Global ETD Search

61	Detección de papiloma virus humano y genes supresores tumorales P16 y P53 en carcinomas de región genital extena Godínez Martínez, José Manuel 29 July 2008 (has links) La implicación del papiloma virus humano (HPV) en carcinomas de cérvix está totalmente demostrada, pero esta infección se puede producir en otras regiones anatómicas con similares consecuencias patológicas. El estudio presenta la detección de HPV en carcinomas de pene y vulva mediante PCR, analizando la sensibilidad de diferentes sistemas, primers GP5+/6* y MY09/11. También se lleva a cabo la detección inmunohistoquímica de proteínas celulares como posibles marcadores diagnóstico de infección por HPV, las proteínas P53 y P16 su expresión supuestamente se altera por la infección de HPV en carcinomas de pene (77,5%), mientras que en los carcinomas de vulva la tasa de detección está dentro de los rangos esperados según trabajos previos publicados (29, 7). El estudio de la relación entre la presencia de HPV y la expresión de los marcadores celulares muestra su no asociación en estas patologías. / The infection of human papilloma virus (HPV) is clearly related with cervical carcinomas, but this infection can be found in other regions whit PCR, analyzing the sensitivity of HPV in penile and vulvar carcinomas whit PCR, analyzing the sensitivity of two differents systems, MY09/11 and GP 5+/6+. Also the immunohistochemical detection of cell proteines as diagnostic markers for the HPV in penile carcinomas in the study populations (77,5%), whereas in vulgar carcinomas . The detection rates is similar to the previously published data ( 29, 7%). The study of the relatioship between HPV and the expression of the cell markers shows no asocciation with the pahologies. HPV Human Papilloma Virus Inmunohistoquímica PCR Cáncer Carcinoma genital Papiloma virus humano Carcinoma genital. Immunohistochemistry Histología y Patología Molecular 576 577 616
62	Výskyt karcinomu děložního čípku u žen v Jihočeském kraji / Occurrence of woman cervical cancer in South Bohemian Region. NĚMCOVÁ, Eva January 2009 (has links) Cervical cancer represents an enormous health, psychological and social stress for every woman. The most important risk factor in the development of cervical carcinoma, which the second most common malignant cancer in women, is infection with a high-risk strain of human papillomavirus - a very frequent sexually transmitted disease. More than 100 types of HPV are acknowledged to exist, with HPV 16 and 18 being classified as high-risk types in particular. Worldwide, 500,000 new cases of cervical cancer are diagnosed every year. In the Czech Republic, there are 1,000 new cases of cervical cancer each year, out of which up to 400 women die. It is estimated that there will be up to 1,000,000 new cases of cervical cancer by 2050 unless the prevention is improved. Every woman is at risk of developing cervical cancer. HPV is sexually transmitted, however not only by sexual intercourse but also by skin-to-skin-contact with infected areas. Other risk factors in the development of the disease are: first sexual intercourse at early age, the number of sexual partners, smoking, other sexually transmitted diseases and a long term use of hormonal contraception. Use of condoms, which protects against sexually transmitted diseases, reduces the transmission of HPV by up to 70%. Having regular gynaecological check-ups with Pap smears is crucial for cervical cancer screening, as the screening suggests the presence of cytological abnormalities and pre-cancer. However, it cannot detect all types of premalignant changes and early stages of the carcinoma. Two vaccines have recently been developed, effective against the most frequent oncogenic strains of HPV (16 and 18), which currently cause about 70% of cervical cancer cases. Active immunisation against human papillomavirus is the first vaccination against carcinoma. Together with screening, it represents the best prevention method against cervical carcinoma. Based on the research of technical literature, the first part of the dissertation gives an overall view of the issue of cervical carcinoma. The second part of the dissertation deals with the research, eliciting the knowledge and attitude of women from Southern Bohemian towns in the field of cervical carcinoma prevention in the period of December 2008 - March 2009 and comparing it to technical literature.
