TY - JOUR A1 - Wehrheim, Maren H. A1 - Faskowitz, Joshua A1 - Sporns, Olaf A1 - Fiebach, Christian J. A1 - Kaschube, Matthias A1 - Hilger, Kirsten T1 - Few temporally distributed brain connectivity states predict human cognitive abilities JF - NeuroImage N2 - Highlights • Brain connectivity states identified by cofluctuation strength. • CMEP as new method to robustly predict human traits from brain imaging data. • Network-identifying connectivity ‘events’ are not predictive of cognitive ability. • Sixteen temporally independent fMRI time frames allow for significant prediction. • Neuroimaging-based assessment of cognitive ability requires sufficient scan lengths. Abstract Human functional brain connectivity can be temporally decomposed into states of high and low cofluctuation, defined as coactivation of brain regions over time. Rare states of particularly high cofluctuation have been shown to reflect fundamentals of intrinsic functional network architecture and to be highly subject-specific. However, it is unclear whether such network-defining states also contribute to individual variations in cognitive abilities – which strongly rely on the interactions among distributed brain regions. By introducing CMEP, a new eigenvector-based prediction framework, we show that as few as 16 temporally separated time frames (< 1.5% of 10 min resting-state fMRI) can significantly predict individual differences in intelligence (N = 263, p < .001). Against previous expectations, individual's network-defining time frames of particularly high cofluctuation do not predict intelligence. Multiple functional brain networks contribute to the prediction, and all results replicate in an independent sample (N = 831). Our results suggest that although fundamentals of person-specific functional connectomes can be derived from few time frames of highest connectivity, temporally distributed information is necessary to extract information about cognitive abilities. This information is not restricted to specific connectivity states, like network-defining high-cofluctuation states, but rather reflected across the entire length of the brain connectivity time series. KW - functional connectivity KW - resting state KW - machine learning KW - predictive modeling KW - general cognitive ability Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-349874 VL - 277 ER - TY - JOUR A1 - Weh, Manuel A1 - Shoyama, Kazutaka A1 - Würthner, Frank T1 - Preferential molecular recognition of heterochiral guests within a cyclophane receptor JF - Nature Communications N2 - The discrimination of enantiomers by natural receptors is a well-established phenomenon. In contrast the number of synthetic receptors with the capability for enantioselective molecular recognition of chiral substrates is scarce and for chiral cyclophanes indicative for a preferential binding of homochiral guests. Here we introduce a cyclophane composed of two homochiral core-twisted perylene bisimide (PBI) units connected by p-xylylene spacers and demonstrate its preference for the complexation of [5]helicene of opposite helicity compared to the PBI units of the host. The pronounced enantio-differentiation of this molecular receptor for heterochiral guests can be utilized for the enrichment of the P-PBI-M-helicene-P-PBI epimeric bimolecular complex. Our experimental results are supported by DFT calculations, which reveal that the sterically demanding bay substituents attached to the PBI chromophores disturb the helical shape match of the perylene core and homochiral substrates and thereby enforce the formation of syndiotactic host-guest complex structures. Hence, the most efficient substrate binding is observed for those aromatic guests, e. g. perylene, [4]helicene, phenanthrene and biphenyl, that can easily adapt in non-planar axially chiral conformations due to their inherent conformational flexibility. In all cases the induced chirality for the guest is opposed to those of the embedding PBI units, leading to heterochiral host-guest structures. KW - coordination chemistry KW - molecular capsules KW - stereochemistry Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-357750 VL - 14 ER - TY - JOUR A1 - Weber, Patrick A1 - Beck, Melina A1 - Klug, Michael A1 - Klug, Andreas