Global ETD Search

61	DARPP-32 expression in acquired resistance of breast cancer cells to trastuzumab Hamel, Sophie. January 2007 (has links) Amplification of the receptor tyrosine kinase ErbB-2 has been linked to the proliferation of breast cancer cells.1,2 Trastuzumab targets the extracellular domain of ErbB-2, leading to growth inhibition of approximately 15% of the breast cancers with genomic amplification of the ERBB2 gene.3 Clinical studies have demonstrated its efficacy in both early4 and metastatic breast cancers. 5,6 However, many tumors with ERBB2 amplification are not responsive to treatment.7 Moreover, the ones that initially respond, eventually progress and acquire drug resistance.8 An in vitro model for this acquired resistance was established by Chan & al.9 The breast cancer cell line, BT474, containing amplified ERBB2, was grown in the presence of trastuzumab for several months until subclones outgrew. Gene expression profiling was performed on these clones to determine differentially expressed genes between the parental and resistant cells. DARPP-32 (Dopamine and cAMP regulated phosphoprotein of 32kDa) was, by far, the most overexpressed transcript. DARPP-32 is coamplified with ERBB2 on the same amplicon of chromosome 17.10 This protein has been mostly described in neurobiology, but DARPP-32 overexpression was recently reported in gastrointestinal, esophageal, prostate and breast cancer.11 Therefore, we suggest that overexpression of DARPP-32 can cause acquired resistance of breast cancer cells to trastuzumab. The in vitro knockout of DARPP-32, using stable shRNA transfection, abolishes the resistance to trastuzumab in the clones, while overexpression of DARPP-32 in the parental cells results in de novo resistance. Overall, our results suggest that DARPP-32 may be a potential therapeutic target in breast cancer patients who develop acquired trastuzumab resistance. Breast Neoplasms -- drug therapy. Drug Resistance, Neoplasm. Receptor, erbB-2. Antibodies, Monoclonal. Antineoplastic Agents.
62	Evaluation of the effect of trastuzumab (Herceptin) on the development and progression of breast cancer associated skeletal metastasis Khalili Boroojeni, Parisa. January 2007 (has links) Breast cancer is the most commonly diagnosed cancer in women. Despite recent advances in screening and early detection, breast cancer continues to result in a high incidence of morbidity and mortality. In its late stage the majority of patients exhibit signs of destructive skeletal metastasis. This complication is promoted by the production of growth factors by tumor cells which can induce tumor cell proliferation via their interaction with their respective receptors to initiate the vicious cycle of bone resorption. Inhibition of growth factors signaling through their receptors can therefore serve as a useful therapeutic approach to block bone metastasis. / The biological characteristics of cancer cells along with the targeting properties of immune system offer a novel approach in the treatment of breast cancer. Directed against HER-2/nue oncogene, the recombinant humanized monoclonal antibody, Trastuzumab (Herceptin), has shown significant clinical benefits for the treatment of HER-2 positive metastatic breast cancer. / In the present study, the effects of Herceptin and its molecular mechanism of action in abrogating the development and progression of osteolytic bone metastasis is investigated in an experimental mouse model of skeletal metastasis using human breast cancer cells BT-474 which are known to express high levels of HER-2. Treatment of BT-474 cells with Herceptin caused a dose dependent decrease in cell proliferation. In in vivo studies BT-474 cells were injected by into the left ventricle of female BALB/c nu/nu mice. Intraperitoneal infusion of Herceptin from the day of tumor cell inoculation or at the time of radiologically detectable skeletal metastasis either slowed the development or prevented the progression of skeletal metastasis as compared to control groups of animals receiving non-specific IgG. Bone histological analysis of long bones showed the ability of Herceptin to reduce the ratio of tumor volume to bone volume as well as mitotic index when Herceptin treatment was initiated from the day of tumor cell inoculation. Immunohistochemical analysis of long bones showed a significantly lower level of activated (phosphorylated) MAPK in bones of Herceptin treated animals. These studies demonstrate the ability of Herceptin to inhibit the development and abrogate the progression of skeletal metastasis associated with breast cancer by blocking the HER-2 mediated signaling pathways. Bone Neoplasms -- secondary. Bone Neoplasms -- drug therapy. Breast Neoplasms -- pathology.
