Global ETD Search

281	Survival of infectious agents and detection of their resistance and virulence factors Tano, Eva January 2015 (has links) In the first study, three different transport systems for bacteria were evaluated. The CLSI M40-A guideline was used to monitor the maintenance of both mono- and polymicrobial samples during a simulated transportation at room temperature that lasted 0-48 h. All systems were able to maintain the viability of all organisms for 24 h, but none of them could support all tested species after 48 h. The most difficult species to recover was Neisseria gonorrhoeae, and in polymicrobial samples overgrowth was an observed problem. The aim of the second study was to study the presence of TSST-1 and three other important toxin genes in invasive isolates of Staphylococcus aureus collected during the years 2000-2012 at two tertiary hospitals. The genes encoding the staphylococcal toxins were detected by PCR, and whole-genome sequencing was used for analyzing the genetic relatedness between isolates. The results showed that the most common toxin was TSST-1, and isolates positive for this toxin exhibited a clear clonality independent of year and hospital. The typical patient was a male aged 55-74 years and with a bone or a joint infection. The third study was a clinical study of the effect of silver-based wound dressings on the bacterial flora in chronic leg ulcers. Phenotypic and genetic silver-resistance were investigated before and after topical silver treatment, by determining the silver nitrate MICs and by detecting sil genes with PCR. The silver-based dressings had a limited effect on primary wound pathogens, and the activity of silver nitrate on S. aureus was mainly bacteriostatic. A silver-resistant Enterobacter cloacae strain was identified after only three weeks of treatment, and cephalosporin-resistant members of the Enterobacteriaceae family were relatively prone to developed silver-resistance after silver exposure in vitro. The last study was undertaken in order to develop an easy-to-use method for simulating the laundering process of hospital textiles, and apply the method when evaluating the decontaminating efficacy of two different washing temperatures. The laundering process took place at professional laundries, and Enterococcus faecium was used as a bioindicator. The results showed that a lowering of the washing temperature from 70°C to 60°C did not affect the decontamination efficacy; the washing cycle alone reduced the number of bacteria with 3-5 log10 CFU, whereas the following tumble drying reduced the bacterial numbers with another 3-4 log10 CFU, yielding the same final result independent of the washing temperature. To ensure that sufficient textile hygiene is maintained, the whole laundering process needs to be monitored. The general conclusion is that all developmental work in the bacterial field requires time and a large strain collection.
282	Host and pathogen genetics associated with pneumococcal meningitis Lees, John Andrew January 2017 (has links) Meningitis is an infection of the meninges, a layer of tissue surrounding the brain. In cases of pneumococcal meningitis (where the bacterium Streptococcus pneumoniae is the causat- ive agent) this causes severe inflammation, requiring intensive care and rapid antibiotic treatment. The contribution of variation in host and pathogen genetics to pneumococcal meningitis is unknown. In this thesis I develop and apply statistical genetics techniques to identify genomic variation associated with the various stages of pneumococcal meningitis, including colonisation, invasion and severity. I start by describing the development of a method to perform genome-wide association studies (GWAS) in bacteria, which can find variation in bacterial genomes associated with bacterial traits such as antibiotic resistance and virulence. I then applied this method to longitudinal samples from asymptomatic carriage, and found lineages and specific variants associated with altered duration of carriage. To assess meningitis versus carriage samples I applied similar analysis techniques, and found that the bacterial genome is crucial in determining invasive potential. As well as bacterial serotype, which I found to be the main effect, I discovered many independent sequence variants associated with disease. Separately, I analysed within host-diversity during the invasive phase of disease and found it to be of less relevance to disease progression. Finally, I analysed host genotype data from four independent studies using GWAS and heritability estimates to determine the contribution of human sequence variation to pneumococcal meningitis. Host sequence accounted for some variation in susceptibility to and severity of meningitis. The work concludes with a combined analysis of pairs of bacterial and human sequences from meningitis cases, and finds variation correlated between the two.
