1 |
Ultrasonograms and Histological Findings of the Postmortem PancreasTANEHIRO, KENJI 03 1900 (has links)
No description available.
|
2 |
Combining gemcitabine with checkpoint kinase inhibitors to sensitize pancreatic tumorsSaini, Priyanka 13 October 2014 (has links)
No description available.
|
3 |
Efeito do silenciamento de SHOC2 na sobrevivência e no controle do estresse oxidativo em linhagens celulares de adenocarcinoma ductal pancreático / Effect of SHOC2 knockdown on survival and oxidative stress control in pancreatic ductal adenocarcinoma cell lines.Borges, Camilla Rodrigues Pereira 18 April 2018 (has links)
O Adenocarcinoma ductal pancreático (ADP) é o tumor pancreático mais comum e apresenta um dos piores prognósticos. A primeira alteração crítica que desencadeia o processo de progressão tumoral, é a ativação desregulada do gene KRAS, na qual está presente em 90% dos casos. Várias iniciativas terapêuticas buscaram como alvo direto a atividade da oncoproteína RAS, sem no entanto, obter resultados satisfatórios. Desta forma, a investigação de moléculas efetoras downstream às vias reguladas por RAS, poderiam resultar em estratégias mais eficazes. Dentre estas moléculas efetoras estão as MAPKs, que modulam diversos processos celulares essenciais para o desenvolvimento tumoral, onde a cascata RAS/RAF/MEK/ERK representa uma importante via canônica de transdução de sinais. A transdução de sinais desta via pode ser favorecida por proteínas conhecidas como proteínas de arcabouço, como SHOC2, funcionando como uma plataforma para ligação de RAS-RAF-1 e consequentemente potencializando sua ligação. KRAS, têm sido associado à regulação de vias metabólicas importantes, como a glicólise que interferem diretamente na capacidade de proliferação e sobrevivência celular, para o estabelecimento e manutenção da biologia tumoral. Assim, o objetivo deste trabalho foi investigar o papel da proteína SHOC2 na indução do estresse oxidativo e capacidade de sobrevivência de linhagens celulares de ADP. Foram realizados os ensaios de morte celular por apoptose, avaliação da capacidade clonogênica e quantificação dos níveis de glutationa e quantificação da produção de espécies reativas de oxigênio. As linhagens celulares MIA PaCa2 e PANC-1 apresentaram uma redução significativa da capacidade de formação de colônias. A taxa de apoptose induzida pelo tratamento com Gemcitabina não diferiu entre as linhagens modificadas para silenciar a função de SHOC2. No ensaio da quantificação dos níveis de glutationa e na produção de espécies reativas de oxigênio, os resultados não foram concordantes com o esperado. Para análise dos níveis proteicos de p-ERK1/2, podemos observar uma redução na sua expressão, mesmo se mostrando de maneira sutil. Os resultados sugerem que pode haver alguma relação entre o silenciamento de SHOC2, estresse oxidativo e sobrevivência, porém existem outras vias alternativas modulando este processo. / Pancreatic ductal adenocarcinoma (PDAC) is the most common pancreatic tumor and has one of the worst prognoses. The first critical change that triggers the process of tumor progression is the dysregulated activation of the KRAS gene, in which it is present in 90% of cases. Several therapeutic initiatives aimed directly at the activity of the RAS oncoprotein, without, however, obtaining satisfactory results. Thus, investigating downstream effector molecules on RAS-regulated pathways could result in more effective strategies. Among these effector molecules are MAPKs, which modulate several cellular processes essential for tumor development, where the RAS / RAF / MEK / ERK cascade represents an important canonical pathway for signal transduction. Signal transduction of this pathway may be favored by proteins known as scaffold proteins, such as SHOC2, serving as a platform for RAS-RAF-1 binding and hence potentiating its interaction. KRAS, have been associated with the regulation of important metabolic pathways, such as glycolysis, for the establishment and maintenance of tumor biology. Thus, the objective of this work was to investigate the role of SHOC2 in the induction of oxidative stress and survival capacity of ADP cell lines. Cell death assays were performed by apoptosis, and quantification of glutathione levels and the production of reactive oxygen species were performed. MIA PaCa2 and PANC-1 cell lines showed a reduction in colony formation capacity. Gemcitabine-mediated cell death by apoptosis has not been induced after SHOC2 knockdown. Also, the measurement of reactive oxygen species and quantification of glutathione levels did not reveal any change mediated by SHOC2. The analysis of ERK1 / 2 activation has shown a discrete reduction in its expression. The results suggest that there may be some relationship between SHOC2 silencing, oxidative stress and survival, but there are other alternative pathways modulating this process which needs claryfication.
