\% to 30\% cannot use the BCI, called the "BCI inefficiency" issue. Alternatively to hardware and software improvements, investigating the individual characteristics of the BCI users has became an interesting approach to overcome BCI inefficiency. In this dissertation, I reviewed existing literature concerning the individual sources of variation in SMR-BCI accuracy and identified generic individual characteristics. In the empirical investigation, attention and motor dexterity predictors for SMR-BCI performance were implemented into a trainings that would manipulate those predictors and lead to higher SMR-BCI accuracy. Those predictors were identified by Hammer et al. (2012) as the ability to concentrate (associated with relaxation levels) and "mean error duration" in a two-hand visuo-motor coordination task (VMC). Prior to a SMR-BCI session, a total of n=154 participants in two locations took part of 23 min sessions of either Jacobson's Progressive Muscle Relaxation session (PMR), a VMC session, or a control group (CG). No effect of PMR or VMC manipulation was found, but the manipulation checks did not consistently confirm whether PMR had an effect of relaxation levels and VMC on "mean error duration". In this first study, correlations between relaxation levels or "mean error duration" and accuracy were found but not in both locations. A second study, involving n=39 participants intensified the training in four sessions on four consecutive days or either PMR, VMC or CG. The effect or manipulation was assessed for in terms of a causal relationship by using a PRE-POST study design. The manipulation checks of this second study validated the positive effect of training on both relaxation and "mean error duration". But the manipulation did not yield a specific effect on BCI accuracy. The predictors were not found again, displaying the instability of relaxation levels and "mean error duration" in being associated with BCI performance. An effect of time on BCI accuracy was found, and a correlation between State Mindfulness Scale and accuracy were reported. Results indicated that a short training of PMR or VMC were insufficient in increasing SMR-BCI accuracy. This study contrasted with studies succeeding in increasing SMR-BCI accuracy Tan et al. (2009, 2014), by the shortness of its training and the relaxation training that did not include mindfulness. It also contrasted by its manipulation checks and its comprehensive experimental approach that attempted to replicate existing predictors or correlates for SMR-BCI accuracy. The prediction of BCI accuracy by individual characteristics is receiving increased attention, but requires replication studies and a comprehensive approach, to contribute to the growing base of evidence of predictors for SMR-BCI accuracy. While short PMR and VMC trainings could not yield an effect on BCI performance, mindfulness meditation training might be beneficial for SMR-BCI accuracy. Moreover, it could be implemented for people in the locked-in-syndrome, allowing to reach the end-users that are the most in need for improvements in BCI performance.}, subject = {Gehirn-Computer-Schnittstelle}, language = {en} }