Global ETD Search

1	MODIFICATION OF VESICULAR STOMATITIS VIRUS G PROTEIN FOR TARGETED GENE DELIVERY INTO PSCA-POSITIVE TUMOR CELLS Günes, Serap 26 June 2007 (has links) (PDF) Gene therapy is a promising treatment option for cancer. Ideally, a therapeutic gene is delivered specifically into tumor cells sparing the neighboring normal cells. For this purpose gene delivery vectors are designed that can recognize structures, which are exclusively expressed on tumor cells (i.e. the tumor-associated antigens -TAA-). Retroviral vectors are commonly used for gene therapy by modifying the envelope protein responsible for the recognition of the target cell. The Vesicular Stomatitis Virus G protein (VSV-G) is a well-liked choice for pseudotyping the retroviral vectors since it confers on the viral particle stability to allow concentration to high titers necessary for the clinical applications. However, the main drawback of VSV-G, the ubiquitously expressed receptor and thus the broad target range, hinders the use of this protein for targeted gene therapy. In this thesis, we aimed to modify the VSV-G for targeted gene therapy against Prostate Stem Cell Antigen (PSCA) -expressing tumors. Therefore we followed two approaches. The first approach comprised of the fusion of a single-chain antibody fragment against PSCA to the N-terminus of VSV-G. In the second approach the VSV-G was modified by insertion of a small epitope. We could demonstrate that two positions in the N-terminal region of VSV-G protein permit insertion of a ten amino acid long epitope. These mutant VSV-G proteins were successfully assembled into retroviral particles. We demonstrated that the mutant retroviral particles can be used for targeting to PSCA-positive cells using nanobeads. The nanobeads were chemically coupled to antibodies against the epitope in the VSV-G protein and PSCA on the tumor cell. These bispecific nanobeads allowed the recruitment of mutant retroviral particles to the PSCApositive cells. Our results point out the potential of these mutant retroviral particles in targeted gene delivery. Further studies will be necessary to assess the efficiency of in vivo targeted gene therapy using these mutant retroviral particles. Vesicular Stomatitis Virus G protein gene therapy viral vectors Vesicular-Stomatitis-Virus G Protein Gentherapie Virale Vektoren ddc:570 rvk:WG 7400
2	MODIFICATION OF VESICULAR STOMATITIS VIRUS G PROTEIN FOR TARGETED GENE DELIVERY INTO PSCA-POSITIVE TUMOR CELLS Günes, Serap 21 June 2007 (has links) Gene therapy is a promising treatment option for cancer. Ideally, a therapeutic gene is delivered specifically into tumor cells sparing the neighboring normal cells. For this purpose gene delivery vectors are designed that can recognize structures, which are exclusively expressed on tumor cells (i.e. the tumor-associated antigens -TAA-). Retroviral vectors are commonly used for gene therapy by modifying the envelope protein responsible for the recognition of the target cell. The Vesicular Stomatitis Virus G protein (VSV-G) is a well-liked choice for pseudotyping the retroviral vectors since it confers on the viral particle stability to allow concentration to high titers necessary for the clinical applications. However, the main drawback of VSV-G, the ubiquitously expressed receptor and thus the broad target range, hinders the use of this protein for targeted gene therapy. In this thesis, we aimed to modify the VSV-G for targeted gene therapy against Prostate Stem Cell Antigen (PSCA) -expressing tumors. Therefore we followed two approaches. The first approach comprised of the fusion of a single-chain antibody fragment against PSCA to the N-terminus of VSV-G. In the second approach the VSV-G was modified by insertion of a small epitope. We could demonstrate that two positions in the N-terminal region of VSV-G protein permit insertion of a ten amino acid long epitope. These mutant VSV-G proteins were successfully assembled into retroviral particles. We demonstrated that the mutant retroviral particles can be used for targeting to PSCA-positive cells using nanobeads. The nanobeads were chemically coupled to antibodies against the epitope in the VSV-G protein and PSCA on the tumor cell. These bispecific nanobeads allowed the recruitment of mutant retroviral particles to the PSCApositive cells. Our results point out the potential of these mutant retroviral particles in targeted gene delivery. Further studies will be necessary to assess the efficiency of in vivo targeted gene therapy using these mutant retroviral particles. info:eu-repo/classification/ddc/570 ddc:570
