Academic literature on the topic 'Infections bactériennes et mycoses'
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Journal articles on the topic "Infections bactériennes et mycoses"
Heumann, D. "Cytokines et infections bactériennes." Revue Française d'Allergologie et d'Immunologie Clinique 36, no. 3 (May 1996): 315–18. http://dx.doi.org/10.1016/s0335-7457(96)80101-8.
Full textPerdikis, Konstantinos Cédric, Nicolas Goossens, and Sebastian Carballo. "Cirrhose hépatique et infections bactériennes." Revue Médicale Suisse 16, no. 711 (2020): 1965–69. http://dx.doi.org/10.53738/revmed.2020.16.711.1965.
Full textBertholom, Chantal. "Les infections bactériennes et parasitaires." Option/Bio 31, no. 625-626 (November 2020): 15–19. http://dx.doi.org/10.1016/s0992-5945(20)30263-4.
Full textBouhnik, Yoram. "Infections intestinales, virales et bactériennes." EMC - Traité de médecine AKOS 1, no. 1 (January 2006): 1–3. http://dx.doi.org/10.1016/s1634-6939(06)75380-7.
Full textSilvain, C., and C. Chagneau-Derrode. "Infections bactériennes et cirrhose alcoolique." EMC - Hépato-Gastroenterologie 2, no. 4 (October 2005): 307–18. http://dx.doi.org/10.1016/j.emchg.2005.07.003.
Full textSilvain, C., and C. Chagneau-Derrode. "Infections bactériennes et cirrhose alcoolique." EMC - Hépatologie 1, no. 1 (January 2006): 1–8. http://dx.doi.org/10.1016/s1155-1976(05)40366-6.
Full textAujard, Y. "Infections néonatales bactériennes, mycosiques et parasitaires." EMC - Pédiatrie - Maladies infectieuses 6, no. 2 (January 2011): 1–26. http://dx.doi.org/10.1016/s1637-5017(11)72485-1.
Full textMarpeau, L. "Infections bactériennes et menace d'accouchement prématuré." Médecine et Maladies Infectieuses 24 (November 1994): 1041–44. http://dx.doi.org/10.1016/s0399-077x(05)80214-8.
Full textKane, Yaghouba, and B. C. Diallo. "Données sur les pathologies du chamelon en Mauritanie." Revue d’élevage et de médecine vétérinaire des pays tropicaux 53, no. 2 (February 1, 2000): 161. http://dx.doi.org/10.19182/remvt.9744.
Full textMachet, L., L. Martin, and L. Vaillant. "Infections bactériennes cutanées superficielles folliculaires et non folliculaires." EMC - Dermatologie 3, no. 1 (January 2008): 1–8. http://dx.doi.org/10.1016/s0246-0319(08)41203-7.
Full textDissertations / Theses on the topic "Infections bactériennes et mycoses"
Messien, Patrick. "Les complications bactériennes et fongiques des 96 premières transplantations hépatiques à Bordeaux." Bordeaux 2, 1991. http://www.theses.fr/1991BOR23027.
Full textRouzé, Anahita. "Impact de l'infection par SARS-CoV-2 sur l'épidémiologie des infections respiratoires bactériennes et des aspergilloses pulmonaires invasives chez les patients de réanimation sous ventilation mécanique." Electronic Thesis or Diss., Université de Lille (2022-....), 2024. https://pepite-depot.univ-lille.fr/ToutIDP/EDBSL/2024/2024ULILS017.pdf.
