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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
331

Desenvolvimento de uma estratégia vacinal dose-reforço heterológo baseada em linhagens recombinantes de Bacillus subitilis para o controle de Spreptococcus mutans. / Development of a heterologous reinforcement dose vaccine strategy based on recombinant strains of Bacillus subtilis for the control of Streptococcus mutans.

Silva, Dalva Adelina da 16 March 2018 (has links)
A cárie dental é uma doença bacteriana infecciosa considerada como um dos principais problemas de saúde pública. O principal agente etiológico para o desenvolvimento da doença é o Streptococcus mutans. A proteína P1, também conhecida como antígeno I/II, do S. mutans é fundamental para a etapa inicial de adesão à superfície dental (sacarose-independente), sendo, portanto, considerada essencial para o processo de colonização deste patógeno. Algumas regiões dessa proteína vêm sendo empregadas como antígenos em estratégias vacinais contra a cárie, entre elas a região A, localizada na porção N-terminal, conhecida como região de ligação à saliva Saliva Binding Region (SBR). No entanto, apesar dos avanços, não existe vacina para a prevenção da cárie licenciada para uso em humanos. Diante disso, o presente trabalho tem como objetivo o desenvolvimento e caracterização de uma nova estratégia vacinal contra o S. mutans baseada em esquema de dose-reforço heterólogo, utilizando o fragmento P139-512, na forma de proteína purificada, expressa a partir de linhagens recombinantes de Bacillus subtilis. A proteína P139-512 compreende os aminoácidos 39-512 da proteína nativa, o que corresponde a toda região A e uma pequena porção da região variável da proteína P1. Utilizamos esporos de B. subtilis 1012, modificados para expressar o antígeno P139-512 (LDV702). A linhagem LDV704, além de expressar o antígeno, foi modificada para expressar uma invasina (InvA) com capacidade de se ligar a epitélios de mucosa. Camundongos da linhagem BALB/c foram imunizados por via sublingual com uma dose de esporos de B. subtilis (linhagens 1012, LDV702, LDV704 ou PBS) seguidos por dois reforços com a proteína P139-512, associada ou não com o adjuvante LTK63. Níveis significativos de anticorpos séricos foram induzidos pelas formulações em associação com o adjuvante após a terceira dose, e mostraram-se capazes de reconhecer os epítopos em diferentes linhagens de S. mutans. No entanto, nenhuma das formulações mostrou-se capaz de ativar respostas de mucosa (S-IgA). Porém, observamos que o adjuvante LTK63 empregado na estratégia dose-reforço heterólogo potencializou a resposta sérica de anticorpos IgG, sendo capaz de modular e melhorar qualitativamente as respostas induzidas. Assim, a administração das formulações na presença do adjuvante representa uma alternativa promissora para o controle do S. mutans. / Dental caries is an infectious bacterial disease considered as one of the main public health problems. The main etiological agent for the development of the disease is the Streptococcus mutans. The P1 protein, also known as S. mutans Ag I / II antigen, is essential for the initial stages of adhesion to the dental surface (sucrose-independent) and is, therefore, considered essential for the colonization process of this pathogen. Some regions of this protein have been used as antigens in vaccine strategies against caries, among them the A region, located at the amino terminal region also known as the Saliva Binding Region (SBR). However, despite the advances, there is no licensed anti-caries vaccine for human use. Therefore, the present work aims to develop and characterize a new vaccine strategy against S. mutans based on a heterologous priming/boost immunization regimen using the recombinant P139-512 fragment, expressed and purified from a Bacillus subtilis strain. The P139-512 protein comprises amino acids that encompasses the entire A region and a small portion of the variable region of the P1 protein. We used spores of B. subtilis 1012 (wild-strain) and recombinants that were modified to express the antigen P139-512 (LDV702). In addition to express the antigen, the LDV704 strain was modified to express a surface-exposed bacterial invasin (InvA) capable of binding to the mucosal epithelia. BALB/c mice were primed via the sublingual route with a dose of B. subtilis spores (1012, LDV702, or LDV704 strains) followed by two boosting doses with the purified protein P139-512, associated or not with the LTK63 adjuvant, by the same administration route. Significant serum antibody levels were induced by the formulations with the adjuvants after the third dose and the antibodies were shown to recognize epitopes exposed on the surface of different S. mutans strains. However, none of the formulations were capable to activate mucosal responses (S-IgA). Nevertheless, we observed that the LTK63 enhanced the serum IgG responses and qualitatively improved the induced antibody response. Thus, the administration of the formulations in the presence of the adjuvant represents a promising alternative for the control of S. mutans.
332

