11 |
Développement d’une nouvelle stratégie neuroprotectrice efficace et d’une méthode de quantification précoce non invasive des lésions de la matière blanche cérébrale immature sur un modèle animalPierre, Wyston Chadwick 08 1900 (has links)
Les grands prématurés sont particulièrement vulnérables aux lésions inflammatoires de la substance blanche (WMI) qui augmentent le risque de troubles cognitifs et neurodéveloppementaux à long terme dans cette population. L’utilisation de l’imagerie par résonance magnétique (IRM) dans cette population a permis une évaluation non invasive de la progression des WMI et une meilleure compréhension de la pathologie. Les WMI sont associées une activation de la microglie et des astrocytes et la production de facteurs pro-inflammatoires, dont l’interleukine 1 (IL-1).
En utilisant un modèle de WMI induite par injection intracérébrale de lipopolysaccharides (LPS), nous avons évalué dans un premier temps les changements de méthylation de l’ADN durant la phase aigüe (24 h) et la phase chronique (21 jours) de l’inflammation. Par la suite, nous avons déterminé la capacité de l’IRM multimodale de détecter la lésion et la réponse thérapeutique à un antagoniste du récepteur de l’IL-1. Finalement, par le biais d’un antagoniste et d’un modulateur allostérique du récepteur à l’IL-1, nous avons évalué in vitro le rôle de la signalisation IL-1 durant la phase aigüe de la modulation de l’activation de la microglie et des astrocytes par le LPS.
Nous avons démontré la présence d’une altération du méthylome cérébral dans divers mécanismes liés au neurodéveloppement et à la réponse immunitaire. De plus, l’application de l’IRM multimodale dans notre modèle a permis d’évaluer in vivo la lésion et le début de la réponse thérapeutique durant la phase aigüe (24 h) de l’inflammation. L’évaluation à l’IRM corrèle aux changements observés par immunomarquage post mortem. In vitro, le LPS induit une réponse mixte de la microglie et des astrocytes qui évoluent dans le temps vers une réponse pro-inflammatoire et neurotoxique. Bien que l’IL-1 est hautement exprimée par la microglie et les astrocytes, son inhibition a un effet limité sur la modulation de l’activation gliale dû à la multitude de voies activées par le LPS durant la phase aigüe de l’inflammation. / Very premature infants are particularly vulnerable to inflammatory white matter injury (WMI) which increases the risk of long-term cognitive and neurodevelopmental disorders in this population. The use of magnetic resonance imaging (MRI) in this population has allowed non-invasive assessment of the progression of WMI and a better understanding of the pathology. WMI is associated with activation of microglia and astrocytes and the production of pro-inflammatory mediators, including interleukin 1 (IL-1).
Using a model of inflammatory WMI induced by intracerebral injection of lipopolysaccharides (LPS), we first evaluated the changes in DNA methylation during the acute phase (24 h) and the chronic phase (21 days) of inflammation. We then determined the ability of multimodal MRI to detect the lesion and the therapeutic response to an IL-1 receptor antagonist. Finally, using an antagonist and an allosteric modulator of the IL-1 receptor, we evaluated in vitro the contribution of IL-1 signaling during the acute phase of the modulation of microglia and astrocytes activation by LPS.
We have shown the presence of persistent alteration DNA methylation profile in the brain that was associated with pathways involved in neurodevelopment and immune response. In addition, the application of multimodal MRI in our model made it possible to evaluate in vivo the lesion and the therapeutic response during the acute phase (24 h) of the inflammation. The changes at the MRI correlated to post-mortem evaluation by immunostaining. In vitro, LPS induce a mixed response of microglia and astrocytes which evolved over time toward a pro-inflammatory and neurotoxic phenotype. Although IL-1 is highly expressed by microglia and astrocytes, its inhibition has a limited effect on the modulation of glial activation due to the multitude of pathways activated by LPS during the acute phase of inflammation.
|
12 |
Pathways to Shortened Gestation among African American WomenGillespie, Shannon L. January 2015 (has links)
No description available.
