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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the 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.
21

Scattering Cross-sections of 4/1 Prolate Spheroids

Tompkins, Keith W. 06 1900 (has links)
This is a report of the second in a projected series of experiments at North Texas State College designed for obtaining information about the microwave scattering properties of various shaped objects.
22

Backscattering from Prolate Spheroids at Microwave Frequencies

Sybert, Jim 08 1900 (has links)
This thesis examines backscattering from prolate spheroids at microwave frequencies.
23

The Impact of Stromal Cells on the Metabolism of Ovarian Cancer Cells in 3D Culture

Pyne, Emily Seton 03 February 2017 (has links)
Ovarian cancer is the leading cause of death among female gynecologic cancers. Current treatments include surgical debulking, and chemotherapy. However, better interventions are needed to reduce the mortality rate of metastatic disease. Ovarian cancer cells have displayed the ability to aggregate and form 3D homogeneous and heterogeneous spheroids, which can function as micrometastases. Ovarian cancer spheroids survive independently prior to adhering to an endothelial tissue. Since aggregation has been shown to provide a survival advantage to the spheroids and increased their aggressive phenotype, this study aimed to investigate how the metabolism of ovarian cancer cells change in 3-dimensional (3D) culture. Examining metabolic pathways and identifying markers of metabolic change could provide the scientific base for new, targeted interventions for this disease. Spheroids of both homogeneous and heterogeneous composition demonstrated overall lower metabolic capacity than their adherent counterparts. Spheroids had a lower basal energetic demand than adherent cells, paralleled by lower maximal respiration capacity, glycolytic capacity, and spare respiratory capacity. We conclude that the lower energetic demand of spheroids may be a mechanism to prolong death by reserving energy and metabolic cellular processes; this may render anti-metabolic drug treatment with AICAR or metformin ineffective against disseminating ovarian cancer aggregates. / Master of Science / Ovarian cancer is currently the leading cause of death among female gynecologic cancers. While treatments exist, better interventions are needed to reduce the mortality rate in this form of cancer. Ovarian cancer cells have displayed the ability to aggregate and form 3D homogeneous and heterogeneous spheroids, which can function as micrometastases. Ovarian cancer spheroids survive independently prior to adhering to an endothelial tissue. Since aggregation has been shown to provide a survival advantage to the spheroids and increased their aggressive phenotype, this study aims to investigate how the metabolism of ovarian cancer cells change in 3- dimensional (3D) culture. Examining metabolic pathways and identifying markers of metabolic change could provide the scientific base for new, targeted interventions for this disease.
24

The effect of hypoxia and 3D culture conditions on heterogeneous ovarian cancer spheroids

Liu, Lu 10 January 2017 (has links)
Epithelial ovarian cancer (EOC) is the leading cause of death from gynecological malignancy due to the insufficient accurate screening programs for the early detection of EOC. To improve the accuracy of the early detection, there is a need to deeply understand the mechanism of EOC progression and the interaction between cancer cells with their unique microenvironment. Therefore, this work investigated the metabolic shift in the mouse model for progressive ovarian cancer, and evaluated the effects of hypoxic environment, spheroid formation as well as stromal vascular fractions (SVF) on the metabolic shift, proliferation rate, drug resistance and protein markers in functional categories. The results demonstrated an increasingly glycolytic nature of MOSE cells as they progress from a tumorigenic (MOSE-L) to a highly aggressive phenotype (MOSE-FFL), and also showed changes in metabolism during ovarian cancer spheroid formation with SVF under different oxygen levels. More specifically, the hypoxic environment enhanced glycolytic shift by upregulating the glucose uptake and lactate secretion, and the spheroid formation affected the cellular metabolism by increasing the lactate secretion to acidify local environments, modulating the expression of cell adhesion molecules to enhance cell motility and spheroids disaggregation, and up-regulating invasiveness markers and stemness makers to promote ovarian cancer aggressive potential. Hypoxia and spheroid formation decreased ovarian cancer cells growth but increased the chemoresistance, which leads to the promotion of aggressiveness and metastasis potential of ovarian cancer. SVF co-cultured spheroids further increased the glycolytic shift of the heterogeneous of ovarian cancer spheroids, induced the aggressive phenotype by elevating the corresponding protein markers. Decreasing the glycolytic shift and suppression of the proteins/pathways may be used to inhibit aggressiveness or metastatic potential of ovarian cancer heterogeneous of ovarian cancer spheroids, induced the aggressive phenotype by elevating the corresponding protein markers. Decreasing the glycolytic shift and suppression of the proteins/pathways may be used to inhibit aggressiveness or metastatic potential of ovarian cancer. / Master of Science / Epithelial ovarian cancer (EOC) is the leading cause of death from gynecological malignancy due to the usually late detection when the cancer has already spread throughout the peritoneal cavity. Physical, cellular and chemical factors can contribute to EOC progression and metastasis. Critical physical factors are the low oxygen content in the peritoneal cavity (hypoxia) that promotes tumor cells survival, and the formation of tumor spheres, which have been demonstrated to have a more aggressive phenotype. Moreover, obesity has been proposed to support ovarian cancer development and progression. Therefore, this work investigated the impact of oxygen deprivation, sphere formation, and white adipose tissue-derived stromal cells on ovarian cancer cells progression. The results showed that all these factors contribute to the aggressive potential of ovarian cancer cells by increasing the drug resistance, and modulation of cellular metabolism. The understanding of the interactions between ovarian cancer and other cells within their unique microenvironment may provide critical targets for chemotherapeutic interventions that are aimed to control the aggressiveness of ovarian metastases in their hypoxic tumor microenvironment, and enhance the life of women afflicted with ovarian cancer.
25