63	Potencial oncogênico de variantes naturais de papilomavírus humano / Oncogenic potential of natural variants of human papillomavirus Laura Sichero 19 December 2003 (has links) O principal fator etiológico da neoplasia do colo do útero é a infecção por HPVs (papilomavírus humano) de alto risco oncogênico, principalmente HPVs 16 e 18. A variabilidade intra-típica de ambos tipos virais tem sido extensivamente estudada. A análise da diversidade genética de isolados oriundos de diferentes regiões dos cinco continentes permitiu traçar a origem e filogenia destes vírus, e sugeriu-se que a evolução destes reflete a relação dos mesmos com seu hospedeiro. Considera-se uma variante molecular de um tipo de HPV um genoma que possui 98% ou mais de identidade nos genes Ll , E6 e E7 com um genoma já descrito. Entretanto, variantes moleculares apresentam aproximadamente 5% de diferença na seqüência da LCR (long contral region). Alguns grupos de pesquisa de diferentes partes do mundo relataram a associação epidemiológica entre variantes específicas de HPVs 16 e 18 e o risco aumentado de infecção persistente e de desenvolvimento de lesão do colo uterino de alto grau. No Brasil foi observada a associação positiva entre variantes não-européias de HPVs 16 e 18 e o risco de lesão do colo uterino em um estudo epidemiológico prospectivo que vem sendo conduzido em São Paulo. Neste estudo foi analisada a atividade transcricional dos promotores P97 e P105 de variantes moleculares de HPVs 16 e 18, respectivamente. A variante asiático-americana de HPV-18, B18-3, apresentou a maior atividade transcricional entre todos os isolados testados. Entre as variantes moleculares de HPV-18, o isolado europeu B18-2 foi o menos ativo transcricionalmente. Entre as amostras de HPV-16, a variante européia B-12 foi a que apresentou a maior atividade transcricional. Foi observado, também, que o promotor P105 de HPV-18 é mais ativo transcricionalmente que o promotor P97. Adicionalmente, foi analisada a capacidade de imortalização de queratinócitos humanos primários por E6/E7 de variantes moleculares de HPV-16. Essas variantes não diferiram muito quanto a eficiência de formação de colônias de queratinócitos crescidos em baixa densidade. Entretanto, a variante asiático-americana gerou um maior número de colônias potencialmente imortalizadas. Esses resultados têm implicações importantes na determinação do risco de desenvolvimento de lesões de colo uterino associadas ao HPV. / Infection by high-risk HPV (human papillomavirus) types, especially HPVs 16 and 18, is the major etiological factor of cervical neoplasia. Intratypic nucleotide variability of both HPV types has been extensively studied. Genetic diversity analyses of isolates from different regions of the five continents permitted to reconstruct the origin and phylogeny of this virus, and suggested that viral evolution reflects the relation between the virus and their host. A molecular variant of HPV possess 98% or more identity in L1, E6 and E7 genes with another viral genome. However, molecular variants have approximately 5% differences within the LCR (long control region). Some research groups from different parts of the world have described the epidemiologic association between specific variants of HPVs 16 and 18 and increased risk of persistent infection and development of squamous intraepithelial lesions. In Brazil, we observed a positive association between non-European variants of HPVs 16 and 18 and risk of cervical lesion in a prospective epidemiologic study that is being conducted in São Paulo. In this study we analyzed P97 and P105 transcriptional activity of molecular variants of HPVs 16 and 18, respectively. The Asian-American variant of HPV-18, B18-3, exhibited the highest transcriptional activity among all isolates tested. Among HPV-18 molecular variants, the B 18-2 European isolate was the less transcriptionally active. Among HPV-16 samples, the B-12 European variant exhibited the highest transcriptional activity. We also observed that the HPV-18 P105 promoter was more active than the HPV-16 P97 promoter. Furthermore, we analyzed the capacity of immortalization of primary human keratinocytes by E6/E7 molecular variants of HPV-16. These variants did not differ much in the efficiency of colony formation by low density keratinocyte plating. However, the Asian-American variant yielded a higher number of colonies potentially immortalized. These results have important implications in the determination of risk for development of HPV -associated cervical lesions. Atividade biológica Atividade transcricional Câncer cervical Neoplasias do colo uterino (Estudo) Papiloma Papilomavírus Potencial oncogênico Transformação Vírus oncogênicos Cervical neoplasms (Study) Oncogenic viruses Papilloma
