Dissertations / Theses on the topic 'Protein electroporation'
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Chen, Zhiqiang. "NANOMETER-SCALE MEMBRANE ELECTRODE SYSTEMS FOR ACTIVE PROTEIN SEPARATION, ENZYME IMMOBILIZATION AND CELLULAR ELECTROPORATION." UKnowledge, 2014. http://uknowledge.uky.edu/cme_etds/33.
Full textSchmotzer, Carolyn Anne. "Assessment of Murine Embryo Development Following Electroporation and Microinjection of a Green Fluorescent Protein DNA Construct." Thesis, Virginia Tech, 2001. http://hdl.handle.net/10919/34369.
Full textMaster of Science
Kawai, Mariko. "Ectopic bone formation by human bone morphogenetic protein-2 gene transfer to skeletal muscle using transcutaneous electroporation." Kyoto University, 2004. http://hdl.handle.net/2433/147446.
Full textMcCray, Andrea Nicole. "Electrogenetherapy of established B16 murine melanoma by using an expression plasmid for HIV-1 viral protein R." [Tampa, Fla] : University of South Florida, 2006. http://purl.fcla.edu/usf/dc/et/SFE0001758.
Full textHua, Ethan Wei. "Maturation of single retinogeniculate projections visualized by in vivo electroporation of fluorescent proteins." Diss., Connect to a 24 p. preview or request complete full text in PDF format. Access restricted to UC campuses, 2008. http://wwwlib.umi.com/cr/ucsd/fullcit?p1459290.
Full textTitle from first page of PDF file (viewed Nov. 10, 2008). Available via ProQuest Digital Dissertations. Includes bibliographical references.
Figueiredo, Lilybeth de Andrade. "Vacinas, novas perspectivas." Master's thesis, [s.n.], 2014. http://hdl.handle.net/10284/4876.
Full textAs vacinas são uma das maiores descobertas da medicina moderna e têm contribuído para salvar a vida de milhares de milhões de pessoas em cooperação com outras medidas de saúde pública (ao nível do saneamento básico, antibióticos, etc.). As vacinas tiveram um forte impacto no combate a muitas doenças, tendo sido a erradicação da varíola uma das maiores conquistas. No entanto, esta área enfrenta ainda desafios complexos, como são os casos do HIV, tuberculose e malária. Os benefícios das vacinas são elevados quando as mesmas são usadas amplamente, no entanto, os custos de produção, distribuição e preservação são elevados sendo dos principais problemas para os países em desenvolvimento, constituindo desta forma um dos principais obstáculos para alcançar uma cobertura vacinal global. Estas limitações levam à necessidade de torná-las mais eficazes, seguras, de produção mais rápida e eficientes, procurando evitar alguns dos seus maiores problemas como a refrigeração, doses múltiplas e injecções intramusculares. Nas últimas décadas foram pesquisadas e estudadas exaustivamente novas tecnologias associadas às vacinas, assim como, foram optimizadas novas formas de administrar e de apresentar os antigénios aos diversos componentes do sistema imunitário. Estas tecnologias incluem mecanismos de produção em que vacinas produzidas em culturas de células são mais rentáveis em comparação com as vacinas que recorrem a ovos. No entanto têm sido implementadas novas estratégias com o objectivo de aumentar a eficácia das vacinas, têm sido implementadas, como é o caso dos adjuvantes, da eletroporação, das vias de imunização e do prime-boost. Finalmente, tem-se tentado encontrar formas diferentes de activar o sistema imunitário através de; vacinas baseadas em proteínas recombinantes; vacinas de DNA; partículas semelhantes a vírus; vacinas universais; vacinas baseadas em vectores virais e vacinas baseadas em péptidos. Nesta área estão constantemente a surgir novas tecnologias de vacinas mais seguras eficazes e de baixo custo. Apesar de algumas estarem ainda em fase experimental, existe um enorme potencial para o surgimento de novas vacinas num futuro próximo, com produção em larga escala, mais eficazes e seguras. Vaccines are one of the greatest discoveries of modern medicine, they have saved the lives of billions of people in cooperation with other public health measures (sanitation, antibiotics, etc.). The vaccines had an impact in reducing many diseases, being the eradication of smallpox one of it's greatest achievements. However this area still faces difficult challenges, such as HIV, tuberculosis and malaria. The benefits of vaccines are high when used widely, however, the costs of manufacturing, distribution and preservation of vaccines are costly and major impediments to developing countries themselves, and represents a major obstacle to achieving global immunization coverage. These limitations lead to the need of improving vaccines to be more effective, safer, faster and more efficient production thus avoiding some of their biggest problems, such as refrigeration, multiple doses and intramuscular injections. In recent decades there have been exhaustively studied and researched new technologies associated with vaccines, as well as new forms were optimised to manage and present the antigens to the various components of the immune system. These technologies include mechanisms that vaccines produced in cell culture are more cost effective in comparison with the vaccine produced in eggs. Strategies for the purpose of increasing the effectiveness of vaccines such as adjuvants, electroporation, routes of immunisation, and the prime-boost. Finally, find different ways to activate the immune system such as vaccines based on recombinant proteins; DNA vaccines; virus-like particles; universal vaccines; vaccines based on viral vectors and vaccines based on peptide. In this area, there are constantly arising new technologies of safer vaccines,effective and inexpensive. Although some of the technologies are still in experimental stages, there is huge potential for the emergence of new vaccines, with large-scale production, effective and safe in the near future.