The convective instability of the boundary-layer flow over families of rotating spheroids

Samad, Abdul January 2011 (has links)
The majority of this work is concerned with the local-linear convective instability analysis of the incompressible boundary-layer flows over prolate spheroids and oblate spheroids rotating in otherwise still fluid. The laminar boundary layer and the perturbation equations have been formulated by introducing two distinct orthogonal coordinate systems. A cross-sectional eccentricity parameter e is introduced to identify each spheroid within its family. Both systems of equations reduce exactly to those already established for the rotating sphere boundary layer. The effects of viscosity and streamline-curvature are included in each analysis. We predict that for prolate spheroids at low to moderate latitudes, increasing eccentricity has a strong stabilizing effect. However, at high latitudes of ϴ ≥ 60, increasing eccentricity is seen to have a destabilizing effect. For oblate spheroids, increasing eccentricity has a stabilizing effect at all latitudes. Near the pole of both types of spheroids, the critical Reynolds numbers approach that for the rotating disk boundary layer. However, in prolate spheroid case near the pole for very large values of e, the critical Reynolds numbers exceed that for the rotating disk. We show that high curvature near the pole of prolate spheroids is responsible for the increase in critical Reynolds number with increasing eccentricity. For both types of spheroids at moderate eccentricity, we predict that the most amplified modes travel at approximately 76% of the surface speed at all latitudes. This is consistent with the existing studies of boundary-layer flows over the related rotating-disk, -sphere and -cone geometries. However, for large values of eccentricity, the traveling speed of the most amplified modes increases up to approximately 90% of the surface speed of oblate spheroids and up to 100% in the prolate spheroid case.
26

AUTOMATING THE PROCESS OF FABRICATING UNIFORM-SIZED CELL SPHEROIDS FOR THREE-DIMENSIONAL BIOPRINTING

Sosale, Ganesh 01 January 2015 (has links)
Although researchers have been able to print small, simple, and avascular tissues, they have been unsuccessful in creating large, complex and vascularized organs. Printing large and complex three-dimensional tissues or organs involves utilizing a large quantity of cellular spheroids and layer-by-layer addition of spheroids. In this study, an in-house cell spheroid fabrication system was developed to produce cell spheroids with human liver cells (hepG2), human endothelial cells (hEC), human neural stem cells (hNSC), and induced pluripotent stem cells (iPSC). It offers the ability of fabricating uniform-sized spheroids repeatedly, which is essential when large and complex structures need to be produced. In order to test the spheroids’ ability to fuse, hEC spheroids were placed in line with one another and revealed successful fusion. Overall, the results indicate the in- house developed cell spheroid fabrication system can play a major role in bioprinting by providing researchers with uniform-sized spheroids in large quantities, consistently.
27

Influence de sécrétions ascitiques sur le comportement des cellules cancéreuses ovariennes : identification de cibles moléculaires adhésives. / Influence of ascitic fluids on the behavior of ovarian cancer cells : identification of molecularadhesive targets.