Proposta de gestão on-line das informações de vigilância epidemiológica de eventos adversos pós-vacinação / Proposal for managing online information for epidemiological surveillance of adverse events following immunization

Silva Junior, Arnaud Marcolino da January 2010 (has links)
Made available in DSpace on 2011-05-04T12:36:26Z (GMT). No. of bitstreams: 0 Previous issue date: 2010 / Hoje em dia, uma série de vacinas são capazes de proteger as pessoas, reduzindo drasticamente a incidência de doenças. Para gerenciar as ações de imunização em saúde pública, o Programa Nacional de Imunizações foi criado em 1973. Através dos seus mecanismos de trabalho, tais como, fornecimento de vacinas para toda a população, financiada pelo Governo Federal, sem custos diretos para os vacinados; armazenamento, transporte e suprimento de vacinas em redes de frio adequadas; sistemas de informações confiáveis, o Programa Nacional de Imunizações tem êxito em seus objetivos por controlar várias doenças evitáveis pela imunização. No entanto, sabemos que a ocorrência de eventos adversos pode surgir após a administração desses produtos imunizantes EAPV. Para monitorar e controlar EAPV, a Vigilância Epidemiológica de Eventos Adversos Pós-Vacinação foi criado pelo Programa Nacional de Imunização, em 1992. Este serviço foi estruturado para reconhecer e identificar os casos de EAPV, subsidiar pesquisas, e assessorar os profissionais de saúde na vigilância de casos, entre outros objetivos que contribuem para o controle de vacinas, saúde e bem-estar da população. Para fazer o controle de eventos adversos, a Vigilância Epidemiológica de EAPV usa um formulário de notificação, manual de monitoramento com informações e instruções para notificar e investigar casos de EAPV e fornecer dados para o sistema de informação. Este último é fundamental para acompanhar os casos suspeitos e confirmados de EAPV, identificando os casos graves, os surtos e controlar os lotes de vacinas que podem causar eventos adversos à população vacinada. Desde 1998, o Programa Nacional de Imunizações tem administrado o Sistema de Informações de Eventos Adversos Pós-Vacinação, desenvolvido pela equipe técnica do Departamento de Informática do Ministério da Saúde DATASUS. Com base nas diretrizes e critérios para avaliação de sistemas de vigilância do Centers for Disease Control and Prevention (CDC) - Atlanta / EUA, várias falhas e erros foram apontadas no sistema, onde surgiu a proposta de um novo sistema de informação para melhorar a eficácia da Vigilância Epidemiológica de Eventos Adversos Pós-Vacinação. O sistema foi revisto de acordo com a padronização da Terminologia de Reações Adversas (WHO-ART) e o Dicionário Médico de Atividades Reguladoras (MedDRA) da Rede Uppsala Monitoring Centre(UMC). O novo sistema de informações proposto nesta dissertação pode beneficiar de Vigilância Epidemiológica de Eventos Adversos Pós-Vacinação facilitando o fluxo de dados de EAPV, ampliando o acesso às informações aos diversos profissionais de saúdee fabricantes de vacinas, atualizando e facilitando a operação, enquanto mantém a segurança e privacidade da informação. Esta proposta inclui um novo formulário de notificação com base no atual formato em uso nas unidades de saúde no país, além das fichas de notificação dos sistemas de vigilância do Canadá e EUA. O Centro de Vigilância Epidemiológica da Secretária de Estado da Saúde de São Paulo, também contribuiu com o seu modelo de formulário. / Nowadays, a number of vaccines are able to protect people, reducing dramatically the incidence of diseases. To manage the immunizing actions in public health, the Brazilian National Immunization Program was created in 1973. Through its working mechanisms, such as, providing vaccines for the whole population, funded the Federal Government, without direct cost for vaccinees; storage, transportation and supply of vaccines in appropriate cold chain settings; reliable information systems, the National Immunization Program has succeed in its goal to control many diseases preventable by immunization. However, we know that the occurrence of adverse events may follow the administration of immunizing products – AEFI. To monitor and control AEFI, the Epidemiological Surveillance of Adverse Events Following Immunization was created by National Immunization Program in 1992. This service was structured to recognize and identify AEFI cases, subsidize research work, and support health professionals in surveillance, and other objectives that contribute to vaccines control, health and welfare of the population. To control adverse events, AEFI’s Epidemiological Surveillance use a notification form, monitoring manual with information and instructions to report and investigate AEFI’s cases and supply data to the information system. The latter is critical to follow up suspected and confirmed cases of AEFI, identifying severe cases, outbreaks and monitor vaccine lots that may cause adverse events to the vaccinated population. Since 1998, the National Immunization Program has managed the Adverse Events Following Immunization’s Informations System, developed by the technical staff in the Ministry of Health Department - DATASUS. Based on the guidelines and criteria for evaluation of the Surveillance Systems for the Centers for Disease Control and Prevention (CDC) – Atlanta / USA, several flaws and errors in systems were pointed out, and a proposal for a new information system was conceived to improve the effectiveness of the Epidemiological Surveillance of Adverse Events Following Immunization. The system was revised according to the standardization of Adverse Reactions Terminology (WHO-ART) and Medical Dictionary of Regulatory Activities (MedDRA) of the Network Uppsala Monitoring Center (UMC). The new informations system proposed in this dissertation may benefit the Epidemiological Surveillance of Adverse Events Following Immunization by expediting the flow of AEFI’s data, expanding the access to information to various health professionals, and to vaccine manufacturers, updating and facilitating operation, while mantaining security and privacy. This proposal include a new notification form based on the current format in use in the health units in the country besides the notification forms of Surveillance Systems in Canada and USA. The Epidemiological Surveillance Center of State Secretary for Health in São Paulo, also contributed to its model of form.
333