Grognot, Marianne. "Imagerie térahertz par réflexion interne totale pour la biologie. : Application à l'étude de la perméabilisation cellulaire." Thesis, Université Paris-Saclay (ComUE), 2016. http://www.theses.fr/2016SACLX068/document.
Full textLying between 0.1 to 10x1012 Hz, the terahertz radiation occupies a middle ground between microwaves and infrared light waves, sometimes named “the terahertz gap” for technologies relevant to generation and detection have only risen at the beginning of the 90’s and aren’t fully developed yet. Nevertheless, there are strong exploratory incentives because of terahertz spectroscopic sensitivity to molecular states (rotational, vibrational…) and weak bounds in and between molecules. In the case of biological object, terahertz waves are especially sensitive to water: its quantity, physico-chemical state and solutes. We implemented an Attenuated Total internal Reflection (ATR) imaging setup in order to distinguish live cells from their physiological bathing medium. Throughout this work, we characterized both experimentally and experimentally the ATR setup. The first demonstration of the contrast origin in the terahertz images obtained was done. It arises from the intracellular content, more specifically the proteins and peptides dissolved in the cytoplasm.A precise analysis of the underlying mechanism of this proteinaceous terahertz contrast has also been developed. It gives access to original spectroscopic information about water, dissolved proteins and the hydration shell around them.Taking advantage of our whole setup comprehension, we proposed it as a non-invasive tool for quantitative live-cell permeabilization assessment in physiological conditions. During permeabilization, aka increased molecular transfers through the cell membrane, our tool allows to quantify the transfer of peptides and proteins. Live-cell permeabilization has a large application range, from fluorochrome entry in imaging, to drugs or gene therapy. In order to ensure molecules crossing the cell membrane, it’s necessary to alter its properties without compromising cell viability.A study of two permeabilization methods is proposed: chemical permeabilization and electroporation. In both cases dose effect mechanisms were quantitatively characterized. Our terahertz tool demonstrated great advantages over classical permeabilization quantification methods and permeabilization reversibility assessment methods
Ferraro, Bernadette. "Intradermal Delivery of Plasmids Encoding Angiogenic Growth Factors by Electroporation Promotes Wound Healing and Neovascularization." [Tampa, Fla] : University of South Florida, 2009. http://purl.fcla.edu/usf/dc/et/SFE0002823.
Full textWalker, Tara L. "The Development Of Microalgae As A Bioreactor System For The Production Of Recombinant Proteins." Thesis, Queensland University of Technology, 2004. https://eprints.qut.edu.au/15905/1/Tara_Walker_Thesis.pdf.
Full textWalker, Tara L. "The Development Of Microalgae As A Bioreactor System For The Production Of Recombinant Proteins." Queensland University of Technology, 2004. http://eprints.qut.edu.au/15905/.
Full textSvoboda, Devon. "The Role of Pocket Proteins pRb and p107 in Radial Migration and Axon Guidance through Cell Cycle Independent Mechanisms." Thesis, Université d'Ottawa / University of Ottawa, 2015. http://hdl.handle.net/10393/32954.
Full textFouquet, Claire. "Effect of adjacent satellite DNA on the electroporation efficiency and on the stability of the TK+ phenotype, of neo and HSV-1 tk containing plasmids, and detection of satellite DNA-binding proteins." Thesis, McGill University, 1992. http://digitool.Library.McGill.CA:80/R/?func=dbin-jump-full&object_id=60703.
Full textMoreover, we have detected (both in nuclear and partially purified HeLa whole cell extracts) the presence of proteins that specifically bind the human 1797 bp satellite II DNA sequence. Four proteins with molecular weights of 100, 93, 77 and 34 kDa were identified and named Satellite DNA-binding protein, Sbp-1, -2, -3 and -4, respectively. The function of these proteins is, as yet, unknown.
PILLAI, Vinoshene. "Intravital two photon clcium imaging of glioblastoma mouse models." Doctoral thesis, Scuola Normale Superiore, 2021. http://hdl.handle.net/11384/109211.
Full textMercatelli, Eleonora. "Development of novel sample preparation strategies for in-cell NMR." Doctoral thesis, 2017. http://hdl.handle.net/2158/1114729.
Full textMühlfriedel, Sven. "Mechanismen der Entwicklung des zerebralen Kortex." Doctoral thesis, 2004. http://hdl.handle.net/11858/00-1735-0000-0006-AC7F-7.
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