|
13 |
Estudo da homeostase dos mediadores pró-inflamatórios e antiinflamatórios na sepse neonatal / A Study of the homeostasis of the pro-inflammatory and anti-inflammatory mediators in neonatal sepsisMarco Antonio Cianciarullo 02 July 2008 (has links)
Objetivos: Avaliar a utilidade dos mediadores pró-inflamatórios (TNF-alfa, IL-1 beta e IL-6), dos mediadores antiinflamatórios (IL-10 e IL-1Ra) e da Proteína C reativa (PCR) para o diagnóstico na sepse neonatal; verificar se os valores séricos isolados ou a relação entre IL-6 e IL-1Ra têm valor preditivo de gravidade, na evolução clínica da doença; determinar se a homeostase entre os mediadores pró-inflamatórios e antiinflamatórios e a PCR definem o prognóstico da doença. Casuística e métodos: Foram incluídos no estudo 31 recém-nascidos (RN) internados na UCINE ou no Hospital Universitário com diagnóstico de sepse, baseado em critérios clínicos e laboratoriais. Os RN com diagnóstico de sepse foram subdivididos em dois grupos de acordo com a evolução clínica: grupo sepse: os que tiveram boa evolução e grupo sepse grave, os que tiveram evolução complicada por choque séptico e/ou CIVD e/ou FMOS e/ou óbito. Além dos exames de rotina para sepse, forma mensurados nos dias 0, 3 e 7 de evolução a partir do diagnóstico, os níveis séricos de TNF-alfa, IL-1 beta, IL-6, IL-10 e IL-1Ra. Resultados: Na análise evolutiva geral, todos os mediadores inflamatórios apresentaram mensuração elevada no dia do diagnóstico (dia 0), com decréscimo dos valores no decorrer do tempo. Entre os mediadores pró-inflamatórios, a TNF-alfa, a IL-6 e a IL-1 beta se mostraram adequados para o diagnóstico, no entanto para o seguimento, a melhor foi a IL-6. Entre os mediadores antiinflamatórios a IL-10 seguiu os padrões dos mediadores próinflamatórios acompanhando a resolução do processo séptico, enquanto a IL-1Ra apresentou decréscimos até o 3º dia e permaneceu estável até o 7º dia caracterizando a perpetuação da ação antiinflamatória desta citocina. Quanto às relações entre mediadores pró-inflamatórios e antiinflamatórios (relação IL-6/IL-1Ra e IL-6/(IL-6 + IL-1Ra) observamos que a IL-6/IL-1Ra apresentou relação com a evolução do processo séptico, mostrando inicialmente predomínio da ação próinflamatória no dia 0 e antiinflamatória no dia 7. A PCR acompanhou de forma muito semelhante as curvas da TNF-alfa, L-6 e IL-10. Quando se subdividiu a casuística em grupos, sepse e sepse grave, observamos que os RN com sepse com boa evolução apresentaram níveis séricos médios de TNF-alfa, IL-1 beta e IL-10 próximos aos níveis mínimos detectáveis e estas citocinas nos RN com sepse grave. / Objectives - To evaluate the utility of the pro-inflammatory mediators (TNF-alfa, IL1-beta, and IL-6), the anti-inflammatory mediators (IL-10 and IL-1Ra) and C-Reactive Protein (CRP) for the diagnosis of neonatal sepsis; to verify whether the isolated seric values or the relation between IL-6 and IL-1Ra have predictive values for severity regarding the clinical outcome, and to ascertain if the homeostasis between the pro-inflammatory and anti-inflammatory mediators and CPR can define the prognosis of the disease. Patients and Methods - The study included 31 newborns (NB) admitted to the UCINE (External Neonatal Unit) or to Hospital Universitário (São Paulo University Hospital) with diagnosis of sepsis based upon clinical and laboratorial parameters. The NB with diagnosis of sepsis were further subdivided into 2 groups according to the clinical outcome: sepsis group: containing those NB who evolved to a positive outcome, and severe sepsis group, in turn composed of the NB with unsatisfactory outcomes due to complications caused by septic shock and/or DIVC and/or FMOS and/or death. On days 0, 3, and 7 following diagnosis the seric levels of TNF-alfa, IL-1 beta, IL-6, IL-10, and IL-1Ra were measured in addition to the routine sepsis workup. Results - The general follow-up analysis revealed that all the inflammatory mediators presented elevated levels