Survey of Procedures Employed and Progress made by Dallas City Schools for the Immunization of Contagious Diseases

Manire, Vera Olivia 08 1900 (has links)
The purpose of this study was to determine the progress of the immunization program for Contagious Diseases in the City Schools of Dallas, Texas, over a period of ten years, dating from September 1928, to September 1938. An endeavor was made to determine how the Health Works Program of the Dallas Public Schools developed, and the protection it gave the public children.
334

Barriers to routine immunisation at Zwelihle Clinic, Overberg district, Western Cape

Hugo, Clair Patricia Bruns 08 May 2015 (has links)
Background: Although immunisation services are provided free at all public health facilities in South Africa, immunisation coverage remains variable and disease outbreaks still occur. The coverage rate in the Overberg district is recorded as 75.8%, below the national target of 90% (Western Cape Government Provincial Treasury 2013:2). The researcher wanted to understand what the barriers to accessing immunisation services were and how this might relate to other primary health care services. Methods: The researcher visited 22 households and interviewed nine mothers who had brought their children to Zwelihle Clinic to be immunised and nine community health workers servicing the Zwelihle community in the Overberg district, Western Cape Province. Findings: A key finding is that the data does not reflect the actual situation – children in the community either are immunised at other facilities or have left the catchment area, hence strong relationships between the facility and the community and an electronic patient tracking system become important. Findings impacting access to services include the attitude of administrative staff, waiting times and the impact of migratory communities. Recommendations are made to improve the quality of data, provide training to administrative staff, improve patient education, reduce waiting times and improve the relationship between the clinic and the community in order to better track patient migration / Health Studies / M.A. (Public Health)
335

Nanoparticles as a carrier for protein and plasmid DNA vaccines in microneedle-mediated transcutaneous immunization

