• Refine Query
  • Source
  • Publication year
  • to
  • Language
  • 82
  • 31
  • 24
  • 13
  • 7
  • 6
  • 5
  • 2
  • 2
  • 2
  • 1
  • 1
  • 1
  • Tagged with
  • 202
  • 202
  • 42
  • 23
  • 20
  • 19
  • 17
  • 17
  • 15
  • 15
  • 14
  • 13
  • 13
  • 13
  • 12
  • 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.
121

The toxigenic element of Clostridium difficile strain 10463 and its transcriptional analysis in strains which differ in toxigenicity

Hammond, Georgia Ann 02 March 2006 (has links)
Clostridium difficile is a Gram positive, anaerobic bacterium which produces two potent protein toxins, A and B. The genes for toxins A and B have been previously cloned and sequenced and lie within 1.4 kb of each other. Upstream and downstream boundaries between sequences shared by both toxigenic and nontoxigenic strains and those sequences which are unique to toxigenic strains were established. A toxigenic element was defined in C. difficile strain 10463 which is 19.6 kb in length and is comprised of five open reading frames, including the toxin A and B genes. One of these open reading frames is previously unidentified and is located upstream of toxin B. Products of Polymerase Chain Reaction (PCR) amplification of three regions in the toxigenic element: the upstream boundary, the downstream boundary, and the region between the toxin A and B genes, were all identical in length in six toxigenic strains, indicating that the toxigenic element is conserved among these strains. A short fragment unique to nontoxigenic strains and occupying the same position on the chromosome as the toxigenic element was identified. peR products of this region were identical in length in three nontoxigenic strains. Transcriptional analyses were undertaken using probes to each of the five open reading frames in the toxigenic element. Transcripts were detected for four of the open reading frames which are contiguous and transcribed in the same direction. In addition, a very large transcript, corresponding to the length of the four open reading frames and processing intermediates were detected, indicating that the toxin genes are cotranscribed. A promoter region and processing sites were identified. Sizes were determined for each of the individual transcripts which correspond well with the sizes of the open reading frames. Six toxigenic strains which vary considerably in toxin production were selected for analysis to determine whether DNA sequence variation could account for the observed differences in toxin production. DNA restriction fragment length polymorphisms were examined, toxin-specific transcripts were analyzed, and sequences of regulatory regions were determined and compared. Whereas quantitative differences in toxin-specific transcripts were found among the toxigenic strains, the remaining analyses showed that DNA sequences were conserved among these strains. / Ph. D.
122

Transdisciplinary Strategies for the Characterization of Mucosal Immune Responses to Enteric Pathogens

Viladomiu Pujol, Monica 31 July 2015 (has links)
The gastrointestinal mucosal immune system has the daunting task of maintaining immune homeostasis by eliminating potentially harmful microorganisms and limiting tissue injury while inducing tolerogenic responses to luminal antigens including innocuous food, commensal bacteria and self-antigens. This carefully orchestrated system depends on elaborate down-regulating mechanisms that mediate and maintain a state of tolerance under normal conditions. Changes in such delicate balance are linked to the development of gastrointestinal pathology as well as systemic disease states. Despite the rapid increase in our appreciation of the gastrointestinal immune system, there is still a major disconnect between the description of how mucosal immune responses are organized and controlled and an insufficient mechanistic understanding of how such responses shape and influence disease outcome and pathogenesis. By using model enteric microorganisms Helicobacter pylori and Clostridium difficile, this dissertation presents a systematic effort to generate novel mechanistic hypothesis based on computational predictions and experimentally elucidate the mechanisms of action underlying mucosal immune responses and pathology in the gut. In this thesis I present i) an overview on mucosal immunology and the need to develop novel therapeutics that limit the pathogenic effects of invading bacteria while maintaining their protective functions, ii) the role of miRNAs in the modulation of immune responses to enteric pathogens, iii) the mechanisms by which Helicobacter pylori is able to limit effector inflammatory responses required for bacterial clearance thus favoring tolerance over immunity, iv) intracellular mechanisms of immune evasion that contribute to bacterial persistence and chronic infection. The knowledge generated throughout this dissertation exemplifies how a combination of computational modeling, immunoinformatics and experimental immunology holds enormous potential for discovering unforeseen targets and developing novel vaccines and cures for infectious, allergic and immune-mediated diseases. / Ph. D.
123

