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A method of maintaining identifiable odontoblasts in vitro a thesis submitted in partial fulfillment ... in pedodontics ... /Fisher, Molly Green. January 1968 (has links)
Thesis (M.S.)--University of Michigan, 1968.
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Selection of simian immunodeficiency virus variants during progression to immunodeficiency /Chackerian, Bryce Charles, January 1996 (has links)
Thesis (Ph. D.)--University of Washington, 1996. / Vita. Includes bibliographical references (leaves [115]-128).
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Insulin-induced endothelial cell proliferation and viability in stretched murine skin and cell cultureShrader, Carl D. January 2007 (has links)
Thesis (Ph. D.)--West Virginia University, 2007. / Title from document title page. Document formatted into pages; contains xiii, 127 p. : ill. (some col.). Vita. Includes abstract. Includes bibliographical references.
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Calibration of a radiobiological irradiator : the Faxitron cabinet X-ray system model CP160AlDahlawi, Ismail January 2008 (has links)
No description available.
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Interfacial study of cell adhesion to liquid crystals using widefield surface plasmon resonance microscopySoon, C. F., Khaghani, S. A., Youseffi, M., Nayan, N., Saim, H., Britland, S., Blagden, N., Denyer, M. C. January 2013 (has links)
Widefield surface plasmon resonance (WSPR) microscopy provides high resolution imaging of interfacial interactions. We report the application of the WSPR imaging system in the study of the interaction between keratinocytes and liquid crystals (LC). Imaging of fixed keratinocytes cultured on gold coated surface plasmon substrates functionalized with a thin film of liquid crystals was performed in air using a 1.45NA objective based system. Focal adhesion of the cells adhered to glass and LC were further studied using immunofluorescence staining of the vinculin. The imaging system was also simulated with 2x2 scattering matrix to investigate the optical reflection of the resonant plasmonic wave via the glass/gold/cell and glass/gold/LC/cell layers. WSPR imaging indicated that keratinocytes are less spread and formed distinct topography of cell-liquid crystal couplings when cultured on liquid crystal coated substrates. The simulation indicates that glass/LC shifted the surface plasmon excitation angle to 75.39 degrees as compared to glass/air interface at 44 degrees . The WSPR microcopy reveals that the cells remodelled their topography of adhesion at different interfaces.
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Exossomos derivados de células dendríticas como adjuvantes naturais na resposta antitumoral. / Dendritic cells-derived exosomes as natural adjuvants in antitumor responses.Romagnoli, Graziela Gorete 18 May 2012 (has links)
Exossomos (Exo) originados de células dendríticas (DCs) carregam moléculas associadas à apresentação antigênica. Neste trabalho procurou-se estabelecer se Exo de DCs seriam capazes de conferir imunogenicidade às células tumorais. Os Exo isolados de culturas de DCs expressavam as moléculas HLA-ABC, HLA-DR, CD86, CD11c, CD81, CD54 e CD18. Estes foram então adicionados às células da linhagem humana de adenocarcinoma mamário, SK-BR-3, as quais passaram a expressar as moléculas HLA-DR, CD86 e CD11c. As células tumorais modificadas pelos Exo induziram a produção de IL-6 e IL-10, detectados no sobrenadante das co-culturas destas com linfócitos T. Estas células tumorais também induziram aumento do número de linfócitos produtores de IFN-<font face=\"Symbol\">g, pré-sensibilizados contra antígenos tumorais, e aumento da expressão de SOCS3 nestes. Em conclusão, nossos resultados mostram que, Exo de DCs alteram o fenótipo de células tumorais, modificando sua interação com linfócitos T, sem induzir nas mesmas capacidade de ativar respostas proliferativas ou citotóxicas de linfócitos T in vitro. / Exosomes (Exo) originated from dendritic cells (DCs) contain molecules involved in antigen presentation. The present work sought to determine if Exo from DCs would be able to transfer immunogenicity to tumor cells. Exo isolated from DCs cultures carried HLA-ABC, HLA-DR, CD86, CD11c, CD81, CD54 and CD18. These Exo were added to cultures of the human breast adenocarcinoma cell line, SK-BR-3, which gained expression of HLA-DR, CD86 and CD11c. Tumor cells modified by Exo induced IL-6 and IL-10 production, detected in the supernatant of their co-cultures with T lymphocytes. These tumor cells also induced an increase in the frequency of IFN-<font face=\"Symbol\">g-producing T lymphocytes, pre-sensitized against tumor antigens, and an increased expression of SOCS3. In conclusion, our results show that, Exo from DCs affect the phenotype of tumor cells, modifying their interaction with T lymphocytes, without inducing the ability to activate cytotoxic or T cell proliferative responses in vitro.
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Imaging the tumor microenvironment : the dynamics and modification of hypoxia /Ljungkvist, Anna, January 2003 (has links)
Diss. (sammanfattning) Umeå : Univ., 2003. / Härtill 4 uppsatser.