63	Functional properties of antibodies in resistance against HIV-1 infection / Devito, Claudia, January 2002 (has links) Diss. (sammanfattning) Stockholm : Karolinska institutet, 2002. / Härtill 6 uppsatser.
64	Characterization and function of the inflammatory response to infection by a gastrointestinal nematode parasite : new insights into protective Th2 responses / Anthony, Robert McCullough January 2006 (has links) (PDF) Thesis (Ph.D.)--Uniformed Services University of the Health Sciences, 2006 / Typescript (photocopy)
65	Desenvolvimento de kit diagnóstico rápido para detecção de resistência à meticilina em cepas de estafilococos Chagas, Marne Coimbra Batalha January 2011 (has links) Submitted by Priscila Nascimento (pnascimento@icict.fiocruz.br) on 2012-12-13T12:38:59Z No. of bitstreams: 1 marne-chagas.pdf: 1100888 bytes, checksum: 7a199f01e03cd65e615b7c57af7901f0 (MD5) / Made available in DSpace on 2012-12-13T12:38:59Z (GMT). No. of bitstreams: 1 marne-chagas.pdf: 1100888 bytes, checksum: 7a199f01e03cd65e615b7c57af7901f0 (MD5) Previous issue date: 2011 / Fundação Oswaldo Cruz. Instituto de Tecnologia em Imunobiológicos. Rio de Janeiro, RJ, Brasil. / O surgimento de resistência a antimicrobianos em bactérias está se agravando ano após ano, constituindo-se um problema de saúde pública em hospitais e centros de tratamento ao redor do mundo. No Brasil, a resistência a meticilina em Staphylococcus aureus(MRSA) chega a 29 % dos casos detectados anualmente. Atualmente, a metodologia convencional para a identificação de MRSA pode levar 48 horas, portanto, este trabalho tem por objetivo o desenvolvimento de um teste para diagnóstico rápido baseado na tecnologia de imunocromatografia de fluxo lateral usando um anticorpo específico contra a proteína PBP2a, a qual confere resistência ao Staphylococcus aureus, permitindo a identificação em minutos, a partir de colônias isoladas. O anticorpo monoclonalanti-PBP2a foi purificado e empregado em um processo de conjugação a microesferas de látex coloridas para a implementação do teste rápido. Os resultados iniciais demonstraram a capacidade do anticorpo de reconhecer a PBP2a em amostras de MRSA, porém foram observados problemas de inespecificidade que deverão ser solucionados para dar confiabilidade ao teste proposto. / The emergence of antibiotic resistance in bacteria is getting worse year after year, becoming a public health problem in hospitals and treatment centers around the world. In Brazil, methicillin resistance in Staphylococcus aureus(MRSA) reaches 29% of cases detected annually. Currently, the conventional methodology for identification of MRSA may take 48 hours of lengthyphenotypical tests, so this work aims at developing a rapid diagnostic test based onthe lateral flow immunochromatography protocol using a specific antibody against the protein PBP2a, which confers the methicillin-resistance phenotype to Staphylococcus aureus, allowing a prompt identification from isolated colonies. The monoclonal antibody anti-PBP2a was purified and used in a process of conjugation to colored latex microspheres for the implementation of the rapid test. Initial results demonstrated the ability of the antibody to recognize the PBP2a in samples of MRSA, but inespecificity issues will have to be solved to improve reliability of the test proposed. Staphylococcus aureus Proteína PBP2a Anticorpos Monoclonais Diagnóstico Staphylococcus aureus Protein PBP2a Antibodies, Monoclonal Diagnosis Staphylococcus aureus Anticorpos Monoclonais Diagnóstico
66	DARPP-32 expression in acquired resistance of breast cancer cells to trastuzumab Hamel, Sophie. January 2007 (has links) No description available. Antineoplastic Agents. Receptor, erbB-2. Antibodies, Monoclonal. Drug Resistance, Neoplasm. Breast Neoplasms -- drug therapy.