283	Oropharyngeal carriage of respiratory bacteria among military conscripts Jounio, U. (Ulla) 02 October 2012 (has links) Abstract The aims of this work were to study the carriage of respiratory bacteria and to identify risk factors affecting pharyngeal colonisation by these pathogens among young Finnish men during military service, and also to investigate the role of mannose-binding lectin (MBL) concentrations and MBL2 gene polymorphisms in the carriage of respiratory bacteria. A total of 892 military recruits entering the Kainuu Brigade, including 224 men with asthma, were followed up prospectively to the end of their military service. Carriage of Streptococcus pneumoniae, Neisseria meningitidis and beta-haemolytic streptococci appeared to be higher during and at the end of military service than at the beginning. Smoking was found to be a significant risk factor for colonisation by these bacteria. S.pneumoniae was more common in the asthmatic than military conscripts in the non-asthmatic ones at the beginning of military service. A low MBL level increased the risk of carrying N. meningitidis and beta-haemolytic streptococci during military service among non-smokers but not among smokers. Low MBL levels producing MBL2 haplotypes seemed to be associated with the carriage of N. meningitidis and S. pneumoniae. Characterisation of all the oropharyngeal N.meningitidis isolates obtained (n=215) by phenotypic and genotypic methods showed that most of them belonged to the carriage-associated ST-60 clonal complex. Clonal complexes ST-41/44, ST-32, and ST-23, which have previously been associated with disease, also accounted for a third of the carriage strains. Furthermore, a significant association was indicated between an acute upper respiratory infection and oropharyngeal carriage of the virulent meningococcal ST-23 clone. In conclusion, the results reported here show a significant increase in bacterial carriage during military service and provide new information on the association between MBL and carriage of respiratory bacteria. These findings also highlight the importance of smoking cessation, especially among military conscripts, who have been found to be a risk group for invasive bacterial diseases, and they also point to the importance of meningococcal vaccination for military recruits and the need for an efficacious vaccine against serogroup B meningococci. / Tiivistelmä Hengitystieinfektiot ovat yleisiä varusmiespalvelun aikana. Myös oireeton bakteerien nielukantajuus on lisääntynyt. Useimmiten infektiot ovat lieviä virusinfektioita, mutta bakteerien nielukantajuus voi johtaa myös vaikeisiin bakteeritulehduksiin. Tämän väitöskirjatyön tarkoituksena oli tutkia bakteerien nielukantajuutta varusmiespalveluksen alkaessa ja päättyessä sekä mahdollisten hengitystieinfektioiden aikana ja näin saada uutta tietoa bakteerien nielukantajuuteen vaikuttavista tekijöistä. Lisäksi tavoitteena oli selvittää mannoosia sitovan lektiinin (MBL) sekä MBL2-geenin polymorfismien yhteyttä bakteerien nielukantajuuteen. Työn tarkoituksena oli myös feno- ja genotyypittää varusmiehiltä palveluksen aikana eristetyt meningokokkikannat ja verrata niitä vastaavana ajankohtana invasiivista tautia sairastaneista henkilöistä eristettyihin meningokokkikantoihin. Tutkimuksessa seurattiin prospektiivisesti 892 varusmiestä, jotka suorittivat asepalveluksen Kainuun Prikaatissa vuosina 2004–2006. Tutkimukseen osallistuneista varusmiehistä 224:llä oli astma. Tutkimuksessa havaittiin, että oireeton bakteerien nielukantajuus lisääntyy merkitsevästi varusmiespalveluksen aikana. Lisäksi havaittiin, että tupakointi oli merkittävä itsenäinen riskitekijä pneumokokin, meningokokin sekä beta-hemolyyttisten streptokokkien nielukantajuudelle varusmiespalveluksen aikana. Astmaatikkojen pneumokokin nielukantajuus varusmiespalveluksen alussa oli yleisempi kuin terveiden varusmiesten. Tutkimuksessa osoitettiin myös pienen seerumin MBL-pitoisuuden sekä MBL2-geenin polymorfismin eksoni 1:n alueella ja geenin säätelyalueella olevan riskitekijöitä meningokokin, pneumokokin sekä beta-hemolyyttisten streptokokkien nielukantajuudelle tupakoimattomilla varusmiehillä. Meningokokin nielukannoista jopa kolmasosa kuului genotyyppiryhmään, jonka on aiemmissa tutkimuksissa havaittu liittyvän invasiiviseen tautiin. Tutkimuksessa osoitettiin myös tietyn hyperinvasiivisen