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Nitric oxide : a marker for inflammation in the lower urinary tract /Hosseini, Abolfazl, January 2004 (has links)
Diss. (sammanfattning) Stockholm : Karol. inst., 2004. / Härtill 5 uppsatser.
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Exposição ocupacional como fator de risco para disgnostico inicial de câncer de bexiga / Occupational exposure as a risk factor for early diagnosis of bladder cancerAdonias, Sanarelly Pires 01 July 2016 (has links)
Introdução: Ocupação foi identificada como o segundo fator de risco mais importante para o câncer de bexiga depois de fumar sendo responsável por até 20% de todos os cânceres de bexiga em países industrializados. Apesar dos esforços consideráveis para investigar ocupações em relação ao risco de câncer de bexiga, muitas não foram encontrados de forma consistente. Material e Métodos: Foram incluídos 200 pacientes com diagnóstico de câncer de bexiga entre os anos de 2009 e 2013. Foi aplicado um questionário para obter informações sobre a profissão, tempo de exposição e hábitos diários, sintomas, e também dados de doenças incluindo estágio, grau e número e tamanho de lesões. Os pacientes do Grupo 1 foram aqueles sem emprego previamente associados com o risco de câncer de bexiga. Grupo 2 representado pacientes em risco devido a profissões. Resultados: Os pacientes do Grupo 2 apresentaram uma proporção significativamente maior de pT2 CaB (P = 0,037), enquanto que os pacientes do grupo 1 apresentaram significativamente mais pTa (p = 0,002) da doença. Analisando preditores de pT2, a presença de ocupação aumento de alto risco por 2,80 vezes a chance de desenvolver uma doença invasiva. Ao analisar o grau do tumor descobriram que um tempo de exposição de 10 anos ou mais aumenta o risco de tumores de alto grau em 4,28 vezes (p = 0,001). Conclusão: Pacientes com história de exposição a agentes cancerígenos devido à sua atividade profissional podem estar em maior risco de desenvolvimento de tumores invasivos e aqueles que estão expostos a estes agentes para mais de 10 anos podem desenvolver doença de alto grau com mais freqüência. População em risco pode, portanto, beneficiar de rastreamento para o câncer de bexiga / Occupation was identified as the second most important risk factor for bladder cancer after smoking accounting for up to 20% of all bladder cancers in industrialized countries. Despite considerable efforts to investigate occupation against the risk of bladder cancer, many have not been found consistently. We included 200 patients diagnosed with bladder cancer between 2009 and 2013. A questionnaire was applied to obtain information about the profession, exposure time and daily habits, symptoms, and also diseases of data including stage, grade and number and lesion size. Patients in Group 1 were those without jobs previously associated with the risk of bladder cancer. Group 2 represented patients at risk because of professions. Group 2 patients had a significantly higher proportion of pT2 CaB (P = 0.037), whereas patients in group 1 had significantly more pTa (p = 0.002) of the disease. Analyzing predictors of pT2, the presence of high-risk occupation increases by 2.80 times the chance of developing invasive disease. In considering the degree of tumor found that a time of 10 or more years of exposure increases the risk of high-grade tumors in 4.28 times (p = 0.001). Patients with a history of exposure to carcinogens because of their duties may be at greater risk of developing invasive tumors and those who are exposed to these agents for more than 10 years can develop high-grade disease more often. Population at risk can therefore benefit from screening for bladder cancer
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Análise de expressão de micro RNA em carcinoma urotelial de bexiga / Analysis of micro RNA expression in bladder urothelial carcinomaDip Júnior, Nelson Gaspar 27 July 2012 (has links)
Introdução: O câncer de bexiga é a segunda neoplasia maligna mais frequente do trato urinário, com 386.000 casos estimados e 150.000 mortes para 2011 no mundo. Noventa e cinco por cento são carcinomas uroteliais (CUB) papilíferos não músculo-invasivos de baixo grau, que apresentam altas taxas de recidiva, mas raramente progridem. Tumores invasivos de alto grau representam 10-20% dos diagnósticos, são altamente agressivos levando à mortalidade elevada. O conhecimento das vias moleculares envolvidas na carcinogênese dessa neoplasia é importante para a identificação de novos marcadores para diagnóstico, acompanhamento, prognóstico e desenvolvimento de novas terapias alvo. Micro RNA (miRNA) são pequenas