64	Avaliação imunoistoquimica de celulas mioepiteliais no diagnostico diferencial de lesões benignas e malignas da mama / Immunohistochemical assessment of myoepithelial cells in the differential diagnosis of benign and malignant lesions of the breast Schenka, Natalia Guimarães de Moraes 30 June 2006 (has links) Orientador: Jose Vassalo / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-08-07T05:09:42Z (GMT). No. of bitstreams: 1 Schenka_NataliaGuimaraesdeMoraes_D.pdf: 3809756 bytes, checksum: d4d7db8aeacfcd3c285cdee5b7c0a182 (MD5) Previous issue date: 2006 / Resumo: O sistema ductal da mama é revestido por duas camadas de células: uma constituída de células epiteliais luminais e outra de células mioepiteliais (CME). A identificação das CMEs é de grande importância na rotina em patologia cirúrgica, já que estas estão presentes em lesões benignas e geralmente ausentes nas malignas. Contudo, esta identificação morfológica (i.e., à hematoxilina-eosina) pode tornar-se difícil, sendo necessários marcadores imunoistoquímicos mioepiteliais. Até o momento, nenhum marcador mostrou-se, isoladamente, sensível e específico o bastante para auxiliar de maneira fidedigna em dilemas diagnósticos específicos, especialmente em: (1) lesões esclerosantes benignas vs. carcinoma tubular e (2) neoplasias papilíferas. No presente trabalho, dois novos marcadores mioepiteliais (p63 e CD10) foram testados e comparados com marcadores tradicionalmente empregados em patologia cirúrgica (1A4 e calponina). No primeiro dilema diagnóstico, foram estudados 10 casos de adenose esclerosante, 10 casos de cicatriz radiada e 10 casos de carcinoma tubular. Todos os marcadores demonstraram expressão nas CMEs de todas as lesões benignas e foram consistentemente negativos nos casos de carcinoma tubular, porém, p63 e CD10 mostraram maior especificidade. Os marcadores tradicionais mostraram positividade em células estromais em todos os casos de carcinoma tubular, sendo que esta reação-cruzada poderia causar problemas de interpretação ao simular uma camada de CMEs em quatro casos. Contudo, 1A4 mostrou uma positividade mais intensa e reprodutível nas CME. Concluímos, assim, que p63 e CD10 devem ser usados como anticorpos complementares ao 1A4 na distinção entre lesões esclerosantes benignas e carcinoma tubular da mama. No estudo das neoplasias papilíferas, foram avaliados 20 casos incluindo papilomas, papilomas atípicos e carcinomas papilíferos, além do tecido mamário normal adjacente. Todos os marcadores foram difusamente positivos no tecido mamário normal e papilomas, indicando sensibilidades semelhantes na identificação de CME. Uma positividade intensa foi encontrada em 100% dos casos corados para 1A4 e CD10, mas em apenas 76% e 60,5% dos corados para calponina e p63, respectivamente, sendo as diferenças estatisticamente significantes (p<0.05). Este dado sugere que os dois primeiros são tecnicamente mais reprodutíveis. Os marcadores mais específicos foram o p63 e CD10, mostrando reação-cruzada com células estromais em 0 e até 33% dos casos, respectivamente. Já os marcadores 1A4 e calponina mostraram reação-cruzada difusa em todos os casos. O CD10 mostrou uma combinação de uma maior especificidade e reprodutibilidade, com uma boa sensibilidade. Apesar de ser o mais específico, o p63 apresentou a menor sensibilidade e a impressão de uma camada de CMEs variavelmente interrompida (mesmo em tecido normal e lesões benignas), o que poderia causar problemas de interpretação. Além disto, o 1A4 mostrou-se também neste contexto, como o mais reprodutível tecnicamente. Assim sendo, no dilema diagnóstico das neoplasias papilíferas, defendemos o uso combinado do marcador CD10 com o 1A4. Em resumo, apesar de variarem em acurácia diagnóstica quando comparados entre si e com marcadores tradicionais, na dependência do dilema considerado, os novos marcadores testados neste trabalho parecem promissores no diagnóstico diferencial de lesões benignas e malignas da mama / Abstract: The myoepithelial cell (MEC) layer is usually present and continuous in normal breast tissue/benign lesions, and discontinuous to absent in atypical/malignant counterparts. Identifying MECs can be difficult on morphological grounds alone and currently relies on immunomarkers. So far, this detection has been carried out using antibodies such as alpha-smooth muscle actin (1A4) and calponin, but no immunomarker has proved to be accurate enough to identify MECs, particularly in specific diagnostic dilemmas such as: (1) benign sclerosing lesions vs. tubular carcinoma and (2) papillary neoplasms. The specificity of these markers has been questioned because they may be expressed in stromal myofibroblasts and vascular smooth muscle. Two novel myoepithelial markers have been described: the nuclear protein p63 and the surface antigen CD10. In the present study, we assessed the