meningokokin genotyypin (ST-23) liittyvän hengitystieinfektioepisodeihin. Tässä väitöskirjatyössä osoitettiin, että bakteerien nielukantajuus lisääntyy merkitsevästi varusmiespalveluksen aikana ja että oireettomilla varusmiehillä tavataan myös hyperinvasiivisia meningokokkikantoja. Tutkimus antoi myös uutta tietoa hyperinvasiivisten meningokokin genotyyppien liittymisestä hengitystieinfektioihin sekä MBL:n vaikutuksesta bakteerien nielukantajuuteen. Tutkimushavainnot tukevat tupakoimattomuuden edistämisen tärkeyttä myös varusmiespalveluksen aikana. Neisseria meningitidis Streptococcus pneumoniae asthma beta-haemolytic streptococci carrier state mannose-binding lectin military conscript smoking mannoosia sitova lektiini meningokokki nielukantajuus pneumokokki tupakointi varusmiehet
284	MicroRNAs cause micro changes: Regulation of expression of membrane-associated complement inhibitors and its effect on Neisseria gonorrhoeae Savin, Avital 18 May 2021 (has links) No description available. Biology Biomedical Research Cellular Biology Genetics Health Immunology Medicine Microbiology Molecular Biology MicroRNAs Neisseria gonorrhoeae mCIs protein regulation antibiotic resistance CD46 CD55 CD59 complement
285	Surveillance de seconde génération du VIH chez les travailleuses du sexe et leurs partenaires sexuels masculins au Sénégal : étude dans deux zones d'intervention du Projet SIDA 3 Cisse, Daouda 11 April 2018 (has links) Objectifs : Cette étude transversale effectuée sur les travailleuses du sexe (TS) et leurs clients dans 2 zones géographiques d'intervention du Projet SIDA 3 au Sénégal avait pour objectifs: de déterminer la prévalence et les rapports de prévalence des facteurs associés aux virus de l'immunodéficience acquise (VIH) et des infections sexuellement transmissibles (IST), chez les TS et leurs clients et d'estimer le potentiel de transmission du VIH et des IST à la population générale par le biais des TS et de leurs clients. Méthodologie : Les prélèvements vaginal, urinaire et sanguin ont été respectivement analysés au laboratoire par Polymérase Chain Réaction (PCR) pour la détection de gonocoque ou chlamydia et Enzyme Linked Sorbent Assay (ELISA) pour le VIH, tandis qu'un test Leucocytes Esterase Dipstick (LED) détectait les leucocytes dans l'urine. Les proportions et les données continues ont été respectivement comparées, en utilisant les tests du X2 ou exact bilatéral de Fisher et test t de Student. Par régression binomiale avec GENMOD en analyse univariée ou multivariée, les rapports de prévalence ont été les estimés des forces d'association. Toutes les analyses statistiques ont été réalisées grâce au logiciel SAS 8 ou 9. L'étude a été approuvée par le comité national éthique du Sénégal. Résultats : Chez les TS, les prévalences du VIH et des IST étaient respectivement de 26,9% (65/242) et 09,8% (21/214) tandis que chez leurs clients, elles étaient de 2,1% (6/285) et 1,4% (4/294). En analyse multivariée chez les TS : l'âge, le nombre d'épisodes IST dans la vie et le nombre de partenaires dans la dernière semaine de travail restaient ensemble toutes significativement associées au VIH. On notait 2 fois plus d'IST chez les TS clandestines que chez les TS officielles (p=0,08) alors qu'il y avait 3 fois moins de VIH chez les premières que chez les dernières (p=0,001). Entre le test LED et l'analyse PCR chez les clients, les sensibilité, spécificité, valeurs prédictives positive et négative étaient respectivement de 100%, 91%, 16% et 100%. La fraction du risque chez le client, attribuable au contact infectant avec la TS était de 67% et 5,2% de l'ensemble des femmes del5-49 ans des sites géographiques étudiés ont été indirectement exposées aux IST/VIH par le biais des clients. Conclusion : Afin d'avoir des données fiables permettant d'établir des programmes appropriés de lutte contre les IST/VIH au Sénégal, des enquêtes répétées auprès des TS et de leurs clients s'avèrent nécessaires Sida -- Épidémiologie -- Sénégal
