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Síntese e caracterização de nanopartículas magnéticas de óxido de ferro para aplicações biomédicas – um estudo citotóxico em linhagem celular de carcinoma cervical humano (células HeLa)Souza, Aryane Tofanello de [UNESP] 29 October 2011 (has links) (PDF)
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000680523.pdf: 1511132 bytes, checksum: c20e5a6a65edf2cba90d4de2b5073a08 (MD5) / Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq) / Nanopartículas magnéticas (NPMs) têm sido alvo de inúmeras investigações por seu grande potencial de aplicação nos mais diferentes campos tecnológicos. Dentre tantos, elas destacam-se na área biomédica, seja no diagnóstico ou tratamento de diversas doenças. Neste trabalho foram sintetizadas nanopartículas magnéticas (NPMs) de óxido de ferro (magnetita) pelo método de coprecipitação de íons Fe2+ e Fe3+ em meio alcalino. O objetivo central foi estudar as características morfológicas, estruturais, magnéticas e o comportamento biológico desses compostos em células cancerígenas, visando futuras aplicações biomédicas. Inicialmente as nanopartículas magnéticas foram avaliadas em função dos parâmetros físico-químicos que influenciam diretamente as características finais do produto (pH, molaridade, temperatura e tipo de base) para se observar as melhores condições de síntese e a influência de cada um nas características do produto. As nanopartículas foram caracterizadas por difratometria de raios-X, microscopia eletrônica de varredura, potencial zeta e magnetometria. Desse primeiro estudo concluiu-se que a coprecipitação produz partículas com polidispersão de tamanhos alta e que os parâmetros de síntese influenciam drasticamente as propriedades dos materiais, no entanto, todas as amostras exibiam características magnéticas. Depois de estabelecida esta etapa, as NPMs foram submetidas à transfecção em cultura celular de carcinoma cervical humano (células HeLa) e a testes biológicos como coloração com Azul da Prússia e hematoxilina-eosina, ensaio de MTT e ensaio de apoptose para averiguação da citotoxidade. A principal observação vinda desses resultados foi que as nanopartículas magnéticas sintetizadas, salvo algumas adaptações de síntese... / Magnetic nanoparticles (MNPs) have been the subject of numerous investigations because of its great potential application in many different fields of technology. Among many, they stand out in the biomedical area, either in diagnosis or treatment of various diseases. In this work were synthesized magnetic nanoparticles (MNPs) of iron oxide (magnetite) by the coprecipitation method of Fe2+ and Fe3+ in an alkaline medium. The main objective was to study the morphological, structural, magnetic and biological behavior of these compounds in cancer cells, in order to future biomedical applications. Initially the magnetic nanoparticles were evaluated against the physical and chemical parameters that directly influence the final characteristics of product (pH, molarity, temperature and type of base) to observe the best synthesis conditions and influence of each characteristics. The nanoparticles were characterized by X-ray diffraction, sccaning electron microscopy, zeta potential and magnetometry. In this first study showed that coprecipitation produces particles with high polydispersity of sizes and that the synthesis parameters dramatically influence the properties of materials, however all samples exhibited magnetic characteristics. After you make this step, the MNP were subjected to transfection in cell culture of human cervical carcinoma (HeLa) and biological tests such as staining with Prussian blue and hematoxylin-eosin, MTT assay and apoptosis assay to investigate cytotoxicity. The main observation was that these results coming magnetic nanoparticles synthesized, except for some adjustments in short, constitute a class of nanocomposites with enormous potential for therapeutic and / or diagnosis. The work brings together information ranging from the synthesis of nanoparticles to their behavior inside the cells, emphasizing the best conditions for each procedure
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Avalia??o das atividades antioxidante, anticoagulante e antiproliferativa de extratos aquosos de marsdenia megalanthaOliveira, Ruth Medeiros de 21 March 2011 (has links)
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Previous issue date: 2011-03-21 / Coordena??o de Aperfei?oamento de Pessoal de N?vel Superior / The species of the genus Marsdenia, Apocynaceae, are widely used in folk
medicine of several countries. In Brazil is found several species belonging to this
genus. The in vitro antioxidant, anticoagulant and antiproliferative activities were
evaluated to aqueous extracts of stalk, leaf and root of Marsdenia megalantha. In
the total antioxidant capacity assay (expressed as ascorbic acid equivalents) the
stalk extract showed 76.0 mg/g, while leaf and root extracts 141.3 mg/g and 57.0
mg/g, respectively. The stalk and leaf extracts showed chelating activity around 40%
at 1.5 mg/mL, while root extract, at the same concentration showed, 17%. Only the
leaf extract showed a significant ability in superoxide scavenging (80% at 0.8
mg/mL). Any extract was able in scavenge hydroxyl, as well anticoagulant activity.