use of p63 and CD10 in comparison to the traditional markers in the specific diagnostic dilemmas specified above. In the first diagnostic problem, we studied 30 cases including sclerosing adenosis, radial scars and tubular carcinomas. All markers were expressed in MECs of all benign lesions and negative in all cases of tubular carcinoma. p63 and CD10 were mostly confined to MECs and thus more specific. Stromal positivity for 1A4 was present in all cases of tubular carcinoma and was misleading in 4 cases, as it simulated a MEC layer around malignant tubules. However, 1A4 was consistently more intensely expressed and thus more technically reproducible than the novel markers. So, we concluded that p63 and CD10 should be used as a complement to 1A4 in distinguishing benign sclerosing lesions from tubular carcinoma of the breast. Concerning the other diagnostic dilemma, we studied 20 cases of papillary neoplasms (including benign papillomas, atypical papillomas and papillary carcinomas), and adjacent normal breast tissue. All markers were diffusely positive in all samples of normal tissue and benign papillomas indicating similar sensitivities in the identification of MECs. Intense positivity was found in 100% of the cases stained with 1A4 and CD10, but in only 76% and 60,5% of those stained with calponin and p63, respectively; the differences were statistically significant (p<0.05), suggesting that the former two rendered more reproducible results. The most specific markers were p63 and CD10 which showed cross-reactivity in 0% and in up to 33% of the cases, respectively. 1A4 and calponin showed diffuse cross-reactivity in all cases. CD10 seems to combine the highest specificity and reproducibility with a good sensitivity. In spite of being the most specific, p63 was the least sensitive, also giving the impression of a discontinuous MEC layer even in normal tissue/benign lesions, which could potentially cause diagnostic problems. Moreover, in this context, 1A4 proved to be the most reproducible. Thus, a minimum panel for immunodetection of MEC to assess papillary lesions should include both markers. In conclusion, in spite of the variable accuracy depending on the diagnostic dilemma considered, the novel markers seem to be promising tools in the differential diagnosis between benign and malignant lesions of the breast / Doutorado / Anatomia Patologica / Doutor em Ciências Médicas Carcinoma papilar Papiloma Mioepitelioma Celulas mioepiteliais Mamas Imuno-histoquímica Adenose esclerosante Papillary neoplasms Papilloma Breast Sclerosing adenosis Myoepithelial cells Immunohistochemistry Tubular carcinoma
65	Estudo clínico, epidemiológico, histológico de papilomas de mucosa oral e sua relação com Papilomavírushumano (HPV) através das técnicas de hibridização in situ e PCR / Clinic, epidemiologic, histologic study of oral papillomas and its relation to Humanpapillomavirus (HPV) by In Situ Hybridization and PCR Angelo Rafael Calabria Tancredi 07 December 2007 (has links) O Papilomavírushumano (HPV) é um DNA vírus do grupo papovavírus, que é altamente transmissível sexualmente, sendo bastante encontrado na região anogenital e mucosa oral. A sua implantação oral pode ser por auto-inoculação ou pelo contato oro-sexual. As principais manifestações orais associadas ao HPV são: papiloma, condiloma acuminado, verruga vulgar e hiperplasia epitelial focal. O papiloma é uma lesão epitelial associada ao HPV e pode ocorrer em vários locais da mucosa oral. Histopatologicamente, o papiloma oral é caracterizado por coilocitose, disceratose, papilomatose, hiperceratose e acantose. A literatura ressalta a importância do estudo dessas lesões, uma vez que estudos demonstram que mesmo com os achados macroscópicos e histológicos serem compatíveis com a presença do vírus, somente técnicas de detecção podem comprovar a presença viral.O objetivo deste estudo foi verificar a presença do HPV, por meio das técnicas de hibridização in situ e PCR, em lesões diagnosticadas histopatologicamente como papilomas e comparar esses resultados com características clínicas e histológicas. Cinqüenta casos foram selecionados da Disciplina de Patologia Bucal e da Disciplina de Estomatologia Clínica da FOUSP. Esta seleção de 50 casos foi submetida à reação de hibridização in situ, e 10 casos dentre os mesmos por técnica da PCR e 100% casos foram negativos. Nenhuma das características histológicas previamente analisadas puderam formar estreita relação com a hibridização in situ e PCR. Conclui-se que a análise histopatológica ao HE não se correlaciona com os resultados das técnicas de hibridização in situ e PCR, porém importante ressaltar para detecção do HPV nas lesões estudadas é imprescindível o uso de técnicas de Biologia Molecular otimizadas como a hibridização in situ e PCR realizadas nesse