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Modulation of folate receptor-[alpha] by glucocorticoid receptor and progesterone receptorTran, Thuyet Van. January 2004 (has links)
Thesis (Ph. D.)--Medical College of Ohio, 2004. / "In partial fulfillment of the requirements for the degree of Doctor of Philosophy in Medical Sciences." Major advisor: Manohar Ratnam. Includes abstract. Document formatted into pages: iii, 293 p. Title from title page of PDF document. Includes bibliographical references (p. 175-281).
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Exossomos derivados de células dendríticas como adjuvantes naturais na resposta antitumoral. / Dendritic cells-derived exosomes as natural adjuvants in antitumor responses.Graziela Gorete Romagnoli 18 May 2012 (has links)
Exossomos (Exo) originados de células dendríticas (DCs) carregam moléculas associadas à apresentação antigênica. Neste trabalho procurou-se estabelecer se Exo de DCs seriam capazes de conferir imunogenicidade às células tumorais. Os Exo isolados de culturas de DCs expressavam as moléculas HLA-ABC, HLA-DR, CD86, CD11c, CD81, CD54 e CD18. Estes foram então adicionados às células da linhagem humana de adenocarcinoma mamário, SK-BR-3, as quais passaram a expressar as moléculas HLA-DR, CD86 e CD11c. As células tumorais modificadas pelos Exo induziram a produção de IL-6 e IL-10, detectados no sobrenadante das co-culturas destas com linfócitos T. Estas células tumorais também induziram aumento do número de linfócitos produtores de IFN-<font face=\"Symbol\">g, pré-sensibilizados contra antígenos tumorais, e aumento da expressão de SOCS3 nestes. Em conclusão, nossos resultados mostram que, Exo de DCs alteram o fenótipo de células tumorais, modificando sua interação com linfócitos T, sem induzir nas mesmas capacidade de ativar respostas proliferativas ou citotóxicas de linfócitos T in vitro. / Exosomes (Exo) originated from dendritic cells (DCs) contain molecules involved in antigen presentation. The present work sought to determine if Exo from DCs would be able to transfer immunogenicity to tumor cells. Exo isolated from DCs cultures carried HLA-ABC, HLA-DR, CD86, CD11c, CD81, CD54 and CD18. These Exo were added to cultures of the human breast adenocarcinoma cell line, SK-BR-3, which gained expression of HLA-DR, CD86 and CD11c. Tumor cells modified by Exo induced IL-6 and IL-10 production, detected in the supernatant of their co-cultures with T lymphocytes. These tumor cells also induced an increase in the frequency of IFN-<font face=\"Symbol\">g-producing T lymphocytes, pre-sensitized against tumor antigens, and an increased expression of SOCS3. In conclusion, our results show that, Exo from DCs affect the phenotype of tumor cells, modifying their interaction with T lymphocytes, without inducing the ability to activate cytotoxic or T cell proliferative responses in vitro.
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Estudo do efeito da fração BRVD obtida a partir da própolis brasileira tipificada, na proliferação de células tumorais / Study of fraction BRVD effects gotten by tipificated Brazilian própolis, in the proliferation of tumorais cellsCosta, Martha Silveira e 17 September 2007 (has links)
A própolis, um produto natural derivado de resinas de plantas coletadas por abelhas, foi usada por milhares de anos na medicina tradicional pelo mundo inteiro. Neste estudo, investigamos o efeito de uma fração da própolis vermelha brasileira (BRVD), no crescimento das células de melanoma murino (B16F10), das linhagens hematológicas humanas (HL-60 e K562), e de fibroblastos humanos (MCR-5 e FP). Após a análise preliminar de várias frações da própolis BRV, encontramos que a Fração BRVD inibiu fortemente o crescimento das células de uma maneira dose-tempo dependente pela necrose. Os resultados mostraram que essa fração induz eficazmente um efeito citotóxico em todas as linhagens estudadas, com média da IC50 em torno de 30 g/mL em 24 h de exposição. Estes resultados sugerem que a atividade antitumor da fração BRVD ocorre com a indução de necrose e os compostos dessa fração podem ser úteis como um agente contra o câncer / Propolis, a natural product derived from plant resins collected by honeybees, has been used for thousands of years in traditional medicine all over the world. In this study we have investigated the effect of some fractions from red Brazilian propolis on the growth of murine melanoma cell ( B16/F10), human hematological cells ( HL-60 and K562), and human fibroblasts cells (MCR-5 and FP). We found that BRVD strongly inhibited the growth of the cells in a dose- and time-dependent through induction of necrosis. Our results showed that BRVD effectively induced a cytotoxic effect on all cell lines studied, with IC50 average about 30 g/mL for 24 h of exposition. These results suggest that the antitumor activity of BRVD from red Brazilian propolis occurs through the induction of necrosis and its compounds may be useful as a anticancer agent
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