The antiproliferative activity of the extracts was evaluated against HeLa tumor cell
line. The extracts inhibited in a dose-dependent manner the cell growth. However,
the leaf extract showed 80% of inhibition at 1.0 mg/mL, while stalk and root extracts
inhibited 63% and 30%, respectively. To assess the mechanism of cell death caused
by the leaf extract in HeLa, was performed flow cytometry and western blot. The
results show that leaf extract induces cell death by apoptosis through an activation
caspase-independent pathway. These data indicate that stalk and leaf extracts
obtained have potential to be used as antioxidants and anticancer drugs / As esp?cies do g?nero Marsdenia, Apocynaceae, s?o bastante utilizadas na
medicina popular de v?rios pa?ses. No Brasil s?o encontradas v?rias esp?cies
pertencentes a esse g?nero. As atividades antioxidante, anticoagulante e
antiproliferativa foram avaliadas para os extratos de caule, folha e raiz de Marsdenia
megalantha. Na capacidade antioxidante total (expressa como equivalente de ?cido
asc?rbico), o extrato do caule apresentou 76,0 mg/g, enquanto os extratos da folha e
raiz apresentaram, respectivamente, 14,3 mg/g e 57,0 mg/g. Os extratos do caule e
da folha mostraram habilidade quelante em torno de 40% na concentra??o de 1,5
mg/mL, enquanto o extrato da raiz, na mesma concentra??o, apresentou 17%.
Apenas o extrato da folha apresentou uma capacidade significante em sequestrar
radicais super?xidos (80% em 0,8 mg/mL). Nenhum extrato mostrou capacidade em
seq?estrar radicais hidroxila, bem como atividade anticoagulante. A atividade
antiproliferativa dos extratos foi avaliada contra a linhagem tumoral HeLa. Os
extratos inibiram, de forma dose-dependente, o crescimento celular. Entretanto, o
extrato da folha foi capaz de inibir em 80% a prolifera??o celular na concentra??o de
1,0 mg/mL, enquanto os extratos de caule e raiz inibiram 63% e 30%,
respectivamente. Para avaliar o mecanismo de morte celular causada pelo extrato
da folha nas c?lulas HeLa, foi realizada citometria de fluxo e western blot. Os
resultados mostraram que o extrato da folha induz morte celular por apoptose
atrav?s de uma via de ativa??o independente de caspase. Estes resultados indicam
que os extratos de caule e folha obtidos t?m potencial para serem futuramente
utilizados como f?rmacos antioxidantes e antic?ncer
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Síntese e caracterização de nanopartículas magnéticas de óxido de ferro para aplicações biomédicas - um estudo citotóxico em linhagem celular de carcinoma cervical humano (células HeLa) /Souza, Aryane Tofanello de. January 2011 (has links)
Orientador: José Geraldo Nery / Banca: Paula Rahal / Banca: Maria Cristina Nonato Costa / Resumo: Nanopartículas magnéticas (NPMs) têm sido alvo de inúmeras investigações por seu grande potencial de aplicação nos mais diferentes campos tecnológicos. Dentre tantos, elas destacam-se na área biomédica, seja no diagnóstico ou tratamento de diversas doenças. Neste trabalho foram sintetizadas nanopartículas magnéticas (NPMs) de óxido de ferro (magnetita) pelo método de coprecipitação de íons Fe2+ e Fe3+ em meio alcalino. O objetivo central foi estudar as características morfológicas, estruturais, magnéticas e o comportamento biológico desses compostos em células cancerígenas, visando futuras aplicações biomédicas. Inicialmente as nanopartículas magnéticas foram avaliadas em função dos parâmetros físico-químicos que influenciam diretamente as características finais do produto (pH, molaridade, temperatura e tipo de base) para se observar as melhores condições de síntese e a influência de cada um nas características do produto. As nanopartículas foram caracterizadas por difratometria de raios-X, microscopia