estudo. / The Humanpapillomavirus (HPV) is a DNA virus from the group of papovavirus, which is highly sexually transmitted and it can be often found in the anogenital area and in the oral mucosal. The oral implantation can be by self-inoculation or by the oral sexual contact. The main oral appearances associated to HPV are: papilloma, condylomata acuminata, verruca vulgaris and focal epithelial hyperplasia. Papilloma is an epithelial lesion that is associated to HPV and can occurs in many places of the oral mucosal. Histopathologically, the oral papilloma is characterized by koylocitosis, dyskeratosis, papillomatosis, hyperkeratosis and acanthosis. The literature shows the importance of these lesions once studies show that macroscopic and histologic founds suggest the presence of the virus, only detection technics can prove the viral presence. The target of this study is to check the presence of HPV, by means of In situ hybridization and PCR, in lesions diagnosed histopathologically as papillomas and compare these results with clinic and histologic features. Fifty cases were selected from the Discipline of Oral Pathology and the Discipline of Oral Diagnose of FOUSP. This selection of 50 cases were submitted to the reaction of In situ hybridization, and 10 cases among the same by PCR and 100% of the cases were negative. None of the histologic features were previously analyzed could form a narrow relation with the In situ hybridization and PCR. Therefore it is concluded that the histopathologic analysis to HE do not correlate with the results of the In situ hybridization and PCR, however the detection of the HPV in the studied lesions it is absolutely necessary the use of Molecular Biology techniques as the In situ hybridization and PCR done in this study. Diagnóstico histopatológico Diagnóstico molecular Hibridização in situ Papiloma oral Papilomavírushumano (HPV) PCR Histopathologic diagnose Humanpapillomavirus (HPV) In situ Hybridization Molecular diagnose Oral papilloma PCR
66	Polimorfismo do códon 72 do gene p53 e risco de infecções persistentes por papiloma vírus humano (HPV) e neoplasia do colo uterino / Polymorphism of codon 72 of the p53 gene and risk of persistent human papillomavirus (HPV) infections and cervical neoplasia Rabachini, Tatiana 20 December 2002 (has links) Nos últimos anos, inúmeros estudos epidemiológicos evidenciaram a forte associação entre o carcinoma do colo uterino e a infecção por papilomavírus humano (HPV). Esta associação deriva do reconhecimento de que estes vírus codificam oncoproteínas, dentre as quais E6 e E7, que apresentam propriedades transformantes. O produto do gene E7 se liga ao produto do gene retinoblastoma que perde a sua função de regular negativamente o ciclo celular. O produto do gene E6 se liga ao produto do gene supressor de tumor p53 levando a sua degradação pela via de proteólise dependente de ubiquitina. O gene p53 é um supressor tumoral com função de regulação do ciclo celular que apresenta vários polimorfismos distintos em diversos grupos étnicos e tem sido amplamente estudado tanto em tecidos normais quanto em tecidos tumorais. O polimorfismo do códon 72 do gene i>p53 é o mais estudado e pode apresentar três alelos diferentes na população. Um alelo codifica arginina (Arg), um codifica prolina (Pro) e outro, raramente encontrado, codifica cisteína (Cys). Em 1993 foi iniciado um estudo epidemiológico da história natural da infecção por HPV e neoplasia da cérvice uterina em uma população feminina de baixa renda em São Paulo (Brasil), uma das áreas de maior risco em todo o mundo. O estudo focaliza a infecção persistente por tipos oncogênicos de HPV como evento precursor que leva à carcinogênese do colo do útero e visa entender os atributos da história natural da infecção viral e das doenças associadas ao colo uterino. Um dos objetivos deste estudo é avaliar se o polimorfismo do códon 72 do gene p53 pode, ou não, ser utilizado como marcador de predisposição ao câncer do colo do útero uma vez que um estudo inicial relatou que pacientes portando o genótipo p53Arg homozigoto seriam 7 vezes mais susceptíveis ao desenvolvimento de neoplasia da cérvice uterina que pacientes contendo o genótipo p53Pro e heterozigoto p53Pro/ Arg. Contudo, vários estudos posteriores contradizem e corroboram esses achados. O presente projeto teve como objetivos, portanto, verificar se o polimorfismo do códon 72 do gene p53 poderia estar associado a infecções persistentes por HPV e ao risco de neoplasia do colo do útero, além de comparar metodologias de detecção utilizadas por outros estudos, visando esclarecer se os motivos que levam à discordância dos resultados podem ser atribuídos a ocorrência de erros classificatórios metodológicos. Ao todo, sete metodologias de detecção foram comparadas. Apenas uma delas, PCR