A1 - Klug, Alexander A1 - Glowalla, Claudio A1 - Gollwitzer, Hans T1 - Survival of patient-specific unicondylar knee replacement JF - Journal of Personalized Medicine N2 - Unicompartmental knee arthroplasty (UKA) in isolated medial or lateral osteoarthritis leads to good clinical results. However, revision rates are higher in comparison to total knee arthroplasty (TKA). One reason is suboptimal fitting of conventional off-the-shelf prostheses, and major overhang of the tibial component over the bone has been reported in up to 20% of cases. In this retrospective study, a total of 537 patient-specific UKAs (507 medial prostheses and 30 lateral prostheses) that had been implanted in 3 centers over a period of 10 years were analyzed for survival, with a minimal follow-up of 1 year (range 12 to 129 months). Furthermore, fitting of the UKAs was analyzed on postoperative X-rays, and tibial overhang was quantified. A total of 512 prostheses were available for follow-up (95.3%). Overall survival rate (medial and lateral) of the prostheses after 5 years was 96%. The 30 lateral UKAs showed a survival rate of 100% at 5 years. The tibial overhang of the prosthesis was smaller than 1 mm in 99% of cases. In comparison to the reported results in the literature, our data suggest that the patient-specific implant design used in this study is associated with an excellent midterm survival rate, particularly in the lateral knee compartment, and confirms excellent fitting. KW - unicompartmental knee arthroplasty KW - osteoarthritis KW - patient-specific implant KW - partial knee arthroplasty KW - patient-specific instruments Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-313650 SN - 2075-4426 VL - 13 IS - 4 ER - TY - JOUR A1 - Waxman, Susannah A1 - Strzalkowska, Alicja A1 - Wang, Chao A1 - Loewen, Ralitsa A1 - Dang, Yalong A1 - Loewen, Nils A. T1 - Tissue-engineered anterior segment eye cultures demonstrate hallmarks of conventional organ culture JF - Graefe’s Archive for Clinical and Experimental Ophthalmology N2 - Background Glaucoma is a blinding disease largely caused by dysregulation of outflow through the trabecular meshwork (TM), resulting in elevated intraocular pressure (IOP). We hypothesized that transplanting TM cells into a decellularized, tissue-engineered anterior segment eye culture could restore the outflow structure and function. Methods Porcine eyes were decellularized with freeze–thaw cycles and perfusion of surfactant. We seeded control scaffolds with CrFK cells transduced with lentiviral vectors to stably express eGFP and compared them to scaffolds seeded with primary TM cells as well as to normal, unaltered eyes. We tracked the repopulation behavior, performed IOP maintenance challenges, and analyzed the histology. Results Transplanted cells localized to the TM and progressively infiltrated the extracellular matrix, reaching a distribution comparable to normal, unaltered eyes. After a perfusion rate challenge to mimic a glaucomatous pressure elevation, transplanted and normal eyes reestablished a normal intraocular pressure (transplanted = 16.5 ± 0.9 mmHg, normal = 16.9 ± 0.9). However, eyes reseeded with eGFP-expressing CrFK cells could not regulate IOP, remaining high and unstable (27.0 ± 6.2 mmHg) instead. Conclusion Tissue-engineered anterior segment scaffolds can serve as readily available, scalable ocular perfusion cultures. This could reduce dependency on scarce donor globes in outflow research and may allow engineering perfusion cultures with specific geno- and phenotypes. KW - ocular anterior segment perfusion culture KW - tissue engineering KW - aqueous humor outflow KW - trabecular meshwork Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-323845 VL - 261 IS - 5 ER - TY - JOUR A1 - Watzling, Martin A1 - Klaus, Lorenz A1 - Weidemeier, Tamara A1 - Horder, Hannes A1 - Ebert, Regina A1 - Blunk, Torsten A1 - Bauer-Kreisel, Petra T1 - Three-dimensional breast cancer model to investigate CCL5/CCR1 expression mediated by direct contact between breast cancer cells and adipose-derived stromal cells or adipocytes JF - Cancers N2 - The tumor microenvironment (TME) in breast cancer is determined by the complex crosstalk of cancer cells with adipose tissue-inherent cells such