eletrônica de varredura, potencial zeta e magnetometria. Desse primeiro estudo concluiu-se que a coprecipitação produz partículas com polidispersão de tamanhos alta e que os parâmetros de síntese influenciam drasticamente as propriedades dos materiais, no entanto, todas as amostras exibiam características magnéticas. Depois de estabelecida esta etapa, as NPMs foram submetidas à transfecção em cultura celular de carcinoma cervical humano (células HeLa) e a testes biológicos como coloração com Azul da Prússia e hematoxilina-eosina, ensaio de MTT e ensaio de apoptose para averiguação da citotoxidade. A principal observação vinda desses resultados foi que as nanopartículas magnéticas sintetizadas, salvo algumas adaptações de síntese... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Magnetic nanoparticles (MNPs) have been the subject of numerous investigations because of its great potential application in many different fields of technology. Among many, they stand out in the biomedical area, either in diagnosis or treatment of various diseases. In this work were synthesized magnetic nanoparticles (MNPs) of iron oxide (magnetite) by the coprecipitation method of Fe2+ and Fe3+ in an alkaline medium. The main objective was to study the morphological, structural, magnetic and biological behavior of these compounds in cancer cells, in order to future biomedical applications. Initially the magnetic nanoparticles were evaluated against the physical and chemical parameters that directly influence the final characteristics of product (pH, molarity, temperature and type of base) to observe the best synthesis conditions and influence of each characteristics. The nanoparticles were characterized by X-ray diffraction, sccaning electron microscopy, zeta potential and magnetometry. In this first study showed that coprecipitation produces particles with high polydispersity of sizes and that the synthesis parameters dramatically influence the properties of materials, however all samples exhibited magnetic characteristics. After you make this step, the MNP were subjected to transfection in cell culture of human cervical carcinoma (HeLa) and biological tests such as staining with Prussian blue and hematoxylin-eosin, MTT assay and apoptosis assay to investigate cytotoxicity. The main observation was that these results coming magnetic nanoparticles synthesized, except for some adjustments in short, constitute a class of nanocomposites with enormous potential for therapeutic and / or diagnosis. The work brings together information ranging from the synthesis of nanoparticles to their behavior inside the cells, emphasizing the best conditions for each procedure / Mestre
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Regulación de la compartimentalización de la comunicación retículo endoplásmico-mitocondria en la línea tumoral helaBravo Sagua, Roberto January 2015 (has links)
Doctor en Bioquímica / El retículo endoplásmico (RE) y la mitocondria son organelos celulares que
entablan una continua y dinámica conversación que permite a la célula
responder coordinadamente a diversas situaciones fisiopatológicas. Datos
previos de nuestro Laboratorio mostraron que ambos organelos incrementan los
puntos de contacto físico durante la fase temprana del estrés de RE,
permitiendo una mayor transferencia de Ca2+ desde el RE hacia la mitocondria y
estimulando así el metabolismo de este último organelo y favoreciendo la
sobrevida celular. El presente proyecto estudió la participación de proteína
quinasa A (PKA) y caveolina-1 (Cav1) como agentes reguladores de esta
interacción física y funcional entre el RE y la mitocondria. Como modelo de
estudio se utilizaron células HeLa tratadas con tunicamicina como agente
inductor de estrés de RE por 4 h.