286	STRUCTURAL INSIGHT INTO THE BIOGENESIS OF OUTER MEMBRANE PROTEINS IN PATHOGENIC NEISSERIA Evan M Billings (18424239) 23 April 2024 (has links) <p dir="ltr">The obligate human pathogen, <i>Neisseria gonorrhoeae </i>(Ngo), has continued to acquire widespread antibiotic resistance. Ngo is the causative agent of the sexually transmitted disease gonorrhea, and can cause additional complications such as endocarditis, septicemia, and infertility if left untreated. The Centers for Disease Control and Prevention (CDC) now recommends a treatment option of a single drug of last resort, ceftriaxone, leaving a need for novel therapeutics against this pathogen.</p><p dir="ltr">Like many bacterial pathogens, Ngo is Gram-negative consisting of both an inner membrane (IM) and outer membrane (OM). The transmembrane proteins in the IM have primarily an α-helical fold, while the transmembrane proteins in the OM have a β-barrel fold. These β-barrel outer membrane proteins (OMPs) have essential functions in regulating the homeostasis and nutrient acquisition of the cell, in addition to promoting virulence in pathogenic strains. These OMPs are folded and inserted into the outer membrane by the β-barrel assembly machinery (BAM) complex. In <i>E. coli,</i> BAM consists of five proteins: BamA, an OMP itself, and four lipoproteins, BamB, C, D, and E.</p><p dir="ltr">Here we present our work toward the structural characterization of BAM from Ngo (<i>Ng</i>BAM) using cryo-EM. Ngo lack a homolog of BamB and may function as a four component complex. To better understand the mechanism for how <i>Ng</i>BAM is able to mediate OMP biogenesis despite lacking a component that is critical in <i>E. coli</i>, we determined the cryo-EM structure of <i>Ng</i>BAM, which revealed several distinct features including that the barrel domain of BamA being observed in the inward-open conformation. We also investigated <i>Ng</i>BAM as a therapeutic target, by studying its interaction with a novel broad spectrum antibiotic darobactin. We first showed darobactin is effective against the laboratory strains of NgoFA19 and ATCC-49226. We also show it is effective against the human isolate WHOX, with a comparable MIC to ceftriaxone. To structurally characterize the mechanism of inhibition by darobactin, we used cryo-EM to determine the structures of <i>Ng</i>BAM bound to two darobactin compounds. In these structures, darobactin binding was accompanied by large conformational changes in <i>Ng</i>BamA. To further probe the effects of darobactin on the conformational plasticity of <i>Ng</i>BAM we performed experiments using double electron-electron resonance spectroscopy, which showed distance changes between the engineered site labels consistent with the conformational changes observed in our structural observation. In addition, narrowing of the peak distributions indicated that darobactin binding was reducing the overall conformational heterogeneity of the complex. Taken together, the work presented here contributes to the understanding of how <i>Ng</i>BAM functions in folding and inserting OMPs and provides a foundation for future structure based drug design of darobactin and other potential compounds.</p> BAM cryo-EM Neisseria gonorrhoeae structural biology outer membrane proteins (OMPs) beta barrel membrane proteins protein folding gram-negative bacteria antibiotic
287	L’HPr, une protéine clé dans l’établissement de la virulence chez Neisseria meningitidis / The HPr, a key protein in Neisseria meningitidis virulence Nait Abdallah, Jamila 12 October 2011 (has links) Neisseria meningitidis (Nm) est un germe commensal du rhinopharynx ayant pour seul hôte l’homme. Malgré un portage asymptomatique largement répandu, et pour des raisons encore inconnues, elle peut échapper au système immunitaire de l’hôte et devenir pathogène provoquant ainsi méningite et septicémie pouvant être mortelles principalement chez les enfants. Au cours du processus infectieux, Nm alterne entre des phases de colonisation et de dissémination, et se retrouve alors confrontée à différents environnements. L’adaptation rapide à ces variations, par modulation de l’expression des gènes de virulence, représente un facteur important dans sa pathogénie. Les facteurs qui contribuent à la virulence de Nm sont essentiellement des structures présentes à la surface de la bactérie parmi lesquelles les pili et la capsule. Les gènes codant ces facteurs sont sous le contrôle de la protéine CrgA, régulateur transcriptionnel de la famille LysR qui intervient lors de l’adhésion de Nm aux cellules humaines. La protéine CrgA régule négativement sa propre expression ainsi de celle des gènes impliqués dans la synthèse de la capsule (sia) et des pili (pilE et pilC1). Par ailleurs, le PTS est un système de