67	Evaluation of the effect of trastuzumab (Herceptin) on the development and progression of breast cancer associated skeletal metastasis Khalili Boroojeni, Parisa. January 2007 (has links) No description available. Breast Neoplasms -- pathology. Bone Neoplasms -- drug therapy. Bone Neoplasms -- secondary.
68	Anti-IL17 associado ou não do inibidor da Rho-quinase em camundongos com inflamação pulmonar alérgica crônica / Anti-IL17 with or without the use of the Rho kinase inhibitor in mice with chronic allergic pulmonary inflammation Santos, Tabata Maruyama dos 03 September 2018 (has links) INTRODUÇÃO: Indivíduos com asma possuem infiltração aumentada de células inflamatórias, produção de quimiocinas e hiperresponsividade de vias aéreas. Estes apresentam níveis aumentados de interleucina (IL)-17, importante na regulação da expressão de mediadores inflamatórios e recrutamento de células inflamatórias, outra característica é aumento da atividade da proteína Rho-quinase em suas vias aéreas. A modulação da IL-17 e da proteína Rho-quinase pode ser promissora para o tratamento desta doença. OBJETIVO: Estudar os efeitos dos tratamentos realizados com anticorpo neutralizador anti-IL17 e do inibidor da Rho-quinase, associados ou não, em camundongos com inflamação pulmonar alérgica crônica. MÉTODOS: Foram utilizados 64 camundongos BALB/c, divididos em 8 grupos (8 animais por grupo): SAL (solução salina); OVA (ovoalbumina), SAL-RHOi (salina e inibidor de Rho-quinase), OVA - RHOi (ovoalbumina e inibidor de Rho-quinase), SAL - anti-IL17 (salina e anti-IL17), OVA - anti-IL17 (ovoalbumina e anti-IL17), SAL - RHOi - anti-IL17 (salina, anti-IL17 e inibidor de Rho-quinase), OVA - RHOi - anti-IL17 (ovoalbumina, anti-IL17 e inibidor de Rho-quinase). O protocolo de sensibilização e indução da inflamação pulmonar por ovoalbumina teve duração de 28 dias. O Anti-IL17A (clone 50104 - 7,5 ug por dose) foi administrado via intraperitoneal e inibidor de Rho-quinase (Y-27632) intranasal (10 mg/kg), 1h antes de cada desafio com ovoalbumina (22, 24, 26 e 28 dias). RESULTADOS: Houve um aumento na resistência do sistema respiratório e na elastância, nos marcadores inflamatórios CD4+, CD8+, ROCK1 e ROCK2, IL-1-beta, IL-2, IL-4, IL-5, IL-6, IL-10, IL-13, IL-17, TNFalfa, em vias sinalizadoras NF-kappaB, FOXP-3 e células dendríticas, em marcadores de remodelamento MMP9, MMP12, TIMP1, iNOS, TGF-beta, no conteúdo de isoprostano, decorina, biglicano, fibronectina e fibras colágenas e na expressão gênica de VAChT, IL-17 e arginase, no grupo OVA em comparação com o grupo controle. O tratamento dos animais sensibilizados, de forma individualizada ou a associação dos dois, atenuou estas respostas quando comparados ao grupo sensibilizado com ovoalbumina e não tratado (p < 0,05). O tratamento do inibidor de Rho-quinase associado ao anti-IL17 gerou potencialização do controle da resposta de hiperresponsividade à metacolina, assim como nas vias aéreas a redução do número de células positivas TNF-alfa, IL-4, IL-5 e nos septos alveolares o número de células positivas IL-4, IL-5, TGF-beta, FOXP3, ROCK1 e ROCK2 (p < 0,05). CONCLUSÃO: O tratamento com anti-IL17 associado ao inibidor da Rho-quinase modula a hiperresponsividade das vias aéreas, inflamação, e remodelamento e estresse oxidativo em animais com inflamação pulmonar alérgica crónica / RATIONALE: Individuals with asthma have increased infiltration of inflammatory cells, chemokines production, and airway hyperresponsiveness. Asthmatics have elevated levels of interleukin (IL)-17, which plays an important role in regulating the expression of inflammatory mediators and recruitment of inflammatory cells, these individuals also have increased Rho-kinase protein activity in their airways. The modulation of IL-17 and Rho-kinase protein may be promising for the