Systems Immunology Approaches for Precision Medicine

Leber, Andrew James 20 June 2017 (has links)
The mucosal immune system encompasses a wide array of interactions that work in concert to protect an individual from harmful agents while retaining tolerance to molecules, microbes, and self-antigens that present no danger. The upheaval in the regulation-response balance is a critical aspect in both infectious and immune-mediated disease. To understand this balance and methods of its restoration, iterative and integrative modeling cycles on the pathogenesis of disease are necessary. In this thesis, I present three studies highlighting phases of a systems immunology cycle. Firstly, the thesis provides a description of the construction of a computational ordinary differential equation based model on the host-pathogen-microbiota interactions during Clostridium difficile infection and the use of this model for the development of the hypothesis that host-antimicrobial peptide production may correlate with increased disease severity and promote increased recurrence. Secondly, it provides insight into the necessity of trans-disciplinary analysis for the understanding of novel molecular targets in disease through the immunometabolic regulation of CD4+ T cell by NLRX1 in inflammatory bowel disease. Third, it provides the assessment of novel therapeutics in disease through the evaluation of LANCL2 activation in influenza virus infection. In total, the computational and experimental strategies used in this dissertation are critical foundational pieces in the framework of precision medicine initiatives that can assist in the diagnosis, understanding, and treatment of disease. / Ph. D. / Many diseases are a result of altered patterns of interaction between the body, bacteria, viruses or nutrients. When these patterns are altered, inflammation occurs. If not controlled, the inflammation can cause pain, damage to the affected area, and other specific symptoms depending on the type of disease. This dissertation details the use of alternative methods of treating disease and analyzing disease in the context of Clostridium difficile infection, inflammatory bowel disease and influenza infection. It provides insight into the development of computational models with equations to capture the response patterns. It assesses the connections between immunology and metabolism that can lead to inflammation. And, it identifies a new therapeutic target for influenza infection. Together, these three phases are important pieces toward a future with improved understanding of disease and treatments that can be specific and customized for every individual.
124

Spores of C. difficile in hospital air

Snelling, Anna M., Beggs, Clive B., Kerr, Kevin G., Shepherd, Simon J. January 2010 (has links)
No
125

Impact des caractéristiques des hôpitaux québécois sur le taux d'incidence d'infection à "Clostridium difficile"