as adipose-derived stromal cells (ASCs) and adipocytes resulting from the local invasion of tumor cells in the mammary fat pad. This leads to heterotypic cellular contacts between these cell types. To adequately mimic the specific cell-to-cell interaction in an in vivo-like 3D environment, we developed a direct co-culture spheroid model using ASCs or differentiated adipocytes in combination with MDA-MB-231 or MCF-7 breast carcinoma cells. Co-spheroids were generated in a well-defined and reproducible manner in a high-throughput process. We compared the expression of the tumor-promoting chemokine CCL5 and its cognate receptors in these co-spheroids to indirect and direct standard 2D co-cultures. A marked up-regulation of CCL5 and in particular the receptor CCR1 with strict dependence on cell–cell contacts and culture dimensionality was evident. Furthermore, the impact of direct contacts between ASCs and tumor cells and the involvement of CCR1 in promoting tumor cell migration were demonstrated. Overall, these results show the importance of direct 3D co-culture models to better represent the complex tumor–stroma interaction in a tissue-like context. The unveiling of tumor-specific markers that are up-regulated upon direct cell–cell contact with neighboring stromal cells, as demonstrated in the 3D co-culture spheroids, may represent a promising strategy to find new targets for the diagnosis and treatment of invasive breast cancer. KW - 3D breast cancer model KW - adipose-derived stromal cells KW - adipocytes KW - adipose tissue KW - spheroids KW - co-culture Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-362502 SN - 2072-6694 VL - 15 IS - 13 ER - TY - JOUR A1 - Watermann, Christoph A1 - Meyer, Malin Tordis A1 - Wagner, Steffen A1 - Wittekindt, Claus A1 - Klussmann, Jens Peter A1 - Erguen, Sueleyman A1 - Baumgart-Vogt, Eveline A1 - Karnati, Srikanth T1 - Peroxisomes are highly abundant and heterogeneous in human parotid glands JF - International Journal of Molecular Sciences N2 - The parotid gland is one of the major salivary glands producing a serous secretion, and it plays an essential role in the digestive and immune systems. Knowledge of peroxisomes in the human parotid gland is minimal; furthermore, the peroxisomal compartment and its enzyme composition in the different cell types of the human parotid gland have never been subjected to a detailed investigation. Therefore, we performed a comprehensive analysis of peroxisomes in the human parotid gland’s striated duct and acinar cells. We combined biochemical techniques with various light and electron microscopy techniques to determine the localization of parotid secretory proteins and different peroxisomal marker proteins in parotid gland tissue. Moreover, we analyzed the mRNA of numerous gene encoding proteins localized in peroxisomes using real-time quantitative PCR. The results confirm the presence of peroxisomes in all striated duct and acinar cells of the human parotid gland. Immunofluorescence analyses for various peroxisomal proteins showed a higher abundance and more intense staining in striated duct cells compared to acinar cells. Moreover, human parotid glands comprise high quantities of catalase and other antioxidative enzymes in discrete subcellular regions, suggesting their role in protection against oxidative stress. This study provides the first thorough description of parotid peroxisomes in different parotid cell types of healthy human tissue. KW - peroxisomes KW - parotid gland KW - human KW - catalase KW - differential expression KW - PSP KW - mRNA KW - immunofluorescence Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-311079 SN - 1422-0067 VL - 24 IS - 5 ER - TY - JOUR A1 - Wang, Xiaoliang A1 - Liu, Xuan A1 - Xiao, Yun A1 - Mao, Yue A1 - Wang, Nan A1 - Wang, Wei A1 - Wu, Shufan A1 - Song, Xiaoyong A1 - Wang, Dengfeng A1 - Zhong, Xingwang A1 - Zhu, Zhu A1 - Schilling, Klaus A1 - Damaren, Christopher T1 - On-orbit verification of RL-based APC calibrations for micrometre level microwave ranging system JF - Mathematics N2 - Micrometre level ranging accuracy between satellites on-orbit relies on the high-precision calibration of the antenna phase center (APC), which is accomplished through properly designed