treatment of this disease. OBJECTIVE: To study the effects of anti-IL17 neutralizing antibody and Rho-kinase inhibitor treatments, associated or not, on mice with chronic allergic lung inflammation. METHODS: Were used 64 BALB/c mice, divided into eight groups (n=8 in each group): SAL (saline-instilled); OVA (exposed-ovalbumin); SAL-RHOi (saline and Rho-kinase inhibitor), OVA-RHOi (exposed-ovalbumin and Rho-kinase inhibitor); SAL - anti-IL17 (saline and anti-IL17), OVA - anti-IL17 (exposed-ovalbumin and anti-IL17); SAL - RHOi -anti-IL17(saline, Rho-kinase inhibitor and anti-IL17), OVA - RHOi - anti-IL17 (exposed-ovalbumin, anti-IL17 and Rho kinase inhibitor). The protocol for sensitization and induction of pulmonary inflammation by ovalbumin has the duration of 28 days. The Anti-IL17A neutralizing antibody (clone 50104-7.5 ug per dose) was administered via the intraperitoneal, and Rho-kinase inhibitor (Y-27632) intranasal (10 mg/kg), 1h before each ovalbumin challenge (22, 24, 26 and 28 day). RESULTS: There was an increase in respiratory system resistence and elastance, in the positive cells evaluated CD4+, CD8+, ROCK1 and ROCK2, IL-1beta, IL-2, IL-4, IL-5, IL-6, IL-10, IL-13, IL-17, TNFalpha, TGF-beta, MMP9, MMP12, TIMP1 and isoprostane, decorin, biglican, fibronectin, collagen fibers content, signaling pathways NF-kappaB, FOX-P3, dendrict cells and gene expression of VAChT, IL-17 and arginase in the OVA group compared to the control group. Treatment of the sensitized animals with the Rho-kinase inhibitor or with the anti-IL17 or with the combination of the two, attenuated these responses when compared to the ovalbumin-sensitized and untreated group (p < 0,05). The treatment of the anti-IL17 associated Rho-kinase inhibitor generated potentiation of the hyper responsiveness response to methacholine, as well as in the airways the reduction of the number of TNF-alpha, IL-4, IL-5 positive cells and in the alveolar septa the number of IL-4, IL-5, FOXP3, TGF-beta, ROCK1 and ROCK2 (p < 0.05). CONCLUSION: Anti-IL17 treatment associated with the Rho-kinase inhibitor modulates airway hyperresponsiveness, inflammation, remodeling and oxidative stress in animals with chronic allergic pulmonary inflammation Airway remodeling Antibodies monoclonal Anticorpos monoclonais Asma Asthma Inflamação Inflammation Interleucina-17 Interleukin-17 Quinases associada a rho Remodelação das vias aéreas Rho-associated kinases
69	Comparison of isoelectric focusing and immunofixation electrophoresis to distinguish oligoclonal from monoclonal immunoglobulin bands. January 1998 (has links) submitted by Liu Dan. / Thesis (M.Sc.)--Chinese University of Hong Kong, 1998. / Includes bibliographical references (leaves 66-80). / Abstract also in Chinese. / CONTENTS --- p.i / LIST OF TABLES --- p.iii / LIST OF FIGURES --- p.iv / LIST OF ABBREVIATIONS --- p.v / ACKNOWLEDGEMENTS --- p.vi / ABSTRACT --- p.vii / Chapter Chapter 1 --- INTRODUCTION --- p.1 / Chapter 1.1 --- History --- p.1 / Chapter 1.2 --- Immunoglobulins --- p.3 / Chapter 1.2.1 --- Structure --- p.3 / Chapter 1.2.2 --- Properties of immunoglobulins --- p.7 / Chapter 1.3 --- Monoclonal proteins and monoclonal gammopathies --- p.12 / Chapter 1.3.1 --- Monoclonal proteins --- p.12 / Chapter 1.3.2 --- Monoclonal gammopathies --- p.14 / Chapter 1.4 --- Laboratory investigation of monoclonal immunoglobulin --- p.17 / Chapter 1.4.1 --- The current procedure of investigation in laboratory --- p.17 / Chapter 1.4.2 --- Problems in identifying monoclonal immunolgobuin --- p.19 / Chapter 1.5 --- Comparison of different techniques --- p.20 / Chapter 1.5.1 --- Immunoelectrophoresis --- p.20 / Chapter 1.5.2 --- Immunofixation electrophoresis --- p.22 / Chapter 1.5.3 --- Isoelectric focusing and immunoisoelectric focusing --- p.24 / Chapter 1.6 --- Aim