transduction du signal qui intervient, par phosphorylation ou via des interactions protéine/protéine, dans le transport des sucres et dans la régulation du métabolisme du carbone. Chez Nm, ce système est incomplet (constitué des protéines EI, HPr, et deux EIIA), il n’est donc pas fonctionnel pour le transport des sucres mais aurait pu conserver ses fonctions régulatrices. Nous avons montré que les protéines du PTS de Nm étaient actives in vitro et in vivo et que la cascade de phosphorylation du PTS était fonctionnelle. Nous avons également montré que l’inactivation du gène ptsH, codant la protéine HPr, entrainait une diminution significative de la synthèse de la capsule, une augmentation de l’adhésion du mutant aux cellules épithéliales humaines et une augmentation de l’expression de crgA. De ce fait, l’absence de l’HPr semble empêcher la répression de crgA et par conséquent celle des gènes sia. Par ailleurs, des expériences de co-immunoprécipitation, nous ont permis de mettre en évidence que l’HPr interagissait directement avec la protéine CrgA in vitro et in vivo. Ces résultats suggèrent que la protéine HPr interviendrait dans la régulation de l’expression des gènes de virulence de Nm via la régulation de l’expression de crgA. Ainsi, un lien entre métabolisme du carbone et virulence a été mis en évidence chez Nm. / Neisseria meningitidis (Nm) is a commensal bacterium of the nasopharynx, which only colonizes humans. Despite a large number of asymptomatic carriers, and for reasons so far unknown, Nm occasionally becomes virulent, escaping the host’s immune system and causing septicaemia and meningitis, the latter being potentially lethal, mostly in children.During the infectious process, Nm alternates between phases of colonization and dissemination, each time facing different environments. This rapid adaptation to the changing environment occurs via the modulation of the expression of virulence genes and represents an important factor of pathogenicity. The structures involved in virulence in Nm are mainly present at the surface of the bacterium, including the pili and the capsule. The genes coding for these structures are controlled by the CrgA protein, a transcriptional regulator of the LysR family, which is induced during the adhesion of Nm to human cells. CrgA negatively regulates its own expression as well as the expression of those genes implicated in the synthesis of the capsule (sia) and pili (pilE and pilC1).Moreover, the PTS is a signal transduction system, which is involved, via phosphorylation or protein/protein interactions, in the transport of sugars and the regulation of the carbon metabolism. In Nm, the PTS is incomplete (only composed of the proteins EI, HPr and two EIIA), thus not functioning in the transport of sugars but it may have conserved regulatory functions.In this work, we demonstrate that the PTS proteins in Nm are active in vitro and in vivo and that the phosphorylation cascade of the PTS is functional. We further show that the inactivation of the ptsH gene, coding for the HPr protein, significantly reduces the synthesis of the capsule, enhances the adhesion of the mutants to human epithelial cells and increases the expression of crgA. Thus, the absence of HPr seems to inhibit the repression of crgA and as a consequence also the repression of the sia genes. Furthermore, from co-immunoprecipitation experiments we provide evidence that HPr directly interacts with the CrgA protein in vitro and in vivo. These results suggest that the HPr protein in Nm regulates the expression of the virulence genes via the regulation of crgA expression. Thus, we provide evidence of a link between carbon metabolism and virulence in Nm. Neisseria meningitidis Virulence Système des phosphotransférases (PTS) PTS incomplet Métabolisme du carbone CrgA Adhésion Régulateur transcirptionnel Phosphorylation Interactions protéine/protéine Régulation de gènes Transport des sucres Capsule Neisseria meningitidis Virulence Incomplete PTS Carbon metabolism CrgA Adhesion Capsule Transcriptional regulator Phosphorylation Protein/protein interaction Gene regulation Carbohydrate uptake