Kumar, Amit, active 21st century 25 September 2014 (has links)
Skin is the largest immune organ and an ideal site to administer vaccines. However, by nature, skin is not permeable to antigens, which are macromolecules. The major hurdle in skin permeation is the outermost stratum corneum layer. Microneedles have proven feasible to create micron-sized channels in the epidermis of the skin, through which protein and plasmid DNA antigens can penetrate into the viable skin epidermis and dermis. However, the immune responses induced by microneedle-mediated transcutaneous immunization with protein or plasmid DNA alone are generally weak, and a vaccine adjuvant is often required to induce strong immune responses. Data from numerous previous studies have shown that nanoparticles as a vaccine carrier can significantly enhance the immunogenicity of antigens, but the feasibility of utilizing nanoparticles as a vaccine carrier to enhance the immune responses induced by microneedle-mediated transcutaneous immunization has rarely been studied. In this dissertation, using protein antigen (OVA) chemically conjugated onto the surface of solid-lipid nanoparticles and plasmid DNA (pCMV-beta, pVax/opt-BoNT/C-Hc50, and pCI-neo-sOVA) physically coated on the surface of cationic polymeric nanoparticles, we showed that the immune responses induced by microneedle-mediated transcutaneous immunization with protein antigens or plasmid DNA vaccines are significantly enhanced by delivering the proteins and plasmid DNA with nanoparticles. Importantly, microneedle-mediated transcutaneous immunization with proteins or plasmid DNA induces not only systemic immune responses, but also mucosal immune responses. In addition, it is generally believed that microneedles are safe. However, it remained unclear whether the micropores created by microneedles on the skin will also facilitate the permeation of microbes such as bacteria into the skin. In this dissertation, we also designed an unique ex vivo model to evaluate the permeation of live bacteria through mouse skin pretreated with microneedles. The results demonstrated that the risk of potential bacterial infection associated with microneedle treatment is not greater than that associated with a hypodermic needle injection. / text
336

Aspects of cash-flow valuation

Armerin, Fredrik January 2004 (has links)
This thesis consists of five papers. In the first two papers we consider a general approach to cash flow valuation, focusing on dynamic properties of the value of a stream of cash flows. The third paper discusses immunization theory, where old results are shown to hold in general deterministic models, but often fail to be true in stochastic models. In the fourth paper we comment on the connection between arbitrage opportunities and an immunized position. Finally, in the last paper we study coherent and convex measure of risk applied to portfolio optimization and insurance.
337

Determinants of Hepatitis B Vaccination among Adults in the United States: NHANES 1999-2006

Wright, Conschetta 07 May 2009 (has links)
Purpose: The primary objective of this study was to estimate the prevalence of vaccination and HBV infection status of adults and to evaluate the trend in self reported vaccination and seroprevalence for Hepatitis B for this population. Additionally, this study sought to assess the association between vaccination rates, seroprevalence (HBsAg, anti-HBc, and anti-HBs), demographic (age, gender, location of birth, race/ethnicity), and socioeconomic (annual household income, education level, insurance coverage and access to care, marital status) characteristics. Methods: Eight years, 1999-2006, of the National Health and Nutrition Examination Survey (NHANES) data were used. NHANES participants aged 20-59 years who contributed data via the household interview and laboratory component were eligible for this study. Two sources of vaccination status were available. The vaccination status was identified through self-report. Those who answered yes to “less than three doses” and “at least three doses” were classified as vaccinated. Vaccination status was also verified through serologic markers. All analyses were weighted to consider the complex weighting scheme and adjusted to the 2000 US census population. Vaccination rates were calculated for both low and high risk populations. 95% confidence intervals (95% CI) of each estimate were also calculated. The association between potential predictors of vaccination (demographic variables, socioeconomic status, high risk, and health care access and utilization variables) and vaccination status was assessed using bivariate analysis. We used logistic regression model to obtain odds ratios and their 95% confidence intervals for the association between predictor variables and vaccination status after adjusting for all potential confounding factors. Results: Vaccinated adults were more likely to be female, younger (20-29), Non-Hispanic white, married, born in the United States, have some education beyond high school, have a household income greater than $20000, health insurance coverage, a source of usual medical care, report a health status of good or higher, be non-smokers, and have no history of alcohol abuse. High risk adults comprised about 16% of adults who had received at least one dose of the Hepatitis B vaccine. Unvaccinated adults were more likely to be male, over the age of 40, Non-Hispanic white, born in the United States, married, have some education beyond high school, have a household income greater than $20,000, live in a household of 6 or fewer people, have health insurance coverage, and a source of usual care. When comparing the self reported vaccination status with serologic status, almost half of the adults who reported receiving all three doses of the vaccine tested negative for immunity. For all adults the prevalence increased from 23.4% to 39.1%. Compared to adults in 1999-2000, adults were twice as likely to report vaccination in 2005-2006 (OR=2.1 95% CI [1.77, 2.49]). Conclusions: Although, hepatitis B vaccination rates are rising, only 32% of high risk adults are vaccinated. The rise in vaccination rates in young adults is mostly related to childhood immunization strategies and not strategies aimed at adults. Older males, those with less than high school education, without health insurance coverage and a source of usual care were least likely to be vaccinated. More targeted interventions are needed to educate and vaccinate the adult population and to create a means for identifying those at risk and those already vaccinated.
338