of the present study --- p.27 / Chapter 1.7 --- Design of experiment --- p.27 / Chapter Chapter 2 --- MATERIALS AND METHODS --- p.30 / Chapter 2.1 --- Study subjects --- p.30 / Chapter 2.2 --- Apparatus --- p.30 / Chapter 2.2 --- Apparatus --- p.30 / Chapter 2.3 --- Reagents and materials --- p.32 / Chapter 2.4 --- Preparation of gels --- p.35 / Chapter 2.5 --- Isoelectric focusing procedure --- p.36 / Chapter 2.6 --- Acid fixation and staining --- p.37 / Chapter 2.7 --- Technical factors affecting results --- p.38 / Chapter Chapter 3 --- RESULTS --- p.40 / Chapter 3.1 --- Interpretation of results in isoelectric focusing --- p.40 / Chapter 3.2 --- Affecting factors --- p.47 / Chapter 3.3 --- Comparison of the results between IEF and IFE --- p.53 / Chapter Chapter 4 --- DISCUSSION --- p.59 / Chapter Chapter 5 --- CONCLUSION --- p.65 / References --- p.66 Immunoelectrophoresis Isoelectric Focusing Liver Cirrhosis--epidemiology Liver Cirrhosis--epidemiology--Hong Kong
70	Resultado do tratamento da doença de Crohn com anti-fator de necrose tumoral alfa / Outcomes in the treatment of Crohn´s disease with anti tumor necrososis factor-alpha Malheiros, Anna Paula Rocha 19 August 2008 (has links) A doença de Crohn é uma inflamação crônica do trato gastrointestinal. O tratamento convencional é muitas vezes desapontador. Apesar da variedade de drogas disponíveis para o tratamento da doença inflamatória intestinal, tais como: salicilatos e seus derivados, corticosteróides, antibióticos e imunossupressores, nenhuma destas mostrou ser totalmente eficaz ou definitiva para o tratamento da doença e seus surtos de exacerbação. Pesquisas têm sido desenvolvidas com o objetivo de apresentar drogas mais efetivas. Dentre estas, destacam-se as drogas biológicas. O infliximabe é um anticorpo monoclonal quimérico anti-fator de necrose tumoral alfa e está indicado na doença de Crohn refratária e fistulizante. O objetivo deste estudo visa avaliar prospectivamente os resultados e efeitos colaterais precoces e tardios do uso do anti-TNF alfa no tratamento de 60 doentes com doença de Crohn, no período de julho de 1999 a dezembro de 2005. Os doentes foram tratados com anti-TNF alfa (infliximabe), na dose de 5mg/kg de peso, aplicado por via endovenosa em intervalos de dois meses. A avaliação foi realizada por protocolo clínico que classificava os quesitos: estado geral, sintomas intestinais e doença perianal em melhor, inalterado e pior, e pelo índice de atividade da doença de Cronh. Os doentes tratados com anti-TNF alfa apresentaram mediana de duração da doença de sete anos, variando de um a 28 anos entre a data do início dos sintomas e a data de início da pesquisa. 34 doentes (56,7%) já haviam sido submetidos a uma ou mais operações abdominais e 38 (63,3%) a operações orificiais. O software utilizado para a realização dos cálculos foi o SPSS® 9.0 for Windows, sendo estatisticamente significantes os testes com p<0,05. Foram aplicadas 225 doses de anti-TNF alfa, em média, 3,7 doses por paciente num período de aproximadamente cinco anos, variando de uma a 14 doses. No tratamento inicial 76% dos pacientes responderam a droga. As principais indicações para o emprego do anti-TNF alfa foram a presença de doença perianal em 36 casos (60%) e a intratabilidade clínica em 24 casos (40%). Observou-se que após a primeira dose da medicação, os doentes com mais de dez anos de doença e submetidos à operação abdominal tiveram resultado satisfatório semelhantemente aqueles doentes com menos de cinco anos de doença e não operados com p<0,05. O índice de atividade da doença de Crohn foi em média de 189,7 antes do início do tratamento e na primeira aplicação diminuiu em média para 135,4, e progressivamente ao longo das aplicações (115, 102, 109 e 88,4 até a quinta dose), sendo o resultado estatisticamente