288	Impacto da vacinação contra o meningococo C na morbidade da doença meningocócica / Impact of meningococcal C vaccination on invasive meningococcal disease in Brazil Tomich , Lísia Gomes Martins de Moura 15 August 2016 (has links) Submitted by Luciana Ferreira (lucgeral@gmail.com) on 2016-09-28T11:44:16Z No. of bitstreams: 2 Dissertação - Lísia Gomes Martins de Moura Tomich - 2016.pdf: 2901743 bytes, checksum: 22cd41bfc4499cfd4754d856635357af (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Approved for entry into archive by Luciana Ferreira (lucgeral@gmail.com) on 2016-09-28T11:44:45Z (GMT) No. of bitstreams: 2 Dissertação - Lísia Gomes Martins de Moura Tomich - 2016.pdf: 2901743 bytes, checksum: 22cd41bfc4499cfd4754d856635357af (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Made available in DSpace on 2016-09-28T11:44:45Z (GMT). No. of bitstreams: 2 Dissertação - Lísia Gomes Martins de Moura Tomich - 2016.pdf: 2901743 bytes, checksum: 22cd41bfc4499cfd4754d856635357af (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Previous issue date: 2016-08-15 / Conselho Nacional de Pesquisa e Desenvolvimento Científico e Tecnológico - CNPq / INTRODUCTION: Routine infant immunization with meningococcal C conjugate vaccine (MenC-V) started in Brazil in November 2010, administered at three, five and 12 months of age with no catch-up for older age-groups. However, by March 2010, a vaccination campaign with MenC-V was performed in Salvador in individuals under five years-old, and from 10 to 24 yearsold. In São Paulo state, the outbreaks occurred in teenagers and young adults prompting one-time vaccination campaign from 2010 to 2014 targeting these age-groups. OBJECTIVE: To assess the direct and indirect impact (herd effect) of vaccination on invasive meningococcal disease (MD) for capsular group C (MenC) four years after the introduction of MenC-V in three scenarios: i) Brazil as a whole (routine vaccination in childhood only); ii) Brazil except for Salvador (vaccination campaign with teenagers during the year of MenC-V introduction); and iii) São Paulo state (vaccination campaign for adolescents and young adults during 2010-2014 to control outbreaks). METHODS: We performed an ecological quasi-experimental design from 2008 to 2014 using data from the National Reference Laboratory for Meningitis, and data from the National Information System for Notifiable Diseases. A deterministic linkage was performed between the two databases to improve the accuracy of the detection of MD, especially in capsular groups. An interrupted time-series analysis was conducted using the Holt-Winters technique to control for pre-existing trends and seasonal variations. The MenC vaccination impact was evaluated as the percentage of reduction in the incidence rates of MenC in the post-vaccination period (2012 to 2014), using the pre-vaccination period (2008 to 2010) to estimate what would be expected on the post-vaccination period, whether the vaccination had not been introduced. For Salvador, we analyzed the effect of the vaccination on the number of MenC cases. RESULTS: A total of 18,136 invasive MD cases were analyzed. For Brazil as a whole, the vaccination reduced 67.4% (lower 95%CI 42.5%) the rates for MenC for infants under 12 months, 92.3% (lower 95%CI 77.7%) for the age-group 12-23 months, and 65.7% (lower 95%CI 28%) for children aged 2-4 years. Indirect impact (20-24.7%) was observed in the age-group 5-19 years. When excluding Salvador from the analysis of Brazil, the indirect impact was observed only for children in the age-group 5-9 years. In the scenario of São Paulo state, similarly to Brazil, significant impact was observed in the target age-groups, in addition to indirect impact in the age group 5-9 years. In Salvador, in addition to the effect on the vaccinated population a sharp and sustainable decline of MenC cases was observed in all age-groups not target for vaccination. Overall, 1,170 cases of MenC were averted in Brazil after the introduced of Men-C vaccination. CONCLUSION: The strategy of catch-up for adolescents and young adults, especially during the year of MenC-V introduction may lead to rapid and sustainable herd effect. / A vacina meningocócica conjugada contra o grupo capsular C (MenC-V) foi introduzida no calendário de imunização infantil brasileiro em novembro de 2010, sendo administrada aos três, cinco e 12 meses de idade sem catch-up para os demais grupos etários. Entretanto, em março de 2010, uma campanha de vacinação com MenC-V foi realizada em Salvador para indivíduos menores de cinco anos de idade e de 10 a 24 anos. No estado