Savard, Andréanne 24 April 2018 (has links)
Introduction: Les infections nosocomiales à Clostridium difficile (C. difficile) représentent un problème majeur de santé publique. La surveillance provinciale québécoise a identifié des facteurs de risque non-modifiables de l’infection(ex.: mission de l’hôpital, nombre de lits), ne permettant toutefois pas de cibler une intervention. Objectifs: Cette étude a pour but: 1)d’identifier les facteurs de risque et/ou protecteurs modifiables associés au taux d’incidence d’infection à C. difficile dans les hôpitaux québécois; 2)d’évaluer si les facteurs sont les mêmes selon le type de mission de l’hôpital (universitaire ou non-universitaire); 3)d’expliquer l’association entre le type de mission et le taux d’incidence de l’infection. Méthodologie: Les facteurs de risque et/ou protecteurs ont été recueillis à l’aide d’un questionnaire sur les mesures de prévention et contrôle des infections à C. difficile dans les hôpitaux(INSPQ 2009-2010). La mesure de résultat est le taux d’incidence de l’infection(2009-2010). Nous avons utilisé des modèles de Poisson multivariés prédictifs pour répondre aux deux premiers objectifs et un modèle explicatif ajusté pour différents facteurs confondants pour répondre au troisième objectif. Résultats: Les facteurs associés à un taux d’incidence plus élevé dans le modèle prédictif pour tous les hôpitaux sont: hôpitaux des grands centres vs régions éloignées(Québec:RTI=2,06, valeur-p=0,0001; Montréal:RTI=1,38, valeur-p=0,005); héberger < 100% des patients symptomatiques d’infection à C. difficile en chambre privée vs 100%(80%-99%: RTI=1,33, valeur-p=0,01; < 80%:RTI=1,84, valeur-p< 0,0001); désinfecter la salle de bain des patients non-infectés 2fois/jour vs 1fois/jour(RTI=1,52, valeur-p=0,02); avoir un plan d’action lors d’éclosion n’incluant pas la surveillance des antibiotiques vs avoir un plan incluant la surveillance(RTI=1,36, valeur-p=0,004). L’hébergement des patients symptomatiques en chambre privée est le seul facteur commun qui ressort dans les modèles spécifiques aux hôpitaux universitaires et non-universitaires. Conclusion: Nous avons identifié des facteurs associés à l’infection sur lesquels il est possible d’intervenir, tant au niveau de la configuration de l’hôpital que des mesures qui y sont appliquées. / Background: Nosocomial Clostridium difficile (C. difficile) infection is a major public health concern. Quebec’s C. difficile provincial surveillance identified risk factors of the infection, such as teaching vocation and number of beds, which are unmodifiable. Thus these factors do not help targeting interventions to reduce the incidence of C. difficile infection. Objectives: This study aims to: 1)identify modifiable risk and/or protective factors associated with the incidence rate of C. difficile infection in Quebec hospitals; 2)evaluate if the risk and/or protective factors are the same according to hospital mission(teaching or non-teaching); 3)explain the association between teaching vocation and higher incidence rate of C. difficile infection. Method: Risk and/or protective factors were collected using a survey on preventive and control measures of C. difficile infection(INSPQ 2009-2010). The outcome is the incidence rate of the infection in Quebec hospitals(2009-2010). We used predictive multivariate Poisson models to answer the first two objectives and an explanatory model adjusted for various confounding factors to answer the third objective. Findings: Factors associated with a higher incidence rate in the multivariate predictive model for all hospitals were: hospitals in large urban centers vs remote regions(Quebec: IRR= 2.06, p-value=0.0001; Montreal: IRR=1.38, p-value=0.005); accommodate < 100% of symptomatic patients with C. difficile infection in private room vs 100%(80%-99%: IRR=1.33, p-value=0.01; < 80%: IRR=1.84, p-value< 0.0001); disinfect washroom of uninfected patients 2 times/day vs 1 time/day(IRR=1.52, p-value=0.02); have an action plan during an outbreak that doesn’t include antibiotic stewardship vs have an action plan during an outbreak that includes antibiotic stewardship(IRR=1.36, p-value=0.004). Accommodation of all symptomatic patients with C. difficile infection in private rooms is the only common risk factor between the models for teaching and non-teaching hospitals. Conclusion: We identified factors associated to the infection on which it is possible to act, whether it is on hospital setting or measures applied in hospitals.
126

Smitteverntiltak ved Clostridium difficileinfeksjon. : En kvantitativ tverrsnittsstudie blant helsepersonell i et norsk sykehus / Infection control measures for Clostridium difficile : a retrospective cross-sectional survey among healthcare professionals in a Norwegian hospit