sequências não codificantes de RNA que regulam a expressão dos genes inibindo a tradução da proteína ou promovendo a degradação do RNA mensageiro, estando atualmente envolvidos em vários processos celulares fisiológicos e patológicos, incluindo o câncer. Objetivos: Caracterizar o perfil de expressão de miRNA no CUB, relacionando-o com os parâmetros prognósticos clássicos para a doença: grau histológico e estadiamento. Além disso, relacionar esse padrão de comportamento dos miRNA com a recidiva tumoral e sobrevida câncer-específica em pacientes tratados cirurgicamente para CUB. Material e Métodos: Catorze miRNA (miR-100, miR-10a, miR-21, miR-205, miR-let7c, miR- 125b, miR-143, miR-145, miR-221, miR-223, miR-15a, miR-16-1, miR-199a e miR- 452) foram isolados de espécimes cirúrgicos de 60 pacientes divididos em 2 grupos: 30 pacientes com CUB não invasivo (pTa) de baixo grau submetidos à RTU de bexiga, 30 com CUB invasivo (pT2-3) de alto grau submetidos à cistectomia radical. O grupo controle é representado por cinco pacientes portadores de bexiga normal sem CUB que realizaram tratamento cirúrgico aberto para tratamento da hiperplasia prostática benigna (HPB). O processamento dos miRNA envolveu três fases: (1) extração do miRNA com kit específico, (2) geração do DNA complementar e (3) amplificação do miRNA por PCR quantitativo em tempo real (qRT-PCR). A expressão de cada miRNA foi obtida através do cálculo 2- CT e os RNU-43 e RNU-48 foram utilizados como controles endógenos. Testes estatísticos foram aplicados para estudar as variáveis envolvidas e curvas de Kaplan-Meyer foram usadas para avaliar a sobrevida livre de recidiva (SLR) e sobrevida câncer-específica (SCE). Resultados: Dos 14 miRNA estudados a maioria apresentou subexpressão nos dois grupos de tumor analisados, com exceção do miR-10a para o grupo pTa de baixo grau e do miR-100, 21 e 205 para os tumores pT2/pT3 de alto grau, onde demonstraram-se superexpressos. Essas diferenças de expressão de miRNA entre os dois grupos foram estatisticamente. Quando estudamos a relação entre expressão de miRNA e a evolução dos pacientes através de curvas de sobrevida, observamos que maiores níveis de expressão do miR-21 relacionou-se com menor SLR para tumores pTa. Ainda, maiores concentrações de miR-10a e miR-145 se associaram com menor SLR e maiores níveis de miR-10a com menor SCE para tumores pT2-3. Conclusões: Demonstramos um predomínio de subexpressão de miRNA em xv carcinomas de bexiga. Os miR-100, miR-10a, miR-21 e miR-205 demonstraram diferenças no perfil de expressão para grau e estadiamento dentro dos dois grupos de tumor, sendo capazes de diferenciá-los. Maiores níveis de miR-21 se relacionaram com menor SLR para tumores pTa de baixo grau, enquanto maiores concentrações de miR-10a estiveram associadas com menor SLR e SCE para tumores pT2/pT3 de alto grau / Introduction: Bladder cancer (BC) is the second most common malignancy of the urinary tract, with 386,000 cases estimated and 150,000 deaths in 2011. Urothelial carcinomas (UC) represent 95% of BC cases, and knowledge of the molecular pathways associated with BC carcinogenesis is crucial to identify new diagnostic and prognostic biomarkers, and development of new target molecular therapies. MicroRNAs (miRNAs) are short non-coding RNA molecules that play important roles in the regulation of gene expression by acting directly on mRNAs, leading to either mRNA degradation or inhibition of translation, involved in many physiological and pathological processes, including cancer. Objectives: To characterize miRNAs expression profiles in UC, associating with classic prognostic factors: grade and stage. Moreover, correlate miRNA expression with tumor recurrence and survival. Material and Methods: Fourteen miRNAs (miR-100, miR-10a, miR-21, miR-205, miR-let7c, miR-125b, miR-143, miR-145, miR-221, miR-223, miR-15a, miR-16-1, miR- 199a e miR-452) were isolated from surgical specimens from 60 patients classified in two groups: 30 patients with low-grade non-invasive pTa UC that underwent TURB, 30 with high-grade invasive pT2/pT3 UC underwent radical cystectomy. The control group consists in five normal bladder tissue taken from patients that underwent retropubic prostatectomy to treat benign prostatic hyperplasia (BPH). miRNA processing involved three phases: (1) miRNA extraction by specific kits, (2) cDNA generation (3) miRNA amplification through qRT-PCR. Expression profiles were obtained by relative quantification determined by 2-ct method. Endogenous control were RNU-43 and RNU-48. Statistic tests were used to study the prognostic variables and Kaplan-Meyer curves were constructed to analyze disease-free (DFS) and disease-specific (DSS) survivals. Results: All miRNAs were underexpressed in both groups, except miR-10a in pTa and miR-100, 21 and 205 in pT2/pT3 tumors, that where over-expressed. miR-100, miR-21, miR-10a and miR-205 differentialy expressed in both groups and this differences were statistically significant. The Kaplan-Meyer survival curves showed that higher levels of miR-21 were related to shorter DFS for pTa group. Also, higher levels of miR-10a and miR-145 were associated with shorter DFS and higher levels of miR-10a were also related to shorter DSS in pT2/pT3 group. Conclusions: The majority of miRNA were shown to be underexpressed in bladder UC. miR-100, miR-10a, miR-21 and miR-205 were differentially expressed considering tumor grade and stage. The miRNA profile was able to distinguish pTa low grade and pT2-3 high grade tumors. Higher levels of miR- 21 were related to shorter DFS in pTa, while higher levels of miR-10a were associated with shorter DFS and DSS in pT2-3, high grade UC
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Estabelecimento de linhagens tumorais para estudos in vitro e in vivo de carcinoma urotelial da bexiga e adenocarcinoma de próstata / Establishment of tumor cell lines from prostate adenocarcinoma and bladder urothelial carcinoma, for in vitro and in vivo studiesPiantino, Camila Belfort 14 August 2009 (has links)
Introdução: Um dos principais obstáculos para compreensão dos eventos biológicos envolvidos no câncer é a falta de modelos adequados para o estudo in vitro em especial em relação ao câncer de próstata (CaP) e ao câncer de bexiga (CaB). Há um número limitado de linhagens celulares de CaP e de CaB sendo a maioria proveniente de tumores invasivos e metastáticos. Sabe-se ainda, que existem diferenças étnicas entre as populações quanto ao comportamento de neoplasias. Desta forma, a pesquisa baseada em linhagens de uma população homogênea seria fonte de resultados limitados, não contemplando a diversidade que sabidamente ocorre entre os diferentes grupos. Além desse aspecto, as linhagens celulares comerciais são na sua maioria adquiridas na Coleção Americana de Culturas de Tecido (ATCC, do inglês American Tissue Cell Culture) que apesar de serem bem padronizadas, requerem processos de importação com aumento do custo e demandas burocráticas que dificultam a pesquisa. Portanto, consideramos vital para a compreensão dos fenômenos relacionados à carcinogênese, assim como estudos de resistência a drogas, quimioprevenção e novas estratégias terapêuticas, o desenvolvimento de linhagens tumorais derivadas de tumores primários que acometem a nossa população, peculiarmente miscigenada. No presente trabalho, fragmentos de carcinoma urotelial da bexiga e de adenocarcinoma da próstata foram obtidos durante cirurgia para remoção de tumores primários de pacientes tratados e acompanhados na Divisão de Urologia da Faculdade de Medicina da Universidade de São Paulo (FMUSP) e no Hospital Sírio Libanês. As linhagens estabelecidas a partir destes fragmentos foram caracterizadas através da análise da cinética de crescimento, análises imunocitoquímicas e anormalidades cromossômicas incluindo cariótipo e hibridização in situ por fluorescência (FISH). Além disso, as linhagens obtidas foram submetidas a estudos de quimiossensibilidade com o uso dos compostos curcumin e Prima-1. Avaliamos ainda, a tumorigenicidade de nossas linhagens em camundongos atímicos. Os resultados deste trabalho demonstram o desenvolvimento de três linhagens de CaB e três linhagens de CaP sendo as mesmas não tumorigênicas em camundongos atímicos. Além disso, demonstramos que o curcumin na concentração de 50 M induziu morte celular em todas as linhagens estudadas, sendo seu efeito mais evidente nas linhagens de CaP. Por fim, Prima-1 reduziu a viabilidade celular independente do status de p53 nas linhagens de CaB / Introduction: One of the main obstacles for understanding biological events involved in cancer is the lack of appropriated models for in vitro studies especially for prostate cancer (PC) and bladder cancer (BC). There are a limited number of PC and BC cell lines being the majority originated from metastatic and invasive tumors. Also it is well known that there are ethnic differences between populations concerning the behavior of tumors. In such a way, the research based on cell lines derived from a homogenous population should be source of limited results, not contemplating the diversity known to occur among different groups. In addition the commercial cell lines are generally acquired at American Tissue Cell Culture (ATCC) that although wellestablished requires importation processes with cost