Prevalência de marcadores sorológicos para hepatite B e C e potenciais fatores de risco em pacientes com diabetes mellitus de uma Unidade Básica Distrital de Saúde, Ribeirão Preto-SP, 2014 / Prevalence of serological markers for hepatitis B and C and potential risk factors in patients with diabetes mellitus at a Basic Health District Unit, Ribeirão Preto- SP, 2014.

Arrelias, Clarissa Cordeiro Alves 05 September 2017 (has links)
Estudo observacional transversal que teve como objetivos caracterizar os pacientes com diabetes mellitus segundo as variáveis demográficas e clínicas; estimar a prevalência de infecção pelo vírus da hepatite B e C e a cobertura vacinal contra hepatite B em pacientes com diabetes mellitus e identificar potenciais fatores de risco relacionados. A amostra de conveniência foi constituída de 255 pacientes com diabetes mellitus que compareceram à consulta médica nos ambulatórios de Endocrinologia e de Clínica Médica Integrado de Unidade Distrital de Saúde de Ribeirão Preto-SP, no período de julho a dezembro de 2014. As variáveis demográficas selecionadas foram sexo, idade e escolaridade e, as clínicas o uso de insulina, monitoramento da glicemia capilar, história de intervenções médicas, cirúrgicas, diagnósticas e terapêuticas e situações e comportamentos de risco para hepatite B e C. Os marcadores sorológicos investigados foram HBsAg, Anti-HBc IgG, Anti-HBc IgM, Anti-HBs e Anti-HCV. Considerou-se vacinação completa três ou mais doses da vacina contra hepatite B registrada. Para a coleta de dados utilizou-se um questionário, consulta ao registro de vacinação no Sistema Informatizado de Gestão em Saúde da Secretaria Municipal de Saúde e coleta de sangue venoso. Os dados foram apresentados por meio de estatística descritiva. A análise univariada das possíveis associações entre as variáveis demográficas e clínicas e os desfechos infecção pelo vírus da hepatite B e C e cobertura vacinal contra hepatite B, foi determinada pelos testes de Qui-quadrado corrigido por Pearson ou Teste exato de Fisher bicaudal e Wilcoxon para amostras não pareadas. Para a análise multivariada, foi construído um modelo de regressão logística onde foram incluídas as variáveis que exibiram p<0,2 na análise univariada. Valores de \'p\' inferiores a 5% foram considerados significativos. Os resultados mostraram que 16,8% dos pacientes apresentaram marcador Anti-HBc total reagente, 8,2% Anti-HBs isolado e 75% foram não reagentes para todos os marcadores de hepatite B. Nenhum caso de HBsAg reagente foi encontrado na amostra estudada. Quanto à infecção pelo vírus da hepatite C, 3,3% dos pacientes apresentaram marcador anti-HCV reagente. A prevalência de infecção pelo vírus da hepatite B (Anti-HBc reagente) em pacientes com diabetes mellitus foi de 16,8%, superior à nacional e mostrou-se diretamente associado ao tempo da doença. A prevalência de infecção pelo vírus da hepatite C (Anti-HCV reagente) foi de 3,3%, superior à nacional, mas não teve associação com as variáveis demográficas e clínicas investigadas. A cobertura vacinal contra hepatite B mostrou-se baixa (15%) em pacientes com diabetes mellitus evidenciando a sua vulnerabilidade a essa doença grave e potencialmente fatal. Maior escolaridade e o trabalho na área da saúde foram associados à melhor cobertura vacinal. Estes resultados fornecem subsídios importantes para a avaliação da prática clínica dos enfermeiros na atenção primaria à saúde para a prestação de cuidados relacionados à cobertura vacinal a pessoas com diabetes mellitus. Assim, esforços devem ser empenhados pelos profissionais e serviços de saúde para enfrentar o desafio de prover ampla cobertura vacinal a essa população, garantindo a prevenção da infecção pelo vírus da hepatite B e C / A cross-sectional observational study aimed at characterizing patients with diabetes mellitus according to demographic and clinical variables; to estimate the prevalence of hepatitis B and C virus infection and vaccine coverage in patients with diabetes mellitus and to identify potential related risk factors. The convenience sample consisted of 255 patients with diabetes mellitus who attended the medical consultation in the outpatient clinics of Endocrinology and Integrated Medical Clinic of the District Health Unit of Ribeirão Preto-SP, from July to December 2014. The selected demographic variables the use of insulin, capillary blood glucose monitoring, history of medical, surgical, diagnostic and therapeutic interventions and risky situations and behaviors for hepatitis B and C. The serological markers investigated were HBsAg, Anti -HBc IgG, Anti-HBc IgM, Anti-HBs and Anti-HCV. Three or more doses of the registered hepatitis B vaccine were considered complete vaccination. To collect data, a questionnaire was used, consulting the vaccination record of the Health Management Computerized System of Health of the Municipal Health Department and venous blood collection. The data were presented by means of descriptive statistics. Univariate analysis of possible associations between demographic and clinical variables and outcomes of hepatitis B and C virus infection and vaccine coverage against hepatitis B was determined by the Pearson-corrected chi-square test or Wilcoxon\'s exact Fisher\'s test for Unpaired samples. For the multivariate analysis, a logistic regression model was constructed in which variables that exhibited p <0.2 were included in the univariate analysis. Values of \'p\' below 5% were considered significant. The results showed that 16.8% of the patients presented total anti-HBc marker reagent, 8.2% Anti-HBs alone and 75% were non-reactive for all hepatitis B markers. No case of HBsAg reagent was found in the sample studied. Regarding hepatitis C virus infection, 3.3% of the patients presented anti-HCV marker reagent. The prevalence of hepatitis B virus (Anti-HBc reagent) in patients with diabetes mellitus was 16.8% higher than the national level and was directly associated with the time of diabetes mellitus. The prevalence of hepatitis C virus infection (Anti-HCV reagent) was 3.3%, higher than the national level, but had no association with the demographic and clinical variables investigated. Hepatitis B vaccination coverage was shown to be low (15%) in patients with diabetes mellitus evidencing their vulnerability to this serious and potentially fatal disease. Higher schooling and work in the health area were associated with better vaccine coverage. These results provide important insights for the evaluation of nurses\' clinical practice in primary health care for care related to vaccination coverage for people with diabetes mellitus. Thus, efforts must be made by health professionals and services to meet the challenge of providing ample vaccination coverage to this population, ensuring the prevention of hepatitis B and C virus infection
339

