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The Global ETD Search service is a free service for researchers
to find electronic theses and dissertations. This service is
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Networked Digital Library of Theses and Dissertations.
Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
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Showing 141 to 150 of 172 (0.163 seconds)Spelling suggestions: "subject:"biophysics."" "subject:"biophysical.""
| 141 |
Spatial and temporal aspects of PI(4,5)P<sub>2</sub> and SNAREs in exocytosis studied using isolated membrane sheets and capacitance measurements / Spatial and temporal aspects of PI(4,5)P<sub>2</sub> and SNAREs in exocytosis studied using isolated membrane sheets and capacitance measurementsMilosevic, Ira 18 January 2006 (has links)
No description available.
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| 142 |
Struktur-Funtionsbeziehung in den spleißosomalen Proteinen des U4/U6•U5 tri-snRNP / Structure-functionrelationship of the Proteins within the U4/U6•U5 tri-snRNPMüllers, Nina 02 November 2006 (has links)
No description available.
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| 143 |
The Mechanics of Mitotic Cell RoundingStewart, Martin 11 July 2012 (has links) (PDF)
During mitosis, adherent animal cells undergo a drastic shape change, from essentially flat to round, in a process known as mitotic cell rounding (MCR). The aim of this thesis was to critically examine the physical and biological basis of MCR.
The experimental part of this thesis employed a combined optical microscope-atomic force microscope (AFM) setup in conjunction with flat tipless cantilevers to analyze cell mechanics, shape and volume. To this end, two AFM assays were developed: the constant force assay (CFA), which applies constant force to cells and measures the resultant height, and the constant height assay (CHA), which confines cell height and measures the resultant force. These assays were deployed to analyze the shape and mechanical properties of single cells trans-mitosis. The CFA results showed that cells progressing through mitosis could increase their height against forces as high as 50 nN, and that higher forces can delay mitosis in HeLa cells. The CHA results showed that mitotic cells confined to ~50% of their normal height can generate forces around 50-100 nN without disturbing mitotic progression. Such forces represent intracellular pressures of at least 200 Pascals and cell surface tensions of around 10 nN/µm. Using the CHA to compare mitotic cell rounding with induced cell rounding, it was observed that the intracellular pressure of mitotic cells is at least 3-fold higher than rounded interphase cells. To investigate the molecular basis of the mechanical changes inherent in mitotic cell rounding, inhibitors and toxins were used to pharmacologically dissect the role of candidate cellular processes. These results implicated the actomyosin cortex and osmolyte transporters, the most prominent of which is the Na+/H+ exchanger, in the maintenance of mechanical properties and intracellular hydrostatic pressure. Observations on blebbing cells under the cantilever supported the idea that the actomyosin cortex is required to sustain hydrostatic pressure and direct this pressure into cell shape changes. To gain further insight into the relationship between actomyosin activity and intracellular pressure, dynamic perturbation experiments were conducted. To this end, the CHA was used to evaluate the pressure and volume of mitotic cells before, during and after dynamic perturbations that included tonic shocks, influx of specific inhibitors, and exposure to pore-forming toxins. When osmotic pressure gradients were depleted, pressure and volume decreased. When the actomyosin cytoskeleton was abolished, cell volume increased while rounding pressure decreased. Conversely, stimulation of actomyosin cortex contraction triggered an increase in rounding pressure and a decrease in volume. Taken together, the dynamic perturbation results demonstrated that the actomyosin cortex contracts against an opposing intracellular pressure and that this relationship sets the surface tension, pressure and volume of the cell.
The discussion section of this thesis provides a comprehensive overview of the physical basis of MCR by amalgamating the experimental results of this thesis with the literature. Additionally, the biochemal signaling pathways and proteins that drive MCR are collated and discussed. An exhaustive and unprecedented synthesis of the literature on cell rounding (approx. 750 papers as pubmed search hits on “cell rounding”, April 2012) reveals that the spread-to-round transition can be thought of in terms of a surface tension versus adhesion paradigm, and that cell rounding can be physically classified into four main modes, of which one is an MCR-like category characterized by increased actomyosin cortex tension and diminution of focal adhesions. The biochemical pathways and signaling patterns that correspond with these four rounding modes are catalogued and expounded upon in the context of the relevant physiology. This analysis reveals cell rounding as a pertinent topic that can be leveraged to yield insight into core principles of cell biophysics and tissue organization. It furthermore highlights MCR as a model problem to understand the adhesion versus cell surface tension paradigm in cells and its fundamentality to cell shape, mechanics and physiology.
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| 144 |
Functional properties and Ca2+-dependent feedback modulation of voltage-gated Ca2+ channels in glutamatergic nerve terminals of the mammalian auditory brainstem / Funktionelle Eigenschaften und Ca2+-abhängige 'feedback'-Regulation spannungsaktivierter Ca2+-Kanäle in glutamatergen Nervterminalien des auditorischen Stammhirns der SäugetiereLin, Kun-Han 08 April 2011 (has links)
No description available.
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| 145 |
Investigation of Interactions between Homeodomain Proteins and DNA / Untersuchung der Wechselwirkungen zwischen Homeodomän-Proteinen und DNSVainius, Darius 18 May 2004 (has links)
No description available.
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| 146 |
Wirkung schwerer Ionen auf strahlenresistente und strahlensensitive Tumorzellen / Effect of heavy ions upon radioresistant and radiosensitive tumor cellsHofman-Hüther, Hana 31 October 2001 (has links)
No description available.
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| 147 |
Stimulus-secretion coupling in pancreatic β-cells of healthy and diabetic rats in tissue slice preparation / Stimulus Sekretions Kopplung pankreatischer β-Zellen gesunder und diabetischer Ratten in Gewebeschnitt PräparationRose, Tobias 18 January 2006 (has links)
No description available.
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| 148 |
Ultraschnelle, lichtinduzierte Primärprozesse im elektronisch angeregten Zustand des Grün Fluoreszierenden Proteins (GFP) / Ultrafast Elementary Events in the Excited State of Green Fluorescent Protein (GFP)Winkler, Kathrin 24 January 2003 (has links)
No description available.
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| 149 |
Eine Symmetrie der visuellen Welt in der Architektur des visuellen Kortex. / A Symmetry of the Visual World in the Architecture of the Visual Cortex.Schnabel, Michael 18 December 2008 (has links)
No description available.
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| 150 |
Crystalline, membrane-embedded, and fibrillar proteins investigated by solid-state NMR spectroscopy / Untersuchung kristalliner, membranständiger und fibrillärer Proteine mittels Festkörper-NMR-SpektroskopieSchneider, Robert 30 January 2009 (has links)
No description available.
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