calibration maneuvers batch estimation algorithms currently. However, the unmodeled perturbations of the space dynamic and sensor-induced uncertainty complicated the situation in reality; ranging accuracy especially deteriorated outside the antenna main-lobe when maneuvers performed. This paper proposes an on-orbit APC calibration method that uses a reinforcement learning (RL) process, aiming to provide the high accuracy ranging datum for onboard instruments with micrometre level. The RL process used here is an improved Temporal Difference advantage actor critic algorithm (TDAAC), which mainly focuses on two neural networks (NN) for critic and actor function. The output of the TDAAC algorithm will autonomously balance the APC calibration maneuvers amplitude and APC-observed sensitivity with an object of maximal APC estimation accuracy. The RL-based APC calibration method proposed here is fully tested in software and on-ground experiments, with an APC calibration accuracy of less than 2 mrad, and the on-orbit maneuver data from 11–12 April 2022, which achieved 1–1.5 mrad calibration accuracy after RL training. The proposed RL-based APC algorithm may extend to prove mass calibration scenes with actions feedback to attitude determination and control system (ADCS), showing flexibility of spacecraft payload applications in the future. KW - reinforcement learning KW - antenna phase center calibration KW - K band ranging (KBR) KW - micrometre level microwave ranging KW - MSC: 49M37 KW - MSC: 65K05 KW - MSC: 90C30 KW - MSC: 90C40 Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-303970 SN - 2227-7390 VL - 11 IS - 4 ER - TY - JOUR A1 - Walther, Rasmus A1 - Krmar, Jovana A1 - Leistner, Adrian A1 - Svrkota, Bojana A1 - Otašević, Biljana A1 - Malenović, Andjelija A1 - Holzgrabe, Ulrike A1 - Protić, Ana T1 - Analytical Quality by Design: achieving robustness of an LC-CAD method for the analysis of non-volatile fatty acids JF - Pharmaceuticals N2 - An alternative to the time-consuming and error-prone pharmacopoeial gas chromatography method for the analysis of fatty acids (FAs) is urgently needed. The objective was therefore to propose a robust liquid chromatography method with charged aerosol detection for the analysis of polysorbate 80 (PS80) and magnesium stearate. FAs with different numbers of carbon atoms in the chain necessitated the use of a gradient method with a Hypersil Gold C\(_{18}\) column and acetonitrile as organic modifier. The risk-based Analytical Quality by Design approach was applied to define the Method Operable Design Region (MODR). Formic acid concentration, initial and final percentages of acetonitrile, gradient elution time, column temperature, and mobile phase flow rate were identified as critical method parameters (CMPs). The initial and final percentages of acetonitrile were fixed while the remaining CMPs were fine-tuned using response surface methodology. Critical method attributes included the baseline separation of adjacent peaks (α-linolenic and myristic acid, and oleic and petroselinic acid) and the retention factor of the last compound eluted, stearic acid. The MODR was calculated by Monte Carlo simulations with a probability equal or greater than 90%. Finally, the column temperature was set at 33 °C, the flow rate was 0.575 mL/min, and acetonitrile linearly increased from 70 to 80% (v/v) within 14.2 min. KW - Analytical Quality by Design KW - fatty acids KW - charged aerosol detector KW - polysorbate 80 KW - magnesium stearate Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-311265 SN - 1424-8247 VL - 16 IS - 4 ER - TY - THES A1 - Walther, Rasmus T1 - Analysis of weakly chromophore impurities by means of liquid chromatography coupled with charged aerosol detection and mass spectrometry T1 - Flüssigchromatographische Untersuchung schwach chromophorer Verunreinigungen mittels Charged Aerosol Detektion und Massenspektrometrie N2 - In all the projects presented, it is evident that the selection of suitable separation conditions is only one side of the coin. Equally crucial in the development of methods for the quality assessment of APIs/drugs is the right detection system. The application of CAD as an alternative to UV detection at low wavelength of the two weak