3	Die OCT-gestützte Analyse des vitreoretinalen Interfaces zur Evaluierung neuer prädiktiver Faktoren für eine erfolgreiche enzymatische Vitreolyse im Rahmen der intravitrealen Ocriplasmin-Therapie / The OCT-based analysis of the vitreoretinal interface for the evaluation of new predictive factors for a successful enzymatic vitreolysis in the context of intravitreal ocriplasmin therapy Krug, Pia Selly Elisabeth 31 December 1100 (has links) No description available. 610 vitreomakuläres Traktionssyndrom Ocriplasmin prädiktive Faktoren Durchmesser 2D-Fläche 3D-Fläche Vektoren vitreomacular traction ocriplasmin predictive factors diameter 2D-surface 3D-surface vectors GOK-MEDIZIN
4	Anti-inflammatorische und zytoprotektive Gentherapie am Beispiel der experimentellen Transplantation Ritter, Thomas 10 January 2003 (has links) Ziel der Arbeit war, zu untersuchen, ob der gezielte Einsatz gentherapeutischer Methoden zu einer Verhinderung der Abstoßung allogener Transplantate bzw. zu einer Verhinderung der Induktion des Ischämie-/Reperfusionsschadens in verschiedenen Transplantationsmodellen der Ratte beitragen kann. Dabei wurden zwei Schwerpunkte gesetzt: Zum einen wurde auf den ex-vivo Gentransfer von therapeutischen Molekülen direkt in das Transplantat mit Hilfe von rekombinanten Adenoviren fokussiert. Zum anderen wurde das Potenzial von retroviral modifizierten, allospezifischen T-Zellen als Träger therapeutischer Gene zur Verhinderung der Transplantatrejektion untersucht. Diese Habilitationsschrift umfasst dreizehn Originalartikel in internationalen Zeitschriften, sechs Übersichtsartikel (Reviews) und vier Manuskripte, die bereits zur Veröffentlichung eingereicht sind. / The aim of the research was to investigate, whether the specific use of gene therapeutic methods can play a role in the prevention of allogeneic graft rejection or in the prevention of the induction of ischemia/reperfusion damage in various rat transplantation models. Doing this there were to main focusses: First we concentrated on the ex-vivo gene transfer of therapeutic molecules directly into the graft, which was done using recombinant adenoviruses. Then we investigated the potential of retrovirally modified, allospecific T-cells as carriers for therapeutic genes for the prevention of graft rejection. This publication consists of thirteen original papers in international journals, six reviews and four manuscripts that have been submitted for publication. Gentherapie virale Vektoren Experimentelle Transplantation Ischämie-/Reperfusionssschaden regulatorische T Zellen gene therapy viral vectors experimental transplantation ischemia-/reperfusion injury regulatory T cells 610 Medizin 33 Medizin WG 7400 ddc:610
5	Hydrodynamische Lyapunov-Moden in mehrkomponentigen Lennard-Jones-Flüssigkeiten Drobniewski, Christian 22 March 2011 (has links) (PDF) Die Charakterisierung hochdimensionaler Systeme mit Lyapunov-Instabilität wird durch das Lyapunov-Spektrum und die zugehörigen Lyapunov-Vektoren ermöglicht. Für eine Vielzahl von derartigen Systemen (Coupled-Map-Lattices, Hartkugel-Systeme, Systeme mit ausgedehnten Potentialen ...) konnte durch die Untersuchung der Lyapunov-Vektoren die Existenz von hydrodynamischen Lyapunov-Moden nachgewiesen werden. Diese kollektiven Anregungen zeigen sich in Lyapunov-Vektoren, deren Lyapunov-Exponenten dem Betrage nach am kleinsten sind. Da Lyapunov-Exponenten charakteristische Zeitskalen innerhalb der Systeme repräsentieren, ist durch die Lyapunov-Moden eine Untersuchung des Langzeitverhaltens möglich. In dieser Arbeit werden die hydrodynamischen Lyapunov-Moden durch Molekulardynamiksimulationen von mehrkomponentigen Lennard-Jones-Flüssigkeiten untersucht. Die Charakterisierung der Lyapunov-Moden zeigt im weiteren eine Ähnlichkeit zu Dispersionsrelationen von Phononen. Molekulardynamik Lennard-Jones-Flüssigkeit Lyapunov-Exponent Lyapunov-Vektoren Hydrodynamische Lyapunov-Moden Molecular dynamic Lyapunov Analysis Lennard Jones Fluid ddc:539 ddc:532 Molekulardynamik Ljapunov-Exponent Lennard-Jones-Potenzial
6	Non-regenerative Two-Hop Wiretap Channels using Interference Neutralization Gerbracht, Sabrina, Jorswieck, Eduard A., Zheng, Gan, Ottersten, Björn 23 May 2013 (has links) (PDF) In this paper, we analyze the achievable secrecy rates in the two-hop wiretap channel with four nodes, where the transmitter and the receiver have multiple antennas while the relay and the eavesdropper have only a single antenna each. The relay is operating in amplify-and-forward mode and all the channels between the nodes are known perfectly by the transmitter. We discuss different transmission and protection schemes like artificial noise (AN). Furthermore, we introduce interference neutralization (IN) as a new protection scheme. We compare the different schemes regarding the high-SNR slope and the high-SNR power offset and illustrate the performance by simulation results. It is shown analytically as well as by numerical simulations that the high SNR performance of the proposed IN scheme is better than the one of AN. Array-Signalverarbeitung Interferenz Receiver Relais Signal-Rausch-Verhältnis Transmitter Vektoren Sonderforschungsbereich 912 Hochadaptive Energieeffiziente Systeme Array signal processing Interference Receivers Relays Signal to noise ratio Transmitters Vectors Collaborative Research Centre 912 ddc:621.3 ddc:620 rvk:ZN 6560 rvk:ZN 6010