Primero, se investigó la participación de PKA en la fase temprana del
estrés de RE. Esta quinasa se activó ante condiciones de estrés, medido por la
fosforilación de DRP1 en Ser637 por Western blot y concomitante elongación
mitocondrial (microscopía confocal). El inhibidor específico de PKA H89 previno
estos cambios, comprobando que ambos son dependientes de PKA.
Posteriormente, se estudió la participación de PKA en el acoplamiento
RE-mitocondria a través de la medición de proximidad (microscopía confocal),
contactos físicos (microscopía electrónica), transferencia de Ca2+ (microscopía de fluorescencia) y bioenergética mitocondrial (tasa de consumo de oxígeno). El
papel de PKA en estos procesos se evaluó por modulación farmacológica con
H89. Los resultados mostraron que la activación de PKA es necesaria para
inducir la formación de contactos RE-mitocondria, y de esta forma, gatillar la
respuesta adaptativa frente a estrés de RE.
Luego se investigó el papel de Cav1 sobre la interface RE-mitocondria. La
expresión de Cav1 abolió completamente la respuesta adaptativa frente a estrés
de RE temprano, evidenciado mediante proximidad entre organelos,
transferencia de Ca2+ y respiración mitocondrial. Además de alterar esta
plasticidad organelar frente a condiciones de estrés, la expresión de Cav1
disminuyó significativamente la bioenergética mitocondrial basal, junto con
inducir un remodelado basal de la interface RE-mitocondria medido por
purificación de las membranas del RE asociadas a mitocondria (MAM).
Finalmente, se determinó que la expresión de Cav1 antagonizó la
señalización de PKA, impidiendo que ella fosforile a DRP1 y promueva la
elongación mitocondrial en respuesta a estrés de RE. Más aún, mediante
fraccionamiento subcelular, se estableció que Cav1 afectó la localización
subcelular de PKA, evitando que se relocalice a las membranas microsomales
en respuesta al estrés de RE. De este modo, Cav1 actúa como un regulador
negativo de PKA, previniendo su activación frente a estrés de RE, evitando así
la respuesta adaptativa celular / The endoplasmic reticulum (ER) and mitochondria are two organelles that
continuously communicate between one another. This organelle crosstalk allows
mitochondria and ER to coordinate responses to a variety of physiological and
pathophysiological situations. Data from a previous work show that during the
early phase of ER stress, both organelles increase their contact sites,
augmenting thereby calcium transfer from ER to mitochondria. This response
boosts mitochondrial bioenergetics and ultimately promotes cell survival. Here,
we sought to study the role of Protein Kinase A (PKA) and Caveolin-1 (Cav1) as
regulators of such organelle crosstalk. As an experimental model, HeLa cells
were treated with tunicamycin to induce ER stress.
First, we observed that PKA was activated during early stages of ER
stress, as assessed by increased phosphorylation of DRP1 at the inhibitory site
Ser637 (Western blot), and that this event was followed by mitochondrial
elongation (confocal microscopy). The specific PKA inhibitor H89 prevented
these changes, thus confirming that they were due to PKA and not another
kinase.
Subsequently, we studied ER-mitochondria coupling by evaluating
organelle proximity (confocal microscopy), physical contact sites (electron
microscopy), Ca2+ transfer (fluorescence microscopy) and mitochondrial
bioenergetics (oxygen consumption rate). PKA was again involved in these processes by pharmacological modulation using the inhibitor H89. Our results
show that PKA activation is necessary to induce the formation of ERmitochondria
contacts and to trigger the adaptive metabolic responses to ER
stress.
Next, we investigated the role of Cav1 as a modulator of the
ER-mitochondria interface. Cav1 overexpression completely abolished the early
adaptive response to ER stress, as assessed by evaluating the proximity
between organelles, calcium transfer and mitochondrial respiration. In addition to
altering organelle plasticity in response to stress conditions, Cav1
overexpression severely decreased baseline mitochondrial bioenergetics and
induced basal remodelling of the ER-mitochondria interface, as determined by
purification and analysis of mitochondria-associated ER membranes.