chromophore main degradation products of the very polar, zwitterionic API carbocisteine requires the volatility of the mobile phase. Therefore, as a substitute for the non-volatile ion pairing reagent tetrabutylammonium hydroxide (TBAOH), six different volatile alkylamines as well as a RP/SAX mixed-mode column were evaluated. The best selectivity and separation performance comparable to TBAOH was achieved with the RP/SAX column and a mixture of formic acid and trifluoroacetic acid. For the simultaneous optimisation of the evaporation temperature of the CAD as a function of two chromatographic parameters, a central composite design was chosen and the “desirability function” was subsequently applied for modelling. In addition, column bleeding was investigated with a second RP/SAX column (different batch) with the result that the acetonitrile percentage had to be adjusted and preconditioning by injection of concentrated samples is essential. The final mixed-mode method was finally validated with both columns according to the ICH Q2 (R1) guideline. Based on this, an MS-compatible method was developed with little effort using an identical RP/SAX column in UPLC dimension for the untargeted analysis by HRMS of two carbocisteine-containing prototype syrup formulations. For a comprehensive characterisation, HRMS and MS/HRMS data were recorded simultaneously by information dependent acquisition mode. Based on the exact masses, isotope patterns and an in silico plausibility check of the fragment spectra, the prediction of the structures of the unknown impurities was possible. In both syrup samples, which had been stored for nine months at 40 °C and 75 % r.h., two additional impurities of carbocisteine (i.e. lactam of the sulfoxides and disulphide between cysteine and thioglycolic acid) were identified by comparison with the corresponding prototype placebo samples using general unknown comparative screening. In addition, the formation of Maillard products by binary mixtures with 13C-labelled sugars was revealed in the sucrose-containing formulation. For the promising hyphenation of the UV detector with the CAD for the simultaneous detection of all UV-active impurities of the cholesterol-lowering drug simvastatin and the only weak chromophore dihydrosimvastatin, the Ph. Eur. method had to be adapted. Besides replacing phosphoric acid with trifluoroacetic acid, the gradient also had to be adjusted and a third critical peak pair was observed. Based on validation experiments (according to the ICH Q2 (R1) guideline), the suitability of the CAD for sensitive detection (LOQ = 0.0175 % m/m) was proven.  To further investigate the robustness of the adapted method and CAD, a Plackett-Burman design was chosen. None of the factors had a statistically significant effect on the S/N of the CAD in the ranges tested. Regarding the three critical peak pairs, on the other hand, the factors to be controlled were statistically established, so that a targeted correction is possible if the system suitability test is not passed. The idea of employing a hyphenated UV-CAD system was finally applied to the structurally closely related lovastatin and its specified impurity dihydrolovastatin. Here, the CAD showed a significantly better S/N compared to the compendial UV detection at 200 nm. The suitability of CAD for the analysis of non-volatile fatty acids in polysorbate 80 (PS80) as favourable alternative to the Ph. Eur. GC method (no time-consuming, error-prone and toxic derivatisation) has already been demonstrated. The aim of this project was therefore to develop a robust method with a focus on the AQbD principles, which can be used for the analysis of other excipients with similar fatty acid composition. After the definition of the analytical target profile and a risk assessment by means of an Ishikawa diagram, a suitable C18 column and the chromatographic framework conditions (formic acid concentration and initial/final gradient conditions) were selected after only few preliminary runs. The remaining critical method parameters were then investigated with the help of DoE and RSM. Using the obtained model equations, Monte Carlo simulations were performed to create the method operable design region as a region of theoretical