Full textObjectives: The CoVAPid project aimed to study the impact of SARS-CoV-2 infection on the epidemiology of bacterial and fungal respiratory infections in critically ill patients requiring mechanical ventilation (MV). Three entities were analyzed: early bacterial pulmonary infections, bacterial ventilator-associated lower respiratory tract infections (VA-LRTI) including ventilator-associated pneumonia (VAP) and ventilator-associated tracheobronchitis (VAT), and invasive pulmonary aspergillosis (IPA). The main objectives were to compare the prevalence of early bacterial pulmonary infection between patients admitted for COVID-19 and influenza, to compare the incidence of VA-LRTI among patients admitted for COVID-19, influenza, or other reasons than viral pneumonia, to compare the prevalence of early bacterial pulmonary infection and the incidence of VA-LRTI between patients from the 1st and 2nd pandemic waves of COVID-19, to determine the impact of VAP on mortality in patients with COVID-19, to assess the effect of corticosteroid therapy on the incidence of VAP in patients with COVID-19, and to compare the incidence of IPA between patients with COVID-19 and influenza. Methods: This was a retrospective observational multicenter European cohort involving 36 centers. Adult patients under MV for more than 48 hours were consecutively included and divided into four groups according to their ICU admission cause: COVID-19 (1st and 2nd wave, influenza, and others. Results: A total of 2172 patients were included. The prevalence of bacterial pulmonary infections within 48 hours following intubation was significantly lower in COVID-19 patients (9.7%) compared to those admitted for influenza (33.6%, adjusted odds ratio (OR) 0.23, 95% confidence interval 0.16-0.33). The incidence of VA-LRTI was significantly higher in COVID-19 patients (50.5%) compared to those admitted for influenza (30.3%, adjusted sub-hazard ratio (sHR) 1.6 (1.26-2.04)) and those without viral infection (25.3%, sHR 1.7 (1.20-2.39)), with a significantly higher incidence of VAP in the COVID-19 group compared to the other two groups. The prevalence of early infection significantly increased between the 1st and 2nd wave (9.7 vs 14.9%, adjusted OR 1.52 (1.04-2.22)), as did the incidence of VAP (36 vs 44.8%; adjusted sHR 1.37 (1.12-1.66)). VAP was associated with a significant increase in 28-day mortality in COVID-19 patients (adjusted HR of 1.65 (1.11-2.46)), which was not observed in patients admitted for influenza and without viral infection. However, no significant difference in the heterogeneity of the association between VAP and mortality was observed among the three study groups. The relationship between corticosteroid exposure and the incidence of VAP was not statistically significant (p=0.082 for the overall effect), despite a varying risk of VAP over time since the initiation of treatment. Finally, the incidence of putative IPA (defined by the AspICU algorithm) was significantly lower in the COVID-19 group compared to the influenza group (2.5% vs 6%, cause-specific adjusted HR 3.29 (1.53-7.02)). Conclusion: The CoVAPid project highlighted a lower prevalence of early bacterial pulmonary infections in COVID-19 patients compared to those with influenza, with a significant increase between the 1st and 2nd pandemic wave. The incidence of VAP was higher in COVID-19 patients, compared to patients admitted for influenza or without viral infection at admission, and significantly increased between the 1st and 2nd wave. In COVID-19 patients, corticosteroid therapy had no significant effect on the incidence of VAP, and the occurrence of VAP was associated with a significant increase in 28-day mortality. The incidence of IPA was lower among patients with COVID-19 than those with influenza
Nivoix, Yasmine. "Infections fongiques invasives : épidémiologie et optimisation thérapeutique." Strasbourg, 2009. http://www.theses.fr/2009STRA2006.
Full textFourmaux, Éric. "Diagnostic et traitement des endophtalmies bactériennes post-opératoires." Bordeaux 2, 1995. http://www.theses.fr/1995BOR23032.
Full textMugabe, Clement, and Abdelwahab Omri. "La gentamicine sous la forme liposomale : aspects technologique et microbiologique." Acfas-Sudbury, 2005. https://zone.biblio.laurentian.ca/dspace/handle/10219/63.
Full textLo, Cheikh Ibrahima. "Répertoire des bactéries identifiées par Maldi-Tof en Afrique de l'Ouest." Thesis, Aix-Marseille, 2015. http://www.theses.fr/2015AIXM5051/document.
Full textThe Africa bacteria repertory is unfamiliar because the available tools in this region are not allowed its best knowledge. In fact, bacteria are most often identified using culture techniques on simple media and biochemical tests which enable the identification of some common characters. These methods do not facilitate an exhaustive knowledge of the bacterial repertory; consequently they have recently been revolutionized by the systematic use of MALDI-TOF mass spectrometry (MS).In our thesis we used two mass spectrometers, respectively, MALDI-TOF Vitek MS currently installed at Dakar (Senegal) and MALDI-TOF Microflex LT installed in Marseille (France). In addition we have also confirmed that MALDI-TOF is a powerful tool for identifying bacterial species rarely involved in human infectious diseases. Thus in adopting the MALDI-TOF as a first-line tool in bacterial identification before Gram staining or other techniques of phenotypic identifications based on chemical characteristics, we discovered seven new species of bacteria isolated for first time in humans. Microbial identification using MALDI-TOF MS is currently feasible in Africa. Its performance and effectiveness in routine diagnosis of clinical microbiology laboratories have been proven. It is necessary either to increase the installation of MALDI-TOF, or establishing a network around a shared MALDI-TOF platform between several structures located in the same area, especially in the underdeveloped countries of Africa amortization of investment costs of the device, because it allowed reducing the time of reporting results and indirectly facilitating better care for patients
Siddle, Katherine Joyce. "Régulation transcriptomique et génétique de la réponse des microARN aux infections (myco)bactériennes." Thesis, Paris 6, 2014. http://www.theses.fr/2014PA066330.