Finally, we determined that Cav1 overexpression antagonizes PKA
signalling, preventing PKA-dependent DRP1 phosphorylation and mitochondrial
elongation in response to ER stress. Moreover, subcellular fractionation
revealed that Cav1 affected PKA localization, prevented redistribution to
microsomal membranes in response to ER stress, and altered the pattern of
DRP1 phosphorylation. Thus, Cav1 functions as a negative regulator of PKA
that precludes PKA activation during early ER stress and thereby prevents the
adaptive cellular response / Fondecyt; Fondap;
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Studie- och yrkesvägledarens förutsättningar att utföra sitt uppdrag : -ur ett ledarskaps- och organisations perspektivLarsson, Pia January 2014 (has links)
Syftet med min undersökning var att belysa förutsättningen för studie- och yrkesvägledaren att utföra sitt uppdrag beroende på rektors strategier att implementera studie- och yrkesvägledning i hela organisationen. Detta ämnade jag belysa på en kommunal gymnasieskola ur ett ledarskaps och organisationsperspektiv. De två frågeställningarna var på vilket sätt påverkas studie- ochyrkesvägledarens förutsättningar att utföra sitt uppdrag beroende av hur implementeringen av att studie- och yrkesorienteringen skett i organisationen samt på vilket sätt ledarskapet och organisationen av studie- och yrkesvägledningen kan underlätta för studie- och yrkesvägledarenatt utföra sitt uppdrag i organisationen. Jag utförde undersökningen med hjälp av kvalitativa semistrukturerade forskningsintervjuer. I undersökningen intervjuades tre rektorer och tre studie- och yrkesvägledare. Resultatet i min undersökning visar att om inte studie- och yrkesvägledningen implementeras som hela skolans ansvar kommer inte heller studie- ochyrkesvägledarna att utföra sitt uppdrag på ett tillfredsställande sätt. Vidare visar resultatet att det fanns en form av segregering av studie- och yrkesvägledningen eftersom den ansågs vara självständig och att de hade en otydlig profession.
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Spatial Distribution and Mobility of the Ran and the Bicoid proteins in Live SystemsAbu-Arish , Asmahan January 2008 (has links)
To the reader
<p> Since I worked on two separate projects towards my doctorate thesis, the arrangement of my thesis is rather unusual. The reader will find that my thesis is divided into four parts. Part 1 is dedicated to a very general introduction about the basic knowledge needed to guide you, the reader, through the rest of the thesis. Within this part, different sections focus on different fundamental aspects of Biophysics related to my work. In Part 2, I discuss my studies of the distribution and dynamics of the nuclear protein Ran in live interphase HeLa cells. This part contains a background section specific to this project, the materials and methods used for this study, experimental results, a discussion of our findings, and it ends with conclusions. Part 3 is dedicated to the study of the dynamical mechanisms responsible for the establishment of the Bed protein concentration gradient along the anterior-posterior axis in live Drosophila melanogaster embryos. Again, a specific background section is included in this part, followed by the materials and methods used to perform this research, results, discussions and finally I will summarize my results to conclude this work. The last part, part 4, is rather short and contains the summary of the overall results of my work on both nuclear proteins with some emphasis on the similarities and differences in their dynamical behavior.</p> / Thesis / Doctor of Philosophy (PhD)
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Genetic and phenotypic characterisation of mumps virusShorrock, Claire Ann January 2000 (has links)
No description available.
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Calcium and MAP kinase regulation during the cell cycleLarman, Mark Graham January 2001 (has links)
No description available.
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Swelling-activated transport of diverse solutes in mammalian cellsHall, James Anthony January 1996 (has links)
No description available.
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Regulation of nuclear calcium in HELA and C6 glioma cells. / CUHK electronic theses & dissertations collectionJanuary 1998 (has links)
by Lui Po Yee Pauline. / Thesis (Ph.D.)--Chinese University of Hong Kong, 1998. / Includes bibliographical references (p. 211-222). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Mode of access: World Wide Web.
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