alelo-específica, apresentou resultado discordante das demais utilizadas. Coincidentemente, essa metodologia foi amplamente utilizada por muitos estudos que encontraram associações tanto positivas quanto negativas. Isso poderia nos dar indícios de que os erros classificatórios dependentes de metodologia poderiam influenciar os resultados de correlação entre o polimorfismo do códon 72 e o risco de neoplasia do colo do útero. As correlações observadas por este trabalho entre este polimorfismo do códon 72 e o risco de neoplasia do colo uterino não mostraram associação deste polimorfismo com o risco de infecções persistentes por HPV e as lesões precursoras do carcinoma do colo uterino. / In recent years, a number of epidemiological studies have pointed toward a strong association between cervical cancer and infection by Human Papillomavirus (HPV). This association derives from the discovery that these viruses code for oncoproteins, among them E6 and E7 that have transforming properties. The E7 gene product associates with the retinoblastoma gene product, causing the latter to lose its function as a negative regulator of the cell cycle. The E6 gene product interacts with the tumor suppressor p53 gene product, resulting in its degradation via ubiquitin dependent proteolysis. The p53 gene is a tumor suppressor that funcions in the regulation of the cell cycle. It presents a number of distinct polymorfisms in diverse ethnic groups, and has been widely studied, both in normal and tumor tissues. The polymorfism of codon 72 is the most studied, and may present three different alleles in the population. One allele codes for arginine (Arg), another codes for proline (Pro), and a third, rarely found, codes for cystein (Cys). In 1993 an epidemilogical study of the natural history of infection by HPV and its possible association with cervical neoplasia was initiated in a population of low income females in São Paulo, Brazil, one of the areas of greatest risk in the world. The study focuses on persistent infection by oncogenic types of HPV as a precursor to carcinogenesis of the cervix, and seeks to understand the attributes of the natural history of viral infection and of illnesses associated with the cervix. One of the objectives of the study is to evaluate if the polymorfisms of codon 72 of p53 can or not be used as a marker of predisposition to cervical cancer, given the finding in the initial study that patients who were homozygous for the p53Arg genotype were 7 times more susceptible to developing cervical neoplasias than those patients who were homozygous for p53Pro, or heterozygous p53 Pro/ Arg. Previous studies have been realized both supporting and disputing these findings. The current study had two main objectives: to verify if the polymorfism of p53 codon 72 could be associated with persistent infections of HPV and the risk of cervical neoplasia, as well as to compare methods of detection used by other studies, in an attempt to clarify if the discording results of past studies could be due to methodological classification errors. Seven detection methods were compared. Only one of these, allele specific PCR, presented discording results from the rest. Coincidentally, this method was widely used in a number of studies which found both positive and negative associations. This might indicate that the method-dependent classification errors could influence the results of correlation between codon 72 polymorphism and the risk of cervical neoplasia. The correlations observed by this study did not demonstrate an association between codon 72 polymorphism and the risk of persistent HPV infection and precursor lesions of cervical cancer. Câncer cervical Cancerable lesions Cervical cancer Cervical neoplasms HPV HPV Lesões cancerizáveis Neoplasias do colo uterino p53 p53 Papilloma (Incidence) Papiloma (Incidência) Polimorfismo do códon 72 Polymorphism of codon 72 Variação entre metodologias Variation between methodologies Virologia Virology
67	DIFFUSE OPTICAL MEASUREMENTS OF HEAD AND NECK TUMOR HEMODYNAMICS FOR EARLY PREDICTION OF CHEMO-RADIATION THERAPY OUTCOMES Dong, Lixin 01 January 2015 (has links) Chemo-radiation therapy is a principal modality for the treatment of head and neck cancers, and its efficacy depends on the interaction of tumor oxygen with free radicals. In this study, we adopted a novel hybrid diffuse optical instrument combining a commercial frequency-domain tissue oximeter (Imagent) and a custom-made diffuse correlation spectroscopy (DCS) flowmeter, which allowed for simultaneous measurements of tumor blood flow and blood oxygenation. Using this hybrid instrument we continually measured tumor hemodynamic responses to chemo-radiation therapy over the treatment period of 7 weeks. We also explored monitoring dynamic tumor hemodynamic changes during