Ørnevik, Grethe January 2014 (has links)
Bakgrunn: Clostridium difficile(CD)er antatt å være den utløsende årsak for 20-30 % av tilfeller med antibiotikaassosiert diaré. CD er den vanligste formen for helsetjenesteervervet diaré, og forår-saker økt sykelighet og dødelighet, samt økte kostnader for helsetjenesten. Desiste tiår er det rappor-tert om endringeri epidemiologien, forårsaket av en ny CD stamme, ribotype 027. Den spres lettere, lager mer alvorlig sykdom og tilbakefall. I Norge har denne stammen til nå ikke vært noe problem. Forekomsten kan reduseres ved en tydelig antibiotikapolitikk, og etterlevelse av anbefalte smitte-verntiltakfor å forebygge CD. Hensikt: Finne ut hvilke smitteverntiltak helsepersonell i sykehuset velger ved håndtering av pasien-ter med CD, og hvor de henter kunnskap om slike smitteverntiltak fra. Metode: En retrospektiv tverrsnittsstudie med spørreskjema til helsepersonell ble gjennomførtvåren og høsten 2011 i Sørlandet sykehus HF (SSHF), sør i Norge. Resultat: 168 helsepersonell deltok i undersøkelsen, fordelt på 59 leger og 109 pleiere. Svarprosen-ten var 94. Antibiotikarestriksjoner sier 94 % av medisinerne og 38 % av kirurgene atde har i sine avdelinger(x²=10.756, p&lt;0.001). Stetoskop brukt i isolat med CD pasienter sier 25 % legerat de spritdesinfiserer og tar med, mens 6 % pleiere sier det samme (x²=22.273, p&lt;0.001). 73 % av leger og 64 % pleiere sier at de både desinfiserer og vasker hendene etter kontakt med CD pasient (x²=6.451, p=0.011). Pasientinformasjon om viktigheten av håndhygiene sier 8 % leger og 36 % pleiere at de alltid gir (p&lt;0.001). Desinfeksjonsmiddel til bruk etter en CD pasient, sier 48 % medi-sinske pleiere og 43 % kirurgiske pleiere at de velgerVirkon (feil). Infeksjonskontroll-programmet (IKP) som kunnskapskilde brukes av 14 % leger og 46 % pleiere, (p&lt;0.001). Kunnskap om smitte-verntiltak ved CD sier 63 % legerog 72 % pleiere at de får fra kolleger. Konklusjon: Helsepersonell har generell kunnskap om smitteverntiltak, men mangler spesifikk kunnskap om smitteverntiltak ved CD. For å møte utfordringen med nye mer spredningspotente CD stammer, må etterlevelsen av smitteverntiltak øke. IKPalene, synes ikke å være tilstrekkelig for å holde helsepersonelloppdatert. Den manglende spesifikke kunnskapen om smitteverntiltak ved CD kan utsette pasienter i sykehuset for smitterisiko / Background: Clostridium difficile(CD) causes 20 %–30 % of all nosocomial infectious diarrhea, resulting in significant morbidity and increasing healthcare costs. Good antibiotic stewardship reduc-es the incidence of CD, andcompliance with infection control measures limits its spread. In recent years, ribotype 027, a new strain of CD, caused several disease outbreaks. Ribotype 027 spreads more easily and increases disease severity and relapse. Thus far, ribotype 027 has caused few prob-lems in Norway. Objective: This thesis aimed to determine whether hospital-based healthcare professionals comply with recommended infection control measures for CD prevention and identify how they learn about such measures. Method: A retrospective cross-sectional survey and questionnaire was performed among healthcare professionals at Sørlandet Hospital, Norway,during the spring and fall of 2011. Results: Survey participants included 168 health professionals (59 physicians and 109 nurses). The response rate was 94 %. Medical doctors (94 %) and surgeons (38 %) said that their clinics impose antibiotic restrictions (x ² = 10.756, p&lt; 0.001). After contact with a CD patient, physicians and nurs-es (73 % and 64 %, respectively) said they disinfect and wash their hands (x ²= 6.451, p&lt; 0.011). Notably, only 8% of physicians and 36 % of nurses always give patients information about the im-portance of hand hygiene (p&lt; 0.001). Even 25 % of physicians and 6 % of nurses reported using ethanol (does not eliminated CD spores) to disinfect stethoscopes before leaving a CD isolation room (x ² = 22.273, p&lt; 0.001). Medical and surgical nurses (48 % and 43 %, respectively) incorrectly used Virkon as a disinfectant in the CD patient’s room. Physicians and nurses (63 % and 72 %, respective-ly) mainly obtain knowledge about infection control measures from colleagues, compared to physi-cians and nurses (14 % and 46 % , respectively) who gain such knowledge from the hospital’s infec-tion control program (p&lt; 0.001). Conclusion: Healthcare professionals have some knowledge about infection control measures, but lack knowledge specific to limiting the spread of CD. Increased compliance with infection control measures is crucial to meeting the challenge of new and more potent strainsof CD. Guidelines alone are likely insufficient to keep healthcare professionals up to date. The lack of specific knowledge about infection control measures for CD may expose hospitalized patients to CD infection / <p>ISBN 978-91-86739-69-0</p>
127

THE USE OF LACTOBACILLUS IN THE TREATMENT OF CLOSTRIDIUM DIFFICILE INFECTION IN HOSPITALIZED ADULT PATIENTS

Alhammad, Ali 29 April 2009 (has links)
Objective To describe the use of Lactobacillus by hospitalized patients and to examine its relationship with various Clostridium difficile infection (CDI) related outcomes. Methods The characteristics of Lactobacillus users and non-users and the initiation of Lactobacillus with respect to initiation of antibiotic therapy and CDI treatment were described using national hospital discharge database. The relationships between Lactobacillus use and post-CDI length of stay, mortality, switch of CDI therapy, and readmission were analyzed. Results Lactobacillus users and non-users were different in most characteristics. Metronidazole and fluoroquinolones were the most frequently used antibiotics by Lactobacillus users. They were mainly CDI cases, used multiple antibiotics, extremely ill, and started Lactobacillus five or more days after initiation of antibiotics or CDI treatment. Lactobacillus use was associated with increased length of stay and switching of CDI therapy. Conclusions The true association between Lactobacillus use and CDI remains unclear. This study provides foundation for future research.
128