increase and bureaucratic demands that difficult the research. Therefore we consider vital to the comprehension of the carcinogenesis phenomena, as well as drug resistance studies, chemoprevention and new therapeutic strategies, the development of tumor lineages derived from primary tumors that assail our miscigenated population. At the present work, fragments of bladder urothelial carcinoma and prostate adenocarcinoma were obtained by surgical resection of primary tumors from patients treated and followed in the Division of Urology of the Clinical Hospital of the São Paulo University (FMUSP) and Syrian Lebanese Hospital. The cell lines established from these fragments were characterized through growth kinetic, immunocytochemistry and chromosome abnormalities including karyotyping and Fluorescence in situ hybridization (FISH). Moreover, the cell lines were submitted to chemosensitivity studies using curcumin and Prima-1 and analyzed regarding their tumorigenicity in athymic mice. The results of this work show the development of three BC and three PC cell lines that were not tumorigenic in athymic mice. Curcumin at 50 M concentration induced cell death in all studied lineages, being more effective in PC cell lines. Finally, PRIMA-1 reduced the cellular viability independent of the p53 status in BC cell lines
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A morphological and molecular study of bladder cancer in a rat model induced by N-butyl-N-(4-hydroxybutyl) nitrosamine and human bladder cancer: with special focus on the changes in mitochondria and mitochondrial DNA. / CUHK electronic theses & dissertations collectionJanuary 2002 (has links)
Guang Fu Chen. / "May 2002." / Thesis (Ph.D.)--Chinese University of Hong Kong, 2002. / Includes bibliographical references (p. 194-221). / 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. / Abstracts in English and Chinese.
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Mouse orthotopic model for therapeutic bladder cancer research.January 2014 (has links)
Objectives: To establish a mouse orthotopic bladder cancer model with consistent tumor-take rate. This orthotopic model was subsequently used to evaluate small animal imaging techniques and investigate new therapeutic agents for bladder cancer treatment. / Materials and Methods: Different orthotopic implantation techniques have been tested. MBT-2 cells and syngeneic C3H/He mice were used in all experiments. Chemical bladder pre-treatment with different agents (saline, hydrochloric acid, trypsin and poly-L-lysine) and different concentration of instilled tumor cells (1 x 10⁶ or 2 x 10⁶) were investigated. In the second part of the experiment, trans-abdominal micro-ultrasound imaging (MUI) technique was investigated and validated. Bladder tumor growths were monitored with longitudinal measurement. Mice were killed at every MUI session. Bladder tumor volumes were measured and correlated with gross stereomicroscopy. Using the optimized orthotopic bladder cancer model, targeted contrast enhanced micro-ultrasound imaging has been investigated. VEGFR2 targeted contrast agent was prepared and injected intravenously before imaging sessions. The intra-tumoral perfusion, VEGFR2 expression and blood volume in real time were quantified. Contrast enhanced MUI was performed on Days 14 and 21. The feasibility of targeted contrast enhanced micro-ultrasound imaging was confirmed. After the establishment of orthotopic model and in vivo molecular imaging techniques, this robust platform was used for investigating new treatment agent in localized bladder cancer. Tumor-bearing mice were randomized into control and sunitinibtreated (40 mg/kg) groups. Tumor volume, intra-tumoral perfusion, and in vivo VEGFR2 expression were measured using a targeted contrast-enhanced micro-ultrasound imaging system. The effects of sunitinib malate on angiogenesis and cellular proliferation were measured by CD31 and Ki-67 immunohistochemistry. The clinical outcomes including total bladder weight, tumor stage, and survival were evaluated. / Results: A consistent tumor take-rate of over 90% was achieved by using poly-L-lysine pretreatment with 2 x 10⁶ MBT-2 cells in all of the experiments. MUI identified all tumors that were present on final histology. Measurements of tumor size by MUI and gross microscopy had a high correlation coefficient (r = 0.97). Measurements of intra-tumoral perfusion and in vivo VEGFR2 expression were also proved to be feasible. After the technical refinement and modification, complete measurements could be performed in all mice (n = 10) at 2 consecutive imaging sessions. No adverse effects occurred due to anesthesia