Carduner, Ludovic 20 December 2013 (has links)
Le cancer de l'ovaire représente la première cause de décès par cancer gynécologique. La survie globale des patientes à 5 ans est inférieure à 30%. Ce sombre pronostic s'explique à la fois par la découverte tardive de la maladie et par le développement d'une chimiorésistance. L'ascite est un fluide exsudatif qui est fréquemment accumulé dans la cavité péritonéale au cours de la progression des cancers de l'ovaire. Ce « microenvironnement tumoral » particulier contribue à la dissémination des cellules cancéreuses et à leurs implantations péritonéales.L'objectif global du travail de thèse a été, d'une part d'évaluer l'influence de l'ascite sur le comportement des cellules cancéreuses ovariennes et d'autre part, d'étudier les mécanismes de résistance à la perte d'ancrage des cellules cancéreuses ovariennes.Nous avons ainsi démontré que l'ascite induit une transition épithélio-mésenchymateuse partielle et que les modifications des comportements cellulaires observées sont dépendantes des intégrines alpha-v.Deux ligands de ces intégrines, la vitronectine et la fibronectine, ont été purifiés selon un protocole original permettant la caractérisation des deux protéines à partir d'une même ascite. Ces protéines ascitiques ont des propriétés différentes selon leur origine, donc selon les patientes dont elles sont issues, et influencent le comportement adhésif des cellules avec un degré variable. L'importance de la signalisation dépendante des intégrines alpha-v et des voies MAP Kinases a également été démontrée dans l'établissement d'une résistance des sphéroïdes tumoraux à l'anoïkis.En perspective, approfondir les connaissances des processus cellulaires et moléculaires conduisant à la dissémination intrapéritonéale et à l'émergence de chimiorésistance ainsi que déterminer le rôle potentiel de protéines ascitiques dans ces processus pourraient permettre la découverte de nouvelles cibles thérapeutiques. / Ovarian cancer is the most lethal gynaecological malignant disease, mainly due to late diagnosis and to acquired chemoresistance. An exudative fluid named ascites is frequently accumulates within the abdominal cavity during ovarian cancer progression. This unique tumor microenvironment contributes to cancer cell dissemination and peritoneal metastasis.The aim of the study was to evaluate the influence of ascites on cancer cell behaviors and to better understand the mechanisms of ovarian cancer cell resistance to the loss of anchorage.We demonstrate that ascites induces a partial epithelial–mesenchymal transition and that the modifications of cell behaviors observed are dependent of alpha-v integrins. A combined purification protocol has been established in order to purify vitronectin and Fibronectin, both ligands of these integrins, from a single pathological sample. These purified ascitic proteins have different molecular features according to the patients and impact the adhesive cell behavior with various degrees.Moreover we showed the importance of alpha-v integrins and MAP Kinases signalling pathways in the anoikis resistance of ovarian cancer spheroids.Our prospects are i) to increase the knowledge of the cellular and molecular processes leading to the intraperitoneal dissemination and to the emergence of chemoresistance and also ii) to determine the potential role of ascitics proteins in these processes. We will expect that these investigations couldlead to the discovery of new therapeutic targets.
28

Análise da viabilidade das células H295R, linhagem de carcinoma adrenocortical tumoral humano, tratadas com diferentes drogas antitumorais. / Antitumor effects of different cytotoxic drugs on the human adrenocortical tumor cells H295R.

Silveira, Elaine 06 November 2014 (has links)
O carcinoma adrenocortical (ACC) é um tumor maligno raro. O objetivo foi testar a ação de drogas antitumorais na linhagem H295R, em cultura 2D e 3D, analisadas por MTS, ensaios multiparamétricos, e microscopia confocal. Em monocamada (2D), as drogas tiveram maior efeito quando utilizadas com o mitotano 10 mM, sendo: everolimus 10 mM (50±0,02% p &#8804 0.001), imatinib (10 mM 52±0.01% p &#8804 0.001), sunitinib 5 mM (47±0.02% p &#8804 0.001), e nilotinib 5 mM (59±0,03% p &#8804 0.001), com evidência de apoptose. Nos esferoides (3D) foi necessário mitotano 30 M com everolimus 10 mM para se obter diminuição de 32±0.02% p &#8804 0.001 na viabilidade das células, e com nilotinib 10 mM para redução de 57±0.03% p &#8804 0.001, com evidência de necrose e apoptose. Em resumo, os dados sugerem que os esferoides são mais resistentes aos tratamentos, como ocorre com tumores in vivo, e podem representar uma importante abordagem para estudos de ACC. O nilotinib foi o que induziu as melhores respostas, tanto no modelo em 2D quanto 3D, resultados que se apresentam promissores para o tratamento dos carcinomas adrenocorticais. / Adrenocortical carcinoma (ACC) is a rare malignant tumor. The objective was to test the antitumor drugs action in the H295R cell line, in 2D and 3D culture system, by using MTS, multiparameter assay (High Content Screening) and confocal microscopy. In monolayer, all drugs were more effective in combination with mitotane 10 mM: everolimus 10 mM (50±0.02%), 10 mM imatinib (52±0.01%), 5 mM sunitinib (47±0.02%), and 5 mM nilotinib (59±0.03%). The spheroids required mitotano 30 mM with everolimus 10 mM to decrease cell viability (32±0.02% p &#8804 0.001); and with 10 mM nilotinib to inhibit cell viability in 57±0.03% (p &#8804 0.001), with induction of apoptosis and necrosis. In summary, the spheroids were more resistant to treatment and may represent an important approach for studies of ACC. Nilotinib was the tyrosine kinase inhibitor that, either alone or in combination with mitotane, induced higher cytotoxicity, in both 2D and 3D cell cultures, showing promising results for the treatment of adrenocortical carcinoma, as well as for the studies of its mechanism of action.
29