de São Paulo os surtos ocorreram em adolescentes e adultos jovens, determinando campanhas de vacinações de bloqueio nessa faixa etária nos anos de 2010 a 2014. OBJETIVO: Avaliar o impacto direto e indireto (rebanho) da vacinação nas taxas de incidência de doença meningocócica (DM) invasiva pelo grupo capsular C (MenC) após quatro anos da introdução da MenC-V em três cenários: i) Brasil como um todo (imunização de rotina somente de crianças); ii) Brasil exceto Salvador (campanha de vacinação em adolescentes no ano de introdução da MenCV); e iii) estado de São Paulo (vacina de rotina na infância e vacinações de bloqueio em adolescentes e adultos jovens para controlar surtos). MÉTODOS: Foi realizado um estudo ecológico quasi-experimental para avaliar o impacto da vacinação em série histórica de 2008 a 2014 usando os bancos de dados do Laboratório Nacional de Referência para Meningites Bacterianas, Instituto Adolfo Lutz (IAL) e o Sistema de Informação de Agravos de Notificação (Sinan). Um processo de vinculação (linkage) determinístico entre as duas bases foi realizado para melhorar a acurácia da detecção de casos de DM, especialmente de grupo capsulares. Uma análise de série temporal interrompida foi conduzida utilizando a técnica de Holt-Winters para controlar por tendência pré-existente e variações sazonais. O desfecho foi taxa de MenC. O impacto da vacinação foi avaliado pelo percentual de redução da incidência de MenC no período pós-vacinal (2012 a 2014), utilizando o período pré-vacinal (2008 a 2010) para estimar o que seria esperado no período pós-vacinal, caso a vacinação não tivesse sido introduzida. Para Salvador foi analisado o efeito da MenC-V no número de casos de MenC. RESULTADOS: Um total de 18.136 casos de DM invasiva foram analisados. Para o Brasil como um todo, a vacinação reduziu significativamente a DM por MenC na faixa etária alvo, com redução de 67,4% (limite inferior do IC95% 42,5%) em menores de 12 meses, 92,3% (limite inferior do IC95% 77,7%) para faixa etária de 12-23 meses e 65,7% (limite inferior do IC95% 28%) em crianças de 2-4 anos, e efeito rebanho foi observado na faixa etária de 5 a 19 anos com 20-24,7%. Quando se exclui Salvador na análise do Brasil, impacto indireto significativo foi observado somente em crianças de 5-9 anos. No cenário São Paulo, semelhante ao Brasil, observou-se impacto estatisticamente significante nas faixas etárias alvo do PNI, além do efeito rebanho na faixa etária de 5-9 anos de idade. Para Salvador, o impacto da vacinação apresentou um declínio acentuado e sustentável em todas as faixas etárias fora do alvo da vacinação. Ao todo, 1.170 casos de MenC foram evitados no período estudado. CONCLUSÃO: A estratégia de vacinação de catch-up em adolescentes e adultos jovens, especialmente no ano de introdução da MenC-V, promoveu um rápido e sustentável rebanho. Neisseria meningitidis Doença meningocócica invasiva Vacinas meningocócicas Impacto da vacinação Vigilância Linkage de dados Série temporal interrompida Efeito rebanho Neisseria meningitidis Medical record linkage Serogroup C meningococcal meningitis Meningococcal meningitis Meningococcal infections Meningococcal vaccines Interrupted time series analysis Epidemiology Herd effect SAUDE COLETIVA::EPIDEMIOLOGIA
289	Novel Complement Blocking Antibodies Against Serogroup B <em>N. meningitidis</em>: A Dissertation Dutta Ray, Tathagat 23 July 2010 (has links) N. meningitidis is a common commensal of the human upper respiratory tract and a leading cause of bacterial meningitis and septicemia worldwide. The classical pathway of complement (C) is essential for both naturally acquired and vaccine induced immunity against N. meningitidis. Qualitative and/or quantitative differences in anti-meningococcal antibodies (Abs) in serum is one reason for variations in C-dependent bactericidal Ab activity among individuals. I showed that IgG isolated from select individuals could block killing of group B meningococci by Abs that were otherwise bactericidal. Ligand overlay immunoblots revealed that these blocking IgG Abs were directed against a meningococcal antigen called H.8, Killing of meningococci in reactions containing bactericidal mAbs and human blocking Abs was restored when blocking Ab binding to meningococci was inhibited (or competed for) using either synthetic peptides corresponding to H.8 or a non-blocking mAb against