radiation delivery. Blood flow data analysis was improved by simultaneously extracting multiple parameters from one single autocorrelation function curve measured by DCS. Patients were classified into two groups based on clinical outcomes: a complete response (CR) group and an incomplete response (IR) group with remote metastasis and/or local recurrence within one year. Interestingly, we found human papilloma virus (HPV-16) status largely affected tumor homodynamic responses to therapy. Significant differences in tumor blood flow index (BFI) and reduced scattering coefficient (μs’) between the IR and CR groups were observed in HPV-16 negative patients at Week 3. Significant differences in oxygenated hemoglobin concentration ([HbO2]) and blood oxygen saturation (StO2) between the two groups were found in HPV-16 positive patients at Week 1 and Week 3, respectively. Receiver operating characteristic curves were constructed and results indicated high sensitivities and specificities of these hemodynamic parameters for early (within the first three weeks of the treatment) prediction of one-year treatment outcomes. Measurement of tumor hemodynamics may serve as a predictive tool allowing treatment selection based on biologic tumor characteristics. Ultimately, reduction of side effects in patients not benefiting from radiation treatment may be feasible. near-infrared diffuse optics head and neck cancer papilloma virus status radiation therapy tumor hemodynamics prediction of treatment outcomes Bioimaging and Biomedical Optics Biomedical Devices and Instrumentation Biostatistics
68	Infecção genital pelo hpv em adolescentes: diagnóstico biomolecular / The HPV genital infection in adolescents: biomolecular diagnosis Barros, Luiza Daura Fragoso de 13 July 2006 (has links) The present study was to diagnose and classify the Human Papilloma Virus (HPV) in pregnant and non-pregnant adolescents, as study the risk factors related to the infection, identify the multiples oncogenics types presents in the study people and associate the differents types of HPV with cytology and colposcopy findings. Methodologic design: the type of study was prospective, descriptive and transversal coorte. Was study 111 sexually active adolescents, between 10 and 19 years old, patients of the Gynecology Service of the Professor Alberto Antunes University Hospital of the Federal University of Alagoas (HUPAA-UFAL). Was utilized the polymerase chain reaction / restriction fragment length polymorphism - sequencing (PCR/RFLPs) to identification of the virus. Results: the viral percentual in the inferior genital tract was 27% of the cases. The molecular genotyping revealed high risk viral genetic material - HPV 16, 33, 51, 58, 66, 1S39, CP8304 and LVX100, in 28,5% of the cases, low oncogenic risk - HPV 6, 11, 53, 61 e CP141, in 40% and, the other 31,4%, considered the indeterminate type, include high and low risk virus. This more incident type is found isolated or associated to other viral types and appears in 40% of the positive cases. The viral infection rate among the pregnant adolescents was 11,7%. The HPV genital infection was associated with a past of sexually transmitted diseases and the consumption of alcohol by the adolescent. The frequency of adolescents infected by HPV, associated to low grade intraepithelial lesion, was 5,0%. No associations were observed between the specific types of HPV and the cytology and colposcopy findings among the studied adolescents. / O objetivo do presente estudo foi para diagnosticar e classificar o papilomavírus humano (HPV) em adolescentes grávidas e não grávidas, bem como estudar os fatores de risco para a infecção, identificar os diversos tipos oncogênicos presentes na população estudada e associar os diferentes tipos de HPV com achados da citologia e colposcopia. Desenho metodológico: o tipo de estudo foi prospectivo, descritivo e de coorte transversal. Foram estudadas 111 adolescentes sexualmente ativas, entre 10 e 19 anos, atendidas no Serviço de Ginecologia do Hospital Universitário Prof. Alberto Antunes da Universidade Federal de Alagoas (HUPAA-UFAL). Utilizou-se a reação de polimerase em cadeia/polimorfismo de comprimento de fragmentos de restrição - sequenciamento (PCR/RFLPs), para a identificação do vírus. Resultados: o percentual do vírus no trato genital inferior foi de 27%. A genotipagem molecular revelou material genético viral de alto risco - HPV 16, 33, 51, 58, 66, 1S39, CP8304 e LVX100, em 28.5% dos casos, enquanto que os de baixo risco oncogênico - HPV 6b, 11, 53, 61 e CP141, em 40%. Os demais 31,4%, foram do tipo considerado indeterminado, que incluem vírus de alto e baixo risco. Esse tipo mais incidente encontra-se isolado ou associado a outros tipos virais e aparece em 40% do total dos casos positivos. A taxa de infecção viral entre as gestantes foi de 11,7%. A infecção genital pelo HPV teve associação com o passado de doenças sexualmente transmissíveis e com o consumo de álcool pela adolescente. A freqüência de adolescentes infectadas pelo HPV, associada à lesão intra-epitelial de baixo grau foi de 5,0%. Não foram observadas associações tipo-específicas do HPV com os achados da citologia e da colposcopia entre as adolescentes estudadas. Human Papilloma Virus Adolescents Genital infection PCR-RFLPs Colposcopy Papanicolau Cervical cancer Papillomavirus humano Adolescentes Infecção genital Fatores de risco PCR-RFLPs Colposcopia Esfregaço vaginal Neoplasias do colo uterino