or the ultrasound contrast agent. This is the first report of applying targeted contrast enhanced MUI in orthotopic bladder cancer model. Finally, sunitinib was found to have significant tumor growth inhibition in both in vitro and in vivo experiments. In the orthotopic model, tumors in sunitinib-treated mice had reduced tumor volume and stage, lower proliferation index and micro-vessel density. Sunitinib prolonged survival in tumor-bearing mice as compared to control group. / Conclusions: The development of reliable orthotopic animal models assists in the discovery of novel therapeutic agents. The establishment in the methods of implantation with improved tumor-take rate and the advances in imaging technology form the important foundation of basic research in bladder cancer. Trans-abdominal MUI is proven to be a valuable tool for translational studies involving orthotopic mouse bladder cancer models. Furthermore, the first report of the application of targeted contrast enhanced MUI in deep-seated tumor in bladder has been published. It enables investigators to monitor tumor angiogenesis and vascular changes after treatment. It will be useful for direct, noninvasive, in vivo evaluation of anti-angiogenesis therapeutic agents. The preclinical study has demonstrated the activities of a new class of targeted therapy against localized bladder cancer in an orthotopic mouse model. Sunitinib inhibits tumor growth and thus decreases the tumor burden and prolongs survival compared with placebo. These results provide a rationale for future clinical trials using VEGFR-targeted treatments of localized bladder cancer in the neo-adjuvant and adjuvant settings. / Chan, Shu Yin Eddie. / Thesis (M.D) Chinese University of Hong Kong, 2014. / Includes bibliographical references (leaves 189-212).
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Time Interval to Diagnosis of Bladder Cancer and Its Associated OutcomesSuh, Lara K. 08 September 2008 (has links)
The purpose of this study is to investigate whether a prolonged delay in diagnosis of bladder cancer will result in worse outcomes for those patients, compared to those patients with a shorter diagnostic time interval. Data was collected on 247 patients newly diagnosed with transitional cell carcinoma of the bladder from January 1996 to December 2006 (10 years). The medical records of these patients were reviewed for demographics, pathological stage, date of consultation to the genitourinary (GU) service, and date of diagnosis by transurethral resection of bladder tumor (TURBT). The specialty delay was calculated as the time between the date of consultation to the GU service to the establishment of a diagnosis by TURBT. Univariate analyses were performed to test the association of specialty delay with clinical features and all-cause mortality. The median specialty delay in this study was 100 days. There was a trend towards a longer specialty delay for muscle-invasive disease (T2-T4) in comparison to superficial disease (Ta and T1). There was a significant correlation between all-cause mortality and increasing clinical stage (p=0.01). There was a paradoxical finding that patients with a specialty delay greater than 100 days had a significant reduction in all-cause death in comparison to patients with a specialty delay of 100 days or less (relative risk=0.59; 95% CI 0.36-0.90; p=0.01). In conclusion, this study did not confirm the hypothesis that a prolonged specialty delay in patients diagnosed with bladder cancer would result in a worse prognosis. In fact, there was a paradoxical finding that patients with a specialty delay greater than the median delay of 100 days had a better prognosis.
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Molecular changes in the tumour suppressor genes p53 and CDKN2A/ARF in human urinary bladder cancer /Berggren, Petra, January 2002 (has links)
Diss. (sammanfattning) Stockholm : Karolinska institutet, 2002. / Härtill 5 uppsatser.
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The role of Ral GTPases and their targets in human bladder cancerSmith, Steven Christopher. January 2008 (has links)
Thesis (Ph. D.)--University of Virginia, 2008. / Title from title page. Includes bibliographical references. Also available online through Digital Dissertations.
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Epigenetic crosstalk between DNA demethylation and histone acetylationOu, Jing-Ni. January 1900 (has links)
Thesis (Ph.D.). / Written for the Dept. of Pharmacology & Therapeutics. Title from title page of PDF (viewed 2009/06/10). Includes bibliographical references.
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