at diagnosis (day 0) with a decrease of these values over time. Regarding the pro-inflammatory mediators, TNF-alfa, IL-6 and IL-1 beta were satisfactory for diagnosis, whereas IL-6 was more accurate for follow-up. In relation to the anti-inflammatory mediators, IL-10 revealed the same pattern of the pro-inflammatory mediators following the septic process resolution, whereas IL-1Ra gradually decreased until the 3rd day but hence remained stable until the 7th day, thus characterizing the continuity of the anti-inflammatory action of this cytokine. Concerning the inter-relation between the pro and anti-inflammatory mediators (IL-6/IL-1Ra relation and IL-6/(IL6+IL-1Ra)) we observed that the IL-6/IL-1Ra correlated with the septic process evolution with predominance of the proinflammatory action on day 0 and of the anti-inflammatory action on day 7. The CRP levels, we observed that in the sepsis group with satisfactory outcome on day 0 the seric values were higher than in the severe sepsis group, although on days 3 and 7 these values decreased more substantially, while in the sepsis group they increased on day 3 followed by a gradual decrease until day 7. Conclusions - The analyzed mediators were effective in the diagnosis of neonatal sepsis and also predictive of the degree of severity, mainly with regards to cytokines IL-6 and IL-1Ra. The homeostatic equilibrium/disequilibrium was correlated to the type of disease outcome: sepsis with no complications versus severe sepsis.
|
14 |
Estudo da homeostase dos mediadores pró-inflamatórios e antiinflamatórios na sepse neonatal / A Study of the homeostasis of the pro-inflammatory and anti-inflammatory mediators in neonatal sepsisCianciarullo, Marco Antonio 02 July 2008 (has links)
Objetivos: Avaliar a utilidade dos mediadores pró-inflamatórios (TNF-alfa, IL-1 beta e IL-6), dos mediadores antiinflamatórios (IL-10 e IL-1Ra) e da Proteína C reativa (PCR) para o diagnóstico na sepse neonatal; verificar se os valores séricos isolados ou a relação entre IL-6 e IL-1Ra têm valor preditivo de gravidade, na evolução clínica da doença; determinar se a homeostase entre os mediadores pró-inflamatórios e antiinflamatórios e a PCR definem o prognóstico da doença. Casuística e métodos: Foram incluídos no estudo 31 recém-nascidos (RN) internados na UCINE ou no Hospital Universitário com diagnóstico de sepse, baseado em critérios clínicos e laboratoriais. Os RN com diagnóstico de sepse foram subdivididos em dois grupos de acordo com a evolução clínica: grupo sepse: os que tiveram boa evolução e grupo sepse grave, os que tiveram evolução complicada por choque séptico e/ou CIVD e/ou FMOS e/ou óbito. Além dos exames de rotina para sepse, forma mensurados nos dias 0, 3 e 7 de evolução a partir do diagnóstico, os níveis séricos de TNF-alfa, IL-1 beta, IL-6, IL-10 e IL-1Ra. Resultados: Na análise evolutiva geral, todos os mediadores inflamatórios apresentaram mensuração elevada no dia do diagnóstico (dia 0), com decréscimo dos valores no decorrer do tempo. Entre os mediadores pró-inflamatórios, a TNF-alfa, a IL-6 e a IL-1 beta se mostraram adequados para o diagnóstico, no entanto para o seguimento, a melhor foi a IL-6. Entre os mediadores antiinflamatórios a IL-10 seguiu os padrões dos mediadores próinflamatórios acompanhando a resolução do processo séptico, enquanto a IL-1Ra apresentou decréscimos até o 3º dia e permaneceu estável até o 7º dia caracterizando a perpetuação da ação antiinflamatória desta citocina. Quanto às relações entre mediadores pró-inflamatórios e antiinflamatórios (relação IL-6/IL-1Ra e IL-6/(IL-6 + IL-1Ra) observamos que a IL-6/IL-1Ra apresentou relação com a evolução do processo séptico, mostrando inicialmente predomínio da ação próinflamatória no dia 0 e antiinflamatória no dia 7. A PCR acompanhou de forma muito semelhante as curvas da TNF-alfa, L-6 e IL-10. Quando se subdividiu a casuística em grupos, sepse e sepse grave, observamos que os RN com sepse com boa evolução apresentaram níveis séricos