Full textMicroRNAs (miRNAs) are important epigenetic regulators of gene expression that play a key role in many biological processes, including the immune response. Although infection is accompanied by marked changes in the transcriptional profiles of host cells, little is known about the variability of host miRNA responses to infection. In this thesis, we aimed to define the extent and specificity of pathogen-induced miRNA transcriptional responses of host cells, and to characterise the genetic basis of miRNA variability upon infection, using the model of Mycobacterium tuberculosis (MTB) infection of human dendritic cells. To this end, we have combined ex vivo approaches with a range of high-throughput genomic techniques to profile miRNA responses to MTB at the population-level and to compare this response with other mycobacterial and non-mycobacterial infections. We show that miRNAs display marked changes in expression and in isomiR distribution upon infection that are highly consistent across diverse bacteria, demonstrating the presence of a strong core miRNA response to bacterial infection. Our results highlight the impact of infection on miRNA-mediated gene regulatory networks and show that the expression of 3% of miRNAs are controlled by proximate expression quantitative trait loci (eQTLs) and identify a number of candidate miRNAs that may play a role in variability in the immune response to infection. Together, these results provide the first assessment of the impact of genotype-environment interactions on the regulation of miRNA expression, as well as offering novel insights into the specificity of these miRNAs in the response to mycobacterial infections
Siddle, Katherine Joyce. "Régulation transcriptomique et génétique de la réponse des microARN aux infections (myco)bactériennes." Electronic Thesis or Diss., Paris 6, 2014. http://www.theses.fr/2014PA066330.
Full textMicroRNAs (miRNAs) are important epigenetic regulators of gene expression that play a key role in many biological processes, including the immune response. Although infection is accompanied by marked changes in the transcriptional profiles of host cells, little is known about the variability of host miRNA responses to infection. In this thesis, we aimed to define the extent and specificity of pathogen-induced miRNA transcriptional responses of host cells, and to characterise the genetic basis of miRNA variability upon infection, using the model of Mycobacterium tuberculosis (MTB) infection of human dendritic cells. To this end, we have combined ex vivo approaches with a range of high-throughput genomic techniques to profile miRNA responses to MTB at the population-level and to compare this response with other mycobacterial and non-mycobacterial infections. We show that miRNAs display marked changes in expression and in isomiR distribution upon infection that are highly consistent across diverse bacteria, demonstrating the presence of a strong core miRNA response to bacterial infection. Our results highlight the impact of infection on miRNA-mediated gene regulatory networks and show that the expression of 3% of miRNAs are controlled by proximate expression quantitative trait loci (eQTLs) and identify a number of candidate miRNAs that may play a role in variability in the immune response to infection. Together, these results provide the first assessment of the impact of genotype-environment interactions on the regulation of miRNA expression, as well as offering novel insights into the specificity of these miRNAs in the response to mycobacterial infections
Bergeau, Caroline Ballereau Françoise. "Place du voriconazole et de la caspofungine dans le traitement des infections fongiques invasives au CHU de Nantes." [S.l.] : [s.n.], 2005. http://theses.univ-nantes.fr/thesemed/PHbergeau.pdf.
Full textGriseri, Thibault. "Rôle immunorégulateur des lymphocytes TNK dans le diabète de type 1 et les infections virales." Paris 5, 2006. http://www.theses.fr/2006PA05N24S.
Full textInvariant natural killer T (iNKT) cells can prevent type 1 diabetes by impairing T cell responses to pancreatic β cells. As iNKT cells can also promote T cell responses to pathogens, and as viruses can trigger autoimmune diabetes, we investigated the effect of iNKT cells on virus-induced diabetes. Mice expressing the lymphochoriomeningitis virus (LCMV) nucleoprotein (NP) in their pancreatic β cells develop diabetes after LCMV infection. Here, we show that although iNKT cells promote systemic anti-LCMV CD8 T cell responses, theyn also completely abolish LCMV-induced diabetes. Locally in the pancreas, iNKT cells induced the production of large amount of antiviral cytokines inhibiting LCMV replication
Books on the topic "Infections bactériennes et mycoses"
Frottier, Jacques. Dictionnaire des maladies infectieuses: Infections bactériennes, virales, parasitaires et fongiques. Paris: Conseil international de la langue française, 2005.
Find full textSymposium on Topics in Mycology on Mycoses in AIDS Patients (1989 Paris, France). Mycoses in AIDS patients. New York: Plenum Press, 1990.
Find full textOrganisation mondiale de la santé. and Organisation des Nations Unies pour l'alimentation et l'agriculture., eds. Évaluation des risques pour Campylobacter spp. dans les poulets et pour Vibrio spp. dans les produits de la pêche: Rapport d'une consultation mixte FAO/OMS d'experts, Bangkok, Thaïlande, 5-9 août 2002. Rome: Organisation mondiale de la santé, 2003.