Geração e caracterização de tecido equivalente endotelial e seu potencial osteopromotor

Feltran, Georgia da Silva January 2019 (has links)
Orientador: Willian Fernando Zambuzzi / Resumo: Com o aumento progressivo da expectativa de vida da população, defeitos ósseos se tornou um problema de saúde pública. Por sua vez, o sistema esquelético abriga um conjunto de células que, de maneira hierárquica, sustentam a formação do osso ao longo da vida, sendo sua capacidade regenerativa comprometida durante o processo de envelhecimento. Com o aumento da expectativa de vida, a população idosa vem crescendo nos últimos anos e com ela o aumento eminente de fraturas ósseas. Sabe-se que o desenvolvimento e regeneração ósseos são eventos complexos e controlados por mecanismos parácrinos de sinalização intercelulares, destacando que a osteogênese está acoplada, principalmente, à angiogênese. Embora relatado, este mecanismo de comunicação entre células endoteliais e células osteoprogenitoras não está bem elucidado, sobretudo considerando o repertório de moléculas tróficas envolvidas. A fim de compreender melhor estes mecanismos, o objetivo deste trabalho foi desenvolver metodologias capazes de mimetizar o microambiente endotelial-ósseo, bem como desvendar eventos acoplados entre os diferentes tipos celulares envolvidos no processo, sobretudo gerando tecido endotelial in vitro, equivalente ao original. Para isso, fizemos uso de células humanas primárias, as quais foram submetidas a diferentes protocolos experimentais, onde a mesma densidade de células endoteliais arterial (HCAEC) e venosa (HUVEC) e de musculatura lisa (AoSMC) (cultivo misto) foi plaqueada em tubos cônicos sem tr... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: With the progressive increase in the life expectancy of the population, bone defects became a public health problem. In turn, the skeletal system houses a set of cells that, in a hierarchical way, support the formation of the bone throughout life, and its regenerative capacity is compromised during the aging process. With the increase in life expectancy, the elderly population has been increasing in recent years and with it the eminent increase of bone fractures. It is known that bone development and regeneration are complex events and controlled by paracrine mechanisms of intercellular signaling, emphasizing that osteogenesis is mainly coupled with angiogenesis. Although reported, this mechanism of crosstalk between endothelial cells and osteoprogenitor cells is not well elucidated, especially considering the repertoire of involved trophic molecules. In order to better understand these mechanisms, the objective of this work was to develop methodologies capable of mimicking the endothelial-bony microenvironment, as well as unveiling the coupled events between the different cell types involved in the process, especially generating endothelial tissue in vitro, equivalent to the original one. For this, we used primary human cells, which were submitted to different experimental protocols, where the same density of arterial (HCAEC) and venous (HUVEC) endothelial cells and smooth muscle cell (AoSMC) (mixed culture) were plated in tubes (s), and after 72 hours the generated spheroid... (Complete abstract click electronic access below) / Mestre
30

A systems biology approach to target identification using three-dimensional multi-cellular tumour spheroids (MCTS) : regio-specific molecular dissection of gene expression, protein expression and functional activity in 3D MCTS

McMahon, Kelly January 2011 (has links)
Within solid tumours, a microenvironment exists that causes resistance to chemotherapy. New drugs that target cells within this microenvironment are required, the first step in this process being the identification of new targets. The aim of this thesis was to characterise changes in the transcriptome and proteome within specific regions of multicell-tumour spheroids (MCTS), an experimental model that mimics many of the features of the tumour microenvironment. HT29 MCTS were separated by sequential trypsinisation into 3 main regions; the outer surface layer (SL) the peri-necroric region (PN) and the necrotic core (NC). Using an iTRAQ quantitative proteomics approach, the proteome of the different MCTS regions was investigated. A 2 dimensional separation approach using Agilent's OffGel system and RP-nano HPLC was incorporated prior to MS analysis. MS analysis was done using both MALDI-TOF-TOF (Bruker Ultraflex II) and ESI-Q-TOF (Agilent 6530 QTOF LC/MS) instruments. Gene expression profiles of the different MCTS were investigated and compared using Agilent's one-color oligonucleotide based microarrays. Transcriptomic and proteomic analysis identified several key differences in the proteins involved in cell metabolism between the SL and PN/NC regions. Similar metabolic changes were also noted between autophagic and normal monolayer cells. Many highlighted proteins represented established cancer associated proteins. Interestingly, a number of proteins were highlighted which have no previous association with cancer and may upon further validation, provide attractive leads for therapeutic intervention.

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