@phdthesis{Bozkaya2023, author = {Bozkaya, Beg{\"u}m}, title = {Influence of Carbon Additives on the Electrochemical Performance of Modern Lead-Acid Batteries}, doi = {10.25972/OPUS-31917}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-319174}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2023}, abstract = {In the first part of this thesis, a validation of both short-term and long-term DCA tests on 2 V laboratory cells is focussed. The aim is to improve the laboratory cell level measurement technology for dynamic charge acceptance regarding the investigation of carbon additives. To address this issue, it is crucial to apply carbon additives generating a remarkable difference in charge acceptance. For this purpose, five different carbon additives providing a variation in the specific external surface were included as additives in the negative plates of 2 V lead-acid cells. Both short-term (charge acceptance test 2 from SBA and DCA from EN) and long-term (Run-in DCA from Ford) DCA tests were executed on the lead-acid cells. Further understanding of the mechanism was studied by applying electrochemical methods like cyclic voltammetry and electrochemical impedance spectroscopy. The second part of this thesis aims to understand the impact of carbon surface functional groups on the electrochemical activity of the negative electrodes as well as the DCA of 2 V lead-acid cells. In order to address this topic, commercially available activated carbon was modified by different chemical treatments to incorporate specific surface functional groups in the carbon structure. A series of activated carbons having a broad range of pH was prepared, which were used as additives in the negative electrodes. The corresponding lead-acid cells were subjected to cyclic voltammetry and DCA test according to EN. Further, the physical and chemical properties of the functionalized carbon additives were intensively analyzed to establish a structure-property relationship with a focus on DCA.}, subject = {Bleiakkumulator}, language = {en} } @phdthesis{Bauer2023, author = {Bauer, Christian}, title = {Towards ecological and efficient electrochemical energy storage in supercapacitors and sodium ion batteries using onion-like carbon}, doi = {10.25972/OPUS-31795}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-317956}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2023}, abstract = {In this thesis, the usage of onion-like carbon (OLC) for energy storage applications was researched regarding sustainability, performance and processability. This work targets to increase the scientific understanding regarding the role of OLC in electrodes and to facilitate a large-scale production, which is the foundation for commercial application. Research was devoted to increase the knowledge in the particular field, to yield synergistic approaches and a shared value regarding sustainability and performance.}, subject = {Elektrochemie}, language = {en} } @phdthesis{Shityakov2011, author = {Shityakov, Sergey}, title = {Molecular modelling and simulation of retroviral proteins and nanobiocomposites}, url = {http://nbn-resolving.de/urn:nbn:de:bvb:20-opus-56960}, school = {Universit{\"a}t W{\"u}rzburg}, year = {2011}, abstract = {Molecular modelling and simulation are powerful methods in providing important in-formation on different biological systems to elucidate their structural and functional proper-ties, which cannot be determined in experiment. These methods are applied to analyse versa-tile biological systems: lipid membrane bilayers stabilized by an intercalated single wall carbon nanotube and retroviral proteins such as HIV protease and integrase. HIV-1 integrase has nuclear localization signals (NLS) which play a crucial role in nuclear import of viral preintegration complex (PIC). However, the detailed mechanisms of PIC formation and its nuclear transport are not known. Previously it was shown that NLSs bind to the cell transport machinery e.g. proteins of nuclear pore complex such as transportins. I investigated the interaction of this viral protein HIV-1 integrase with proteins of the nuclear pore complex such as transportin-SR2 (Shityakov et al., 2010). I showed that the transportin-SR2 in nuclear import is required due to its interaction with the HIV-1 integrase. I analyzed key domain interaction, and hydrogen bond formation in transportin-SR2. These results were discussed in comparison to other retroviral species such as foamy viruses to better understand this specific and efficient retroviral trafficking route. The retroviral nuclear import was next analyzed in experiments regarding the retroviral ability to infect nondividing cells. To accomplish the gene transfer task successfully, ret-roviruses must efficiently transduce different cell cultures at different phases of cell cycle. However, promising and safe foamy viral vectors used for gene transfer are unable to effi-ciently infect quiescent cells. This drawback was due to their inability to create a preintegra-tion complex (PIC) for nuclear import of retroviral DNA. On the contrary, the lentiviral vec-tors are not dependant on cell cycle. In the course of reverse transcription the polypurine tract (PPT) is believed to be crucial for PIC formation. In this thesis, I compared the transduction frequencies of PPT modified FV vectors with lentiviral vectors in nondividing and dividing alveolar basal epithelial cells from human adenocarcinoma (A549) by using molecular cloning, transfection and transduction techniques and several other methods. In contrast to lentiviral vectors, FV vectors were not able to effi-ciently transduce nondividing cell (Shityakov and Rethwilm, unpublished data). Despite the findings, which support the use of FV vectors as a safe and efficient alternative to lentiviral vectors, major limitation in terms of foamy-based retroviral vector gene transfer in quiescent cells still remains. Many attempts have been made recently to search for the potential molecules as pos-sible drug candidates to treat HIV infection for over decades now. These molecules can be retrieved from chemical libraries or can be designed on a computer screen and then synthe-sized in a laboratory. Most notably, one could use the computerized structure as a reference to determine the types of molecules that might block the enzyme. Such structure-based drug design strategies have the potential to save off years and millions of dollars compared to a more traditional trial-and-error drug development process. After the crystal structure of the HIV-encoded protease enzyme had been elucidated, computer-aided drug design played a pivotal role in the development of new compounds that inhibit this enzyme which is responsible for HIV maturation and infectivity. Promising repre-sentatives of these compounds have recently found their way to patients. Protease inhibitors show a powerful sustained suppression of HIV-1 replication, especially when used in combi-nation therapy regimens. However, these drugs are becoming less effective to more resistant HIV strains due to multiple mutations in the retroviral proteases. In computational drug design I used molecular modelling methods such as lead ex-pansion algorithm (TriposĀ®) to create a virtual library of compounds with different binding affinities to protease binding site. In addition, I heavily applied computer assisted combinato-rial chemistry approaches to design and optimize virtual libraries of protease inhibitors and performed in silico screening and pharmacophore-similarity scoring of these drug candidates. Further computational analyses revealed one unique compound with different protease bind-ing ability from the initial hit and its role for possible new class of protease inhibitors is dis-cussed (Shityakov and Dandekar, 2009). A number of atomistic models were developed to elucidate the nanotube behaviour in lipid bilayers. However, none of them provided useful information for CNT effect upon the lipid membrane bilayer for implementing all-atom models that will allow us to calculate the deviations of lipid molecules from CNT with atomistic precision. Unfortunately, the direct experimental investigation of nanotube behaviour in lipid bilayer remains quite a tricky prob-lem opening the door before the molecular simulation techniques. In this regard, more de-tailed multi-scale simulations are needed to clearly understand the stabilization characteristics of CNTs in hydrophobic environment. The phenomenon of an intercalated single-wall carbon nanotube in the center of lipid membrane was extensively studied and analyzed. The root mean square deviation and root mean square fluctuation functions were calculated in order to measure stability of lipid mem-branes. The results indicated that an intercalated carbon nanotube restrains the conformational freedom of adjacent lipids and hence has an impact on the membrane stabilization dynamics (Shityakov and Dandekar, 2011). On the other hand, different lipid membranes may have dissimilarities due to the differing abilities to create a bridge formation between the adherent lipid molecules. The results derived from this thesis will help to develop stable nanobiocom-posites for construction of novel biomaterials and delivery of various biomolecules for medi-cine and biology.}, subject = {Kohlenstoff}, language = {en} }