Épidémiologie des infections à Clostridium difficile chez les patients hospitalisés dans un centre hospitalo-universitaire / Clostridium difficile infection in patients hospitalized in a large tertiary hospital

Khanafer, Nagham 23 September 2013 (has links)
Clostridium difficile est responsable de 15 à 25% des cas de diarrhées post-antibiotiques (ATB) et de plus de 95% des cas de colite pseudomembraneuse. Depuis 2003 et suite à l'émergence du clone 027, les ICD sont devenues plus fréquentes et plus sévères. Compte tenu des conséquences, il a été décidé d'explorer en détail et prospectivement cette maladie au Groupement Hospitalier Edouard Herriot L'inclusion des patients a débuté fin février 2011 et devrait s'arrêter fin février 2014. Dans une méta-analyse, nous avons montré que l'ICD communautaire est associée à l'exposition aux mêmes ATB qu'une ICD nosocomiale. Une analyse de la littérature, en utilisant la grille ORION comme outil, nous a permis de synthétiser les connaissances sur la prévention et le contrôle d'ICD en milieu hospitalier. Par la suite sur la base d'une étude rétrospective, le sexe, la CRP et l'exposition aux fluoroquinolones ont été identifiés comme associés à une ICD sévère chez les patients hospitalisés en réanimation. Entre 2011 et 2013, 430 patients ont été inclus dans notre cohorte. L'analyse des données de la prise en charge thérapeutique de 118 cas d'ICD a montré un niveau insuffisant de la connaissance des recommandations actuelles concernant le traitement de cette infection. L'analyse pronostique a montré un taux de mortalité de 19,5% dans les 30 jours qui suivent le diagnostic. L'ICD était indiquée comme une cause principale ou contributive de décès dans quinze cas (65,7% des décédés). Les analyses multivariées ont montré que les facteurs associés au décès sont différents entre les patients avec une ICD et les patients présentant une diarrhée non liée au Clostridium difficile / Clostridium difficile is responsible for almost all cases of pseudomembranous colitis and for 15%-25% of cases of post-antibiotic (ATB) diarrhea. Since 2003 and the emergence of 027 strain, CDI epidemiology is changing, with evidence of rising incidence and severity. In response to the alarming situation we decided to conduct a prospective study at Eduard Herriot Hospital to explore in details this infection. Patient’s inclusion has started in February 2011 and will end in February 2014. In a meta-analysis we found that the risk profiles for antimicrobial classes as risk factors for community-acquired CDI are similar to those described for nosocomial CDI. We used the ORION statement (Outbreak Reports and Intervention Studies Of Nosocomial infection) to synthesize knowledge of interventions to reduce and to control CDI in hospitals. Then in a retrospective study, we found that male gender, rising serum C-reactive protein level, and previous exposure to fluoroquinolones were independently associated with severe CDI in ICU. Between 2011 and 2013, 430 patients were included in our prospective cohort study. Data analysis of 118 cases of CDI showed an inefficient knowledge of current recommendations of CDI treatment. The crude mortality rate within 30 days after CDI diagnosis was 19.5%, with 15 deaths (65.7% of deceased patients) related to CDI. In a multivariate cox regression model, gender, serum albumin, antidiarrheal medications, cephalosporins, peritonitis and septic shock were independently associated with mortality in CDI patients. When diarrhea was not related to C. difficile, mortality was rather associated with cancer and high WBC level
129

Phäno- und genotypische Charakterisierung konsekutiver Isolate eines Patienten mit rezidivierenden Clostridium difficile-Infektionen / Pheno- and genotypic characterisation of consecutive isolates of a patient with recurrent Clostridium difficile infections

Sachsenheimer, Friederike Emilie 20 March 2019 (has links)
No description available.
130

Diarrhées nosocomiales post-antibiothérapie liées à Clostridium difficile en gériatrie à propos de 39 cas /

Jurchescu Marbot, Cristina Daniela. Beinis, Jean-Yves. January 2005 (has links) (PDF)
Thèse d'exercice : Médecine. Médecine générale : Paris 12 : 2005. / Titre provenant de l'écran-titre. Bibliogr. f. 119-131.

Page generated in 0.0579 seconds