robustness. After validation according to ICH Q2 (R1), the fatty acid composition of a magnesium stearate batch was successfully analysed as a further application example in addition to PS80. The CAD was able to prove its potential in all the issues investigated in the context of this doctoral thesis. As a cost-effective alternative compared to MS instruments, it thus closes a gap in the quality assessment of APIs or excipients without a suitable chromophore. The easy method transfer to (HR)MS instruments also allows for a unique degree of sample characterisation through untargeted approaches in case of new impurities. For resource- and time-efficient work, the possibilities and limitations of software tools for method development and data evaluation as well as the application of risk-based approaches such as AQbD should also be considered. N2 - In allen vorgestellten Projekten wird deutlich, dass die Auswahl geeigneter Trennbedingungen nur eine Seite der Medaille darstellen. Ebenso entscheiden bei der Entwicklung von Methoden zur Qualitätsbeurteilung von Wirkstoffen und Arzneimitteln ist das richtige Detektionssystem. Die Verwendung des CAD als Alternative zur UV-Detektion bei niedriger Wellenlänge der beiden schwach chromophoren Hauptabbauprodukte des sehr polaren, zwitterionischen Wirkstoffs Carbocystein erfordert die Flüchtigkeit der mobilen Phase. Daher wurden als Ersatz für das nichtflüchtige Ionenpaarreagenz Tetrabutylammoniumhydroxid (TBAOH) sechs verschiedene flüchtige Alkylamine sowie eine RP/SAX Mixed-Mode-Säule untersucht. Die Beste mit TBAOH vergleichbare Selektivität und Trennleistung wurde mit der RP/SAX-Säule und einer Mischung aus Ameisensäure und Trifluoressigsäure erreicht. Für die gleichzeitige Optimierung der Verdampfungstemperatur des CAD in Abhängigkeit von zwei chromatographischen Parametern wurde ein zentral zusammengesetztes Versuchsdesign gewählt und anschließend die desirability function zur Modellierung eingesetzt. Darüber hinaus wurde das Säulenbluten mit einer zweiten RP/SAX-Säule (einer anderen Charge) untersucht, mit dem Ergebnis, dass der Acetonitrilanteil angepasst werden musste und eine Vorkonditionierung durch Injektion konzentrierter Proben unerlässlich ist. Die endgültige Mixed-Mode-Methode wurde schließlich mit beiden Säulen gemäß der ICH-Richtlinie Q2 (R1) validiert. Darauf aufbauend konnte mit geringem Aufwand ein MS-kompatibles Methode mit einer identischen RP/SAX-Säule in UPLC-Dimension für die ungezielte HRMS-Analyse von zwei Carbocystein-haltigen Sirup-Prototypformulierungen entwickelt werden. Für eine umfassende Charakterisierung wurden HRMS- und MS/HRMS-Daten gleichzeitig im information dependent analysis-Modus aufgenommen. Anhand der exakten Massen, Isotopenmuster und In-silico-Plausibilitätsprüfung der Fragmentspektren war die Vorhersage der Strukturen der unbekannten Verunreinigungen möglich. In den beiden Sirupproben, die neun Monate lang bei 40 °C und 75 % r.F. gelagert worden waren, wurden zwei zusätzliche Verunreinigungen von Carbocystein (sprich das Lactam der Sulfoxide und das Disulfid zwischen Cystein und Thioglykolsäure) durch Vergleich mit den entsprechenden Prototyp-Placeboproben mittels general unknown comparative screening identifiziert. Darüber hinaus wurde die Bildung von Maillard-Produkten durch binäre Mischungen mit 13C-markierten Zuckern in der Saccharose-haltigen Formulierung bestätigt. Für die vielversprechende Kopplung des UV-Detektors mit dem CAD zum gleichzeitigen Nachweis aller UV-aktiven Verunreinigungen des Cholesterinsenkers Simvastatin und des nur schwach chromophoren Dihydrosimvastatins musste die Ph. Eur.-Methode angepasst werden.  