Idade com fator de risco para gravidade e complicações nos acidentes botrópicos atendidos no Hospital Vital Brazil do Instituto Butantan/SP / Age as a predictor of severity and complication on snakebites accidents of the genus Bothrops, admitted at Hospital Vital Brazil/Instituto Butantan/SP

Franco, Marília Miranda 03 April 2006 (has links)
Alguns estudos têm proposto que os acidente ofídicos em crianças estão associados a maior gravidade e ao maior risco de desenvolvimento de complicações comparados aos acidentes em adultos. Este estudo retrospectivo descreve as características de acidentes causados por serpentes do gênero Bothrops admitidos no Hospital Vital Brazil/Instituto Butantan/SP (HVB/IB) e compara a gravidade, e necessidade de soroterapia antiveneno e o risco para o desenvolvimento de complicações entre crianças (menores de 13 anos) e adultos. Trata-se de uma coorte histórica que utilizou dados de prontuários do arquivo do HVB/IB de dezembro de 1999 a junho de 2003. Foram incluídos no estudo pacientes que trouxeram a serpente ou apresentavam manifestações clínicas ou laboratoriais compatíveis com envenenamento botrópico. Não foi observada diferença estatisticamente significante na freqüência da gravidade dos envenenamentos, no número de ampolas administradas e na freqüência de complicações entre os dois grupos estudados. O estudo sugere que os acidentes ofídicos causados por serpentes do gênero Bothrops apresentam gravidade semelhante na avaliação admissional e evolução com a mesma proporção de complicações em crianças quando comparados aos acidentes em adultos / Some studies propose that the level of severity of the accidents caused by snakes in children can be associated with a stronger envenoming and a higher risk of later complication if compared to the same accidents in adults. This retrospective study aim to describe the caracteristics of snakebites acidents of the genus Bothrops, and compare their severities, necessity of antivenom, and the risk of developing later complications between children (less than 13 years) and adults, all the accidents where admitted at Hospital Vital Brazil/Instituto Butantan/SP, Brazil (HVB). This retrospective cohort study was carried out by using HVB\'s records of snakebite victims, from December 1999 to June 2003. Patients included were those who brought the snake and/or have the clinical or laboratorial presence of abnormalities compatible with Bothrops envenoming. No statistic differences were found between the two groups of this study concerning the severity of envenoming, number of antivenom vials and the frequency of complications. This study suggests that snakebite accidents are similar between adults and children. Age is not supposed to be a predictor of complication in such accidents
340