69	Knowledge, attitude and practices on cervical cancer screening and prevention methods among nurses at two Nairobi hospitals in Kenya Kieti, Susan Ndila 06 1900 (has links) Background: Cervical cancer is the second most common cause of death from cancer among women in Kenya. Various international studies indicate that the knowledge level of cervical cancer and its predisposing and preventive measures is low among the nurses as well as general population. This study aimed to assess knowledge, practices and attitudes of nurses with regards to cervical cancer screening and preventive measures at two Nairobi hospitals in Kenya. Across-sectional quantitative descriptive study design was used. Convenience sampling method was applied and data were collected from respondents using self-administered questionnaire. About 114 nurses aged 18 years and above participated in the study. The study revealed that nurses have the information about cervical cancer, available screening tests and the purpose of screening. Nurses have the knowledge that cancer screening could detect this cancer at an early stage; however, uptake is low. Cervical screening services were hampered by barriers relating to health care institutions, nurses perception and fear of screening technique, embarrassment, stigma, social influence, financial costs and available sources of information / Health Studies / M.A. (Nursing Science) Awareness Attitude Cervix Cervical cancer Cervical screening and prevention Cervical screening barriers Human Papilloma Virus Uptake 616.994660967625
70	Knowledge of cervical cancer and awareness of screening regimes/routines among HIV positive women in Swaziland Chili, Thembisile 02 1900 (has links) Background Cervical cancer is one of the common cancers worldwide. Despite the available screening services, the uptake of cancer of the cervix is very low. The incidence and mortality in western countries has reduced greatly due to the introduction of cervical cancer screening programmes. However, this is not the same in Africa where cervical cancer is more prevalent in lower resource countries to lack of access to effective screening and services that enhances early detection and treatment. Purpose/Aim of the study The purpose of this research is to determine knowledge of cervical cancer and the level of awareness of screening regimes/routines among HIV positive women in Swaziland. The study was conducted at one hospital specifically at the HIV Care Unit and Public Health Unit between January and June 2015. Methods The questionnaire was administered to collect data and consisted both open and close-ended questions. The questionnaire comprises of three sections: Section A: Socio-demographic data and Section B: Awareness on Cervical Cancer. Section C: Awareness/knowledge on cervical cancer screening. The sample consisted of 123 HIV positive who are on antiretroviral therapy (ART) or ART naive. The mean age for the respondents was 35 years. Results From this study, N=28 (23%) out of 123 (77%) reported to have received annual Pap smear for cervical cancer screening. A low proportion of the respondents (45%) had knowledge on cervical cancer screening. In addition, 63% of those who got information about cervical cancer screening through the radio perceived themselves to be at risk of getting cervical cancer. Only 4% heard about cervical cancer at the ART clinic, despite having been followed up for their care at the HIV clinic. Those who screened for cervical cancer were younger in age 25-34 years (80%). This study also revealed that education increased the changes of a woman to be screened for cervical cancer. If a woman had a university or high school education, she perceived herself to be at risk of getting cervical cancer. Conclusion Knowledge is power, cervical cancer campaigns should be conducted at national level in order to promote prevention through screening. Cervical cancer screening should be fully integrated into HIV services / Health Studies / M.A. (Public Health) Awareness Cervix Cervical cancer Human papilloma virus Risk factor 362.196994096887

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