H.8. Further, genetic deletion of H.8 from target organisms abrogated blocking. The Fc region of the blocking IgG was required for blocking because F(ab)2 fragments alone generated by pepsin treatment were ineffective. Blocking required IgG glycosylation; deglycosylation of blocking IgG with peptide:N-glycanase (PNGase) eliminated blocking. C4 deposition mediated by a bactericidal mAb directed against a meningococcal vaccine candidate, called factor H-binding protein (fHbp), was reduced by blocking Ab. Anti-fHbp-mediated C4 deposition was unaffected, however, by deglycosylated blocking IgG. Although preliminary, our data suggests blocking of serum bactericidal activity by human anti-H.8 blocking antibody may require mannan-binding lectin (MBL), which itself is a complement activator. Also, whether MBL recruits a complement inhibitor(s) that facilitates blocking remains to be determined. In conclusion, we have identified H.8 as a meningococcal target for novel blocking antibodies that are commonly found in human serum. Blocking Ab may reduce the efficacy of meningococcal vaccines. We propose that outer membrane vesicle-containing meningococcal vaccines may be more efficacious if purged of subversive immunogens such as H.8. Neisseria meningitidis Serogroup B Meningococcal Vaccines Amino Acids, Peptides, and Proteins Bacteria Bacterial Infections and Mycoses Environmental Public Health Immunology and Infectious Disease Investigative Techniques Nervous System Diseases Therapeutics
290	Antibiotic susceptibility and resistance in Neisseria meningitidis : phenotypic and genotypic characteristics Thulin Hedberg, Sara January 2009 (has links) Neisseria meningitidis, also known as the meningococcus, is a globally spread obligate human bacterium causing meningitis and/or septicaemia. It is responsible for epidemics in both developed and developing countries. Untreated invasive meningococcal disease is often fatal, and despite modern intensive care units, the mortality is still remarkably high (approximately 10%). The continuously increasing antibiotic resistance in many bacterial pathogens is a serious public health threat worldwide and there have been numerous reports of emerging resistance in meningococci during the past decades. In paper I, the gene linked to reduced susceptibility to penicillins, the penA gene, was examined. The totally reported variation in all published penA genes was described. The penA gene was highly variable (in total 130 variants were identified). By examination of clinical meningococcal isolates, the association between penA gene sequences and penicillin susceptibility could be determined. Isolates with reduced susceptibility displayed mosaic structures in the penA gene. Two closely positioned nucleotide polymorphisms were identified in all isolates with reduced penicillin susceptibility and mosaic structured penA genes. These alterations were absent in all susceptible isolates and were successfully used to detect reduced penicillin susceptibility by real-time PCR and pyrosequencing in paper II. In papers III and IV, antibiotic susceptibility and characteristics of Swedish and African meningitis belt meningococcal isolates were comprehensively described. Although both populations were mainly susceptible to the antibiotics used for treatment and prophylaxis, the proportion of meningococci with reduced penicillin susceptibility was slightly higher in Sweden. A large proportion of the African isolates was resistant to tetracycline and erythromycin. In paper V, the gene linked to rifampicin resistance, the rpoB gene, was examined in meningococci from 12 mainly European countries. Alterations of three amino acids in the RpoB protein were found to always and directly lead to rifampicin resistance. A new breakpoint for rifampicin resistance in meningococci was suggested. The biological cost of the RpoB alterations was investigated in mice. The pathogenicity/virulence was significantly lower in rifampicin resistant mutants as compared with susceptible wild-type bacteria. Neisseria meningitidis meningococcal disease antibiotic resistance antibiotic susceptbility biological cost PCR sequencing Cell and Molecular Biology Cell- och molekylärbiologi Microbiology in the medical area Microbiology in the medical area Microbiology in the medical area

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