Neben dem Austausch von Phosphorsäure durch Trifluoressigsäure musste auch der Gradient geändert werden, und es wurde ein drittes kritisches Peakpaar beobachtet. Anhand von Validierungsexperimenten (gemäß der ICH Q2 (R1) Richtlinie) wurde die Eignung des CAD für einen empfindlichen Nachweis (LOQ = 0.0175 % m/m) bewiesen. Um die Robustheit der angepassten Methode und des CAD näher zu untersuchen, wurde ein Plackett-Burman-Design gewählt. Keiner der Faktoren hatte einen statistisch signifikanten Einfluss auf das S/N des CAD in den getesteten Bereichen. Für die drei kritischen Peakpaare hingegen wurden die zu kontrollierenden Faktoren statistisch ermittelt, sodass eine gezielte Korrektur möglich ist, wenn der Systemeignungstest nicht bestanden wird. Die Idee der Verwendung eines kombinierten UV-CAD-Systems wurde schließlich auf das strukturell eng verwandte Lovastatin und dessen spezifizierte Verunreinigung Dihydrolovastatin angewendet. Hier zeigte der CAD ein deutlich besseres S/N im Vergleich zur kompendialen UV-Detektion bei 200 nm. Die Eignung von CAD für die Analyse von nichtflüchtigen Fettsäuren in Polysorbat 80 (PS80) als vorteilhafte Alternative zur GC-Methode im Ph. Eur. (keine zeitaufwändige, fehleranfällige und toxische Derivatisierung) wurde bereits gezeigt. Ziel dieses Projekts war es daher, eine robuste Methode zu entwickeln, die sich an den Prinzipien des AQbD orientiert und auch für die Analyse weiterer Hilfsstoffe mit ähnlicher Fettsäurezusammensetzung eingesetzt werden kann. Nach der Definition des analytical target profiles und einer Risikobewertung mit einem Ishikawa-Diagramms wurden nach nur wenigen Vorversuchen eine geeignete C18-Säule und die chromatographischen Rahmenbedingungen (Ameisensäurekonzentration und Anfangs-/Endbedingungen des Gradienten) ausgewählt. Die übrigen kritischen Methodenparameter wurden dann mit Hilfe von DoE und RSM untersucht. Unter Verwendung der erhaltenen Modellgleichungen wurden Monte-Carlo-Simulationen durchgeführt, um die Method Operable Design Region als Zone der theoretischen Robustheit zu erstellen. Nach der Validierung gemäß ICH Q2 (R1) wurde als weiteres Anwendungsbeispiel neben PS80 auch die Fettsäurezusammensetzung einer Magnesiumstearat-Charge erfolgreich analysiert. Das CAD konnte sein Potential in allen im Rahmen dieser Dissertation untersuchten Fragestellungen unter Beweis stellen. Als kostengünstige Alternative zu MS-Geräten schließt es damit eine Lücke bei der Qualitätsbewertung von Wirk- oder Hilfsstoffen ohne geeignetes Chromophor. Der einfache Methodentransfer auf (HR)MS-Instrumente ermöglicht zudem einen einzigartigen Grad der Probencharakterisierung durch ungezielte Ansätze im Falle neuer Verunreinigungen. Für ein ressourcen- und zeiteffizientes Arbeiten sollten zudem die Möglichkeiten und Grenzen von Softwaretools für die Methodenentwicklung und Datenauswertung sowie die Anwendung risikobasierter Ansätze wie AQbD bedacht werden. KW - Carbocistein KW - Statine KW - High-performance liquid chromatography KW - Charged aerosol detection KW - Weakly chromophore impurities Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-321862 ER - TY - JOUR A1 - Wagner, N. A1 - Crippa, L. A1 - Amaricci, A. A1 - Hansmann, P. A1 - Klett, M. A1 - König, E. J. A1 - Schäfer, T. A1 - Di Sante, D. A1 - Cano, J. A1 - Millis, A. J. A1 - Georges, A. A1 - Sangiovanni, G. T1 - Mott insulators with boundary zeros JF - Nature Communications N2 - The topological classification of electronic band structures is based on symmetry properties of Bloch eigenstates of single-particle Hamiltonians. In parallel, topological field theory has opened the doors to the formulation and characterization of non-trivial phases of matter driven by strong electron-electron interaction. Even though important examples of topological Mott insulators have been constructed, the relevance of the underlying non-interacting band topology to the physics of the Mott phase has remained unexplored. Here, we show that the momentum structure of the Green’s function zeros defining the “Luttinger surface" provides a topological characterization of the Mott phase related, in the simplest description, to the one of the single-particle electronic dispersion. Considerations on the zeros lead to the prediction of new phenomena: a topological Mott insulator with an inverted gap for the bulk zeros must possess gapless zeros at the boundary, which behave as a form of “topological antimatter” annihilating conventional edge states. Placing band and Mott topological insulators in contact produces distinctive observable signatures at the interface, revealing the otherwise spectroscopically elusive Green’s function zeros. KW - electronic properties and materials KW - topological insulators Y1 - 2023 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-358150 VL - 14 ER -