7	Communications with 1-Bit Quantization and Oversampling at the Receiver: Benefiting from Inter-Symbol-Interference Krone, Stefan, Fettweis, Gerhard 25 January 2013 (has links) (PDF) 1-bit analog-to-digital conversion is very attractive for low-complexity communications receivers. A major drawback is, however, the small spectral efficiency when sampling at symbol rate. This can be improved through oversampling by exploiting the signal distortion caused by the transmission channel. This paper analyzes the achievable data rate of band-limited communications channels that are subject to additive noise and inter-symbol-interference with 1-bit quantization and oversampling at the receiver. It is shown that not only the channel noise but also the inter-symbol-interference can be exploited to benefit from oversampling. AWGN-Kanäle Transinformation Quantisierung Receiver Signal-Rausch-Verhältnis Vektoren Sonderforschungsbereich 912 HAEC Hochadaptive Energieeffiziente Systeme AWGN channels Mutual information Quantization Receivers Signal to noise ratio Vectors Collaborative Research Centre 912 ddc:620 ddc:621.3 rvk:ZN 6100
8	Hydrodynamische Lyapunov-Moden in mehrkomponentigen Lennard-Jones-Flüssigkeiten Drobniewski, Christian 22 June 2010 (has links) Die Charakterisierung hochdimensionaler Systeme mit Lyapunov-Instabilität wird durch das Lyapunov-Spektrum und die zugehörigen Lyapunov-Vektoren ermöglicht. Für eine Vielzahl von derartigen Systemen (Coupled-Map-Lattices, Hartkugel-Systeme, Systeme mit ausgedehnten Potentialen ...) konnte durch die Untersuchung der Lyapunov-Vektoren die Existenz von hydrodynamischen Lyapunov-Moden nachgewiesen werden. Diese kollektiven Anregungen zeigen sich in Lyapunov-Vektoren, deren Lyapunov-Exponenten dem Betrage nach am kleinsten sind. Da Lyapunov-Exponenten charakteristische Zeitskalen innerhalb der Systeme repräsentieren, ist durch die Lyapunov-Moden eine Untersuchung des Langzeitverhaltens möglich. In dieser Arbeit werden die hydrodynamischen Lyapunov-Moden durch Molekulardynamiksimulationen von mehrkomponentigen Lennard-Jones-Flüssigkeiten untersucht. Die Charakterisierung der Lyapunov-Moden zeigt im weiteren eine Ähnlichkeit zu Dispersionsrelationen von Phononen. info:eu-repo/classification/ddc/539 ddc:539 info:eu-repo/classification/ddc/532 ddc:532
9	Communications with 1-Bit Quantization and Oversampling at the Receiver: Benefiting from Inter-Symbol-Interference Krone, Stefan, Fettweis, Gerhard January 2012 (has links) 1-bit analog-to-digital conversion is very attractive for low-complexity communications receivers. A major drawback is, however, the small spectral efficiency when sampling at symbol rate. This can be improved through oversampling by exploiting the signal distortion caused by the transmission channel. This paper analyzes the achievable data rate of band-limited communications channels that are subject to additive noise and inter-symbol-interference with 1-bit quantization and oversampling at the receiver. It is shown that not only the channel noise but also the inter-symbol-interference can be exploited to benefit from oversampling. info:eu-repo/classification/ddc/620 ddc:620 info:eu-repo/classification/ddc/621.3 ddc:621.3
10	Non-regenerative Two-Hop Wiretap Channels using Interference Neutralization Gerbracht, Sabrina, Jorswieck, Eduard A., Zheng, Gan, Ottersten, Björn January 2012 (has links) In this paper, we analyze the achievable secrecy rates in the two-hop wiretap channel with four nodes, where the transmitter and the receiver have multiple antennas while the relay and the eavesdropper have only a single antenna each. The relay is operating in amplify-and-forward mode and all the channels between the nodes are known perfectly by the transmitter. We discuss different transmission and protection schemes like artificial noise (AN). Furthermore, we introduce interference neutralization (IN) as a new protection scheme. We compare the different schemes regarding the high-SNR slope and the high-SNR power offset and illustrate the performance by simulation results. It is shown analytically as well as by numerical simulations that the high SNR performance of the proposed IN scheme is better than the one of AN. info:eu-repo/classification/ddc/621.3 ddc:621.3 info:eu-repo/classification/ddc/620 ddc:620

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