significativo. Houve efeito colateral em 40 aplicações (17,8%), sendo os efeitos principais: eritema cutâneo, dispnéia e dor abdominal. O tratamento com anti-fator de necrose tumoral alfa, obedecidas as indicações precisas, associou-se a baixo índice de efeitos colaterais graves tendo apresentado bons resultados na resolução da doença de Crohn perianal, na melhora da sintomatologia intestinal e no estado geral dos pacientes / Crohn´s disease is a chronic inflammatory disorder of the gastrointestinal tract. Conventional treatment is many times disappointing. Besides the great number of available medications to treat inflammatory bowel diseases, such as salicilates and derivatives, corticosteroids, antibiotics and immunosuppressive agents, none of them proved to be totally efficient or the ultimate treatment for inflammatory diseases and their exacerbation. Researches have been carried out to find more effective therapeutic drugs. Among these therapeutics, biologic treatments have been in evidence. Infliximab is a chimeric IgG1 monoclonal antibody against tumor necrosis factor-alpha, and is indicated for refractory luminal and fistulizing Crohns disease. The aim of this study is to prospectively evaluate the outcome, early and late adverse events, in 60 patients diagnosed with Crohn´s disease and treated with infliximab between July 1999 and December 2005. All patients were treated with anti-TNF-alpha (infliximab), 5mg/kg/dose, intravenously, each two months. Patients were clinically evaluated using a protocol that classified the evolution of the health status, intestinal symptoms and perianal disease, as better, worse or unchanged, during the treatment. Crohn´s disease activity index was also evaluated. Patients treated with anti-TNF-alpha presented a median disease duration of seven (range 1-28) years, between the beginning of the disease symptoms and the beginning of the research protocol. Thirty-four patients (56.7%) have been submitted to one or more abdominal surgeries before, and 38 (63.3%) to anal-rectum surgeries. All statistics tests were performed with computer software Statistical Package for the Social Sciences (SPSS® 9.0) for WindowsTM, and p values of less than 0.05 were considered statistically significant. Totals of 225 anti-TNF-alpha doses were administered. The mean doses administered per patient, in a period of approximately five years, were 3.7 (range 1-14) doses. After the initial treatment, 76% of the patients achieved a response. The most frequent indications for anti-TNF-alpha was perianal disease, occurring in 36 patients (60%), and clinical failure to the conventional treatment, happening in 24 patients (40%). After the first dose of anti-TNF-alpha, patients with more than 10 years of treatment and previously submitted to abdominal surgery presented a satisfactory outcome, similar to those with less than 5 years of disease and not submitted to surgery, p<0.05. Crohn´s disease activity index showed a mean index of 189.7 before treatment, that decreased to 135.4 after the first dose, and progressively decreased with the subsequent doses (means: 115, 102, 109 and 88.4, until the fifth dose, p<0.05). Adverse events were reported in 40 administrations (17,8%) from the total. The most prevalent adverse events were: rash, dyspnoea and abdominal pain. The treatment with anti-TNF-alpha, following precise indications, was associated with a low incidence of severe adverse events and presented good outcomes in the resolution of perianal Crohn´s disease, improving intestinal symptomatology and patients´ health status Antibodies monoclonal/therapeutic use Anticorpos monoclonais/uso terapêutico Crohn's disease/therapy Doença de Crohn/terapia Fator de necrose tumoral alfa Tumor necrosis factor-alpha

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