|
4 |
Development and evaluation of new approaches for fluorescence-guided surgery and therapy of pancreatic ductal adenocarcinoma using orthotopic mouse modelsSaccomano, Mara 20 June 2016 (has links)
No description available.
|
5 |
Positron Emission Tomography in the Management of Neuroendocrine TumorsÖrlefors, Håkan January 2003 (has links)
<p>Neuroendocrine tumors (NET´s) are often characterized by overproduction of peptide hormones. In spite of pronounced clinical symptoms, the tumor lesions can be small and difficult to detect. The general aim of this thesis was to investigate, in vitro and in vivo, some of the potential monoamine pathways present in NET´s, using radiolabeled tracers for positron emission tomography (PET), with the intention to explore the value of PET-imaging in the management of NET´s.</p><p>We used the 11C-labeled serotonin precursor 5-hydroxy tryptophan (HTP) as the tracer for imaging of NET´s. More than 95% of the subjects displayed a high tracer uptake on PET and tumor detection rate with PET was higher in >50% of the patients compared both to computed tomography (CT) and somatostatin receptor scintigraphy (SRS). The primary tumor was imaged by PET in 84% (16/19), compared to 47% and 42% for SRS and CT, respectively. Tumor visibility was better with PET due to a higher tumor-to-background ratio and a better spatial resolution. There was a strong correlation (r = .907) between changes in urinary-5-hydroxy indole acetic acid and changes in transport rate of 11C-5-HTP during treatment, indicating the use of PET in treatment monitoring of NET´s. </p><p>Pretreatment with carbidopa decreased the urinary radioactivity concentration four-fold and significantly (p<0.001) increased the tumor tracer uptake. This greatly improved image interpretation and tumor lesion detection.</p><p>A screening for expression of monoamine pathways in NET´s revealed a high in vitro binding of the monoamineoxidase-A ligand harmine to tumor sections. PET examinations with 11C-harmine could visualize tumors in all patients, including non-functioning endocrine pancreatic tumors (EPT´s).</p><p>Finally, the in vitro turnover and in vivo distribution of the amino acids glutamate, glutamine and aspartate was investigated. Limited uptake in vivo indicates the lack of utility for these substances as PET-tracers for imaging and characterization of NET´s. </p>
|
6 |
Positron Emission Tomography in the Management of Neuroendocrine TumorsÖrlefors, Håkan January 2003 (has links)
Neuroendocrine tumors (NET´s) are often characterized by overproduction of peptide hormones. In spite of pronounced clinical symptoms, the tumor lesions can be small and difficult to detect. The general aim of this thesis was to investigate, in vitro and in vivo, some of the potential monoamine pathways present in NET´s, using radiolabeled tracers for positron emission tomography (PET), with the intention to explore the value of PET-imaging in the management of NET´s. We used the 11C-labeled serotonin precursor 5-hydroxy tryptophan (HTP) as the tracer for imaging of NET´s. More than 95% of the subjects displayed a high tracer uptake on PET and tumor detection rate with PET was higher in >50% of the patients compared both to computed tomography (CT) and somatostatin receptor scintigraphy (SRS). The primary tumor was imaged by PET in 84% (16/19), compared to 47% and 42% for SRS and CT, respectively. Tumor visibility was better with PET due to a higher tumor-to-background ratio and a better spatial resolution. There was a strong correlation (r = .907) between changes in urinary-5-hydroxy indole acetic acid and changes in transport rate of 11C-5-HTP during treatment, indicating the use of PET in treatment monitoring of NET´s. Pretreatment with carbidopa decreased the urinary radioactivity concentration four-fold and significantly (p<0.001) increased the tumor tracer uptake. This greatly improved image interpretation and tumor lesion detection. A screening for expression of monoamine pathways in NET´s revealed a high in vitro binding of the monoamineoxidase-A ligand harmine to tumor sections. PET examinations with 11C-harmine could visualize tumors in all patients, including non-functioning endocrine pancreatic tumors (EPT´s). Finally, the in vitro turnover and in vivo distribution of the amino acids glutamate, glutamine and aspartate was investigated. Limited uptake in vivo indicates the lack of utility for these substances as PET-tracers for imaging and characterization of NET´s.
|
Page generated in 0.0816 seconds