Aplicação de linhagens geneticamente modificadas de Bacillus subtilis no desenvolvimento de vacinas de mucosas contra patógenos entéricos. / Genetically modified Bacillus subtilis strains applied in the development of mucosal vaccines against enteric pathogens.

Paccez, Juliano Domiraci 03 December 2007 (has links)
Bacillus subtilis é uma bactéria gram positiva de solo, não patogênica, não colonizadora de tecidos, naturalmente transformável e formadora de esporos utilizada como modelo de estudo de bactérias gram-positivas. Essas características acarretam em vantagens para a produção de proteases de interesse industrial e para utilização como veículo de antígenos vacinais, porém a falta de vetores induzíveis torna sua utilização como ferramenta biológica pouco explorada. No presente trabalho descrevemos a construção de diferentes vetores capazes de expressar os antígenos subunidade B da toxina termo-lábil (LTB) e subunidade estrutural da fímbria CFA/I (CFAB) de Escherichia coli enterotoxigênica (ETEC) e avaliamos seu potencial vacinal. Foi avaliada a imunogenicidade de linhagens capazes de expressar LTB sob o controle de diferentes promotores: PgsiB (induzido em condições de estresse), PlepA (promotor constitutivo) e Pspac (induzido pela adição de IPTG) e em diferentes locais da célula (ancorada à parede celular ou secretada para o meio externo). Avaliamos ainda a imunogenicidade de linhagens capazes de co-expressar LTB e a listeriolisina O (LLO) de Listeria monocytogenes. O antígeno CFAB foi produzido no citoplasma ou ancorado à parede celular de B. subtilis em condições de estresse e as linhagens bacterianas administradas sozinhas ou conjuntamente com a toxina termo-lábil (LT) como adjuvante de mucosa. Camundongos imunizados com células ou esporos de B. subtilis recombinantes desencadearam respostas de anticorpos sistêmicos e secretados específicos para os antígenos (LTB e CFAB), não alterados pela adição do adjuvante. A expressão de LLO causou a supressão da resposta de anticorpos específicos para o antígeno LTB. Os resultados obtidos demonstram a viabilidade do uso de B. subtilis como veículo vacinal. / Bacillus subtilis is a gram positive, generally regarded as safe and spore forming soil bacteria used as a model for genetic and phisiological studies. This safety status allow its use as host for production of industrial protases and its application as vaccine vehicles, however the lack of epissomal inducible expression systems disable the exploration of this organism as a biotechnologic tool. In this work we describe the construction of epissomal vectors able to express the B subunit of the heat-labile toxin (LTB) and the structural subunit of the CFA/I fimbrae (CFAB) from the enterotoxigenic Escherichia coli (ETEC). We evaluate strains able to express LTB under the control of three promoters: PgsiB (stress inducible), PlepA (constitutive) e Pspac (IPTG inducible) and allowing the expression of LTB secreted or anchored to the cell wall We also evaluate the immunogenicity of strains able to co-express LTB and the listeriolysin O (LLO) from Listeria monocytogenes. CFAB was expressed in the cytoplasm or anchored to the cell wall and administred alone or with the mucosal adjuvant LT. Mice immunized both with cells or spores elicited secreted and systemic specific antibodies responses, which were not altered by the addition of the adjuvant LT. LLO expression suppressed the antibodies responses against LTB. The data shows the ability of B. subtilis to be used as vaccine vehicle.

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