Find full textParasitoses et mycoses courantes de la peau et des phanère. Paris: Elsevier, 2003.
Find full text(Editor), Geert Cauwenbergh, Edouard Drouhet (Editor), Donald W.R. Mackenzie (Editor), Jan Van Cutsem (Editor), and Hugo Vanden Bossche (Editor), eds. Mycoses in AIDS Patients. Springer, 1990.
Find full textHarry, Merlin. Ámóxil: Meilleur Traitement Pour les Infections Bactériennes , l'Infection À H. Pylori et les Ulcères Duodénaux. Independently Published, 2019.
Find full textMichael, Hutton. Amoxicillin: TRAITEMENT SUPER ACTIF des INFECTIONS BACTÉRIENNES , l'infection à H. Pylori, les Infections des Voies Urinaires et les Ulcères Duodé. Independently Published, 2019.
Find full textmahlare, wilson. §lx Þills: Le Traitement Idéal Pour éliminer les Infections Bactériennes Telles Que la Pneumonie, la Bronchite, les Infections des Voies Urinaires et H. Pylori. Independently Published, 2019.
Find full textSmith, Chris. ANTIBIOTIC 500mg: La Solution Antibiotique Parfaite Pour éliminer les Infections Bactériennes Telles Que la Bronchite, la Pneumonie, les Infections des Voies Urinaires et H. Pylori. Independently Published, 2019.
Find full textColton, Max. Cèf∆lèx: La Solution Antibiotique Idéale Pour Éliminer les Infections Bactériennes Telles Que la Pneumonie, la Bronchite, les Infections des Voies Urinaires et H. Pylori. Independently Published, 2019.
Find full textBook chapters on the topic "Infections bactériennes et mycoses"
Caumes, Éric. "Infections bactériennes systémiques." In Manifestations dermatologiques des maladies infectieuses, métaboliques et toxiques, 1–8. Paris: Springer Paris, 2008. http://dx.doi.org/10.1007/978-2-287-48494-0_1.
Full textLavigne, Jean-Philippe, Jacques Jourdan, and Albert Sotto. "Autres infections bactériennes." In Manifestations dermatologiques des maladies infectieuses, métaboliques et toxiques, 78–87. Paris: Springer Paris, 2008. http://dx.doi.org/10.1007/978-2-287-48494-0_9.
Full textHausser-Hauw, Chantal. "Infections bactériennes." In Manuel d'EEG de l'adulte. Veille et sommeil, 217–20. Elsevier, 2007. http://dx.doi.org/10.1016/b978-2-294-07145-4.50049-0.
Full textButin, M. "Infections bactériennes secondaires." In Réanimation et Soins Intensifs en Néonatologie, 722–24. Elsevier, 2024. http://dx.doi.org/10.1016/b978-2-294-77019-7.00117-6.
Full textSilvain, C., and C. Chagneau-Derrode. "Infections bactériennes et cirrhose." In Réanimation hépatosplanchnique, 139–51. Elsevier, 2010. http://dx.doi.org/10.1016/b978-2-8101-0186-3.50009-6.
Full textBarrail-Tran, Aurélie. "Traitement des infections urinaires bactériennes." In Pharmacie Clinique et Thérapeutique, 791–800. Elsevier, 2018. http://dx.doi.org/10.1016/b978-2-294-75077-9.00043-8.
Full textRaignoux, Cécile, Robert Farinotti, Robert Farinotti, François Gimenez†, and Anne-Claude Crémieux. "Traitement des infections urinaires bactériennes." In Pharmacie clinique et thérapeutique, 959–69. Elsevier, 2008. http://dx.doi.org/10.1016/b978-2-294-06234-6.50046-6.
Full textArmoiry, Xavier, Xavier Dode, Gilles Aulagner, François Gimenez†, Bruno Crestani, and Sophie Raymond. "Traitement des infections respiratoires basses bactériennes." In Pharmacie clinique et thérapeutique, 971–80. Elsevier, 2008. http://dx.doi.org/10.1016/b978-2-294-06234-6.50047-8.
Full textBoyer-Grand, Anne, Anne Boyer-Grand, François Gimenez†, Joël Depondt, and Sophie Raymond. "Traitement des infections respiratoires hautes bactériennes." In Pharmacie clinique et thérapeutique, 981–92. Elsevier, 2008. http://dx.doi.org/10.1016/b978-2-294-06234-6.50048-x.
Full textAujard, Yannick. "Infections primitives systémiques et focales bactériennes : diagnostic, pronostic et traitement." In Infections néonatales, 65–80. Elsevier, 2015. http://dx.doi.org/10.1016/b978-2-294-74135-7.00007-3.
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