médios de TNF-alfa, IL-1 beta e IL-10 próximos aos níveis mínimos detectáveis e estas citocinas nos RN com sepse grave. / Objectives - To evaluate the utility of the pro-inflammatory mediators (TNF-alfa, IL1-beta, and IL-6), the anti-inflammatory mediators (IL-10 and IL-1Ra) and C-Reactive Protein (CRP) for the diagnosis of neonatal sepsis; to verify whether the isolated seric values or the relation between IL-6 and IL-1Ra have predictive values for severity regarding the clinical outcome, and to ascertain if the homeostasis between the pro-inflammatory and anti-inflammatory mediators and CPR can define the prognosis of the disease. Patients and Methods - The study included 31 newborns (NB) admitted to the UCINE (External Neonatal Unit) or to Hospital Universitário (São Paulo University Hospital) with diagnosis of sepsis based upon clinical and laboratorial parameters. The NB with diagnosis of sepsis were further subdivided into 2 groups according to the clinical outcome: sepsis group: containing those NB who evolved to a positive outcome, and severe sepsis group, in turn composed of the NB with unsatisfactory outcomes due to complications caused by septic shock and/or DIVC and/or FMOS and/or death. On days 0, 3, and 7 following diagnosis the seric levels of TNF-alfa, IL-1 beta, IL-6, IL-10, and IL-1Ra were measured in addition to the routine sepsis workup. Results - The general follow-up analysis revealed that all the inflammatory mediators presented elevated levels at diagnosis (day 0) with a decrease of these values over time. Regarding the pro-inflammatory mediators, TNF-alfa, IL-6 and IL-1 beta were satisfactory for diagnosis, whereas IL-6 was more accurate for follow-up. In relation to the anti-inflammatory mediators, IL-10 revealed the same pattern of the pro-inflammatory mediators following the septic process resolution, whereas IL-1Ra gradually decreased until the 3rd day but hence remained stable until the 7th day, thus characterizing the continuity of the anti-inflammatory action of this cytokine. Concerning the inter-relation between the pro and anti-inflammatory mediators (IL-6/IL-1Ra relation and IL-6/(IL6+IL-1Ra)) we observed that the IL-6/IL-1Ra correlated with the septic process evolution with predominance of the proinflammatory action on day 0 and of the anti-inflammatory action on day 7. The CRP levels, we observed that in the sepsis group with satisfactory outcome on day 0 the seric values were higher than in the severe sepsis group, although on days 3 and 7 these values decreased more substantially, while in the sepsis group they increased on day 3 followed by a gradual decrease until day 7. Conclusions - The analyzed mediators were effective in the diagnosis of neonatal sepsis and also predictive of the degree of severity, mainly with regards to cytokines IL-6 and IL-1Ra. The homeostatic equilibrium/disequilibrium was correlated to the type of disease outcome: sepsis with no complications versus severe sepsis.
|
15 |
Der Einfluss von Interleukin-1 und des Interleukin-1-Rezeptorantagonisten (Anakinra) auf die epithelial-mesenchymale Transition von Tubulusepithelzellen in vitro / The effect of interleukin-1 and interleukin-1-receptor antagonist (Anakinra) on epithelial-mesenchymal transition of tubular epithelial cells in vitroTakes, Julia 26 October 2011 (has links)
No description available.
|
16 |
Promote neuroprotection and axonal outgrowth in the central and peripheral neural system / Främja neuroprotection och axonal utväxt i det centrala och perifera nervsystemetPetersson, Elin January 2021 (has links)
Acute spinal cord injury is often caused by collisions with motor vehicles, falls or violence. This injury could potentially lead to paraplegia or tetraplegia, causing great economic and personal loss. The patophysiology is biphasic, with primary and secondary mechanisms. Regarding secondary spinal cord injury, glutamate and interleukin-1 beta (IL-1<img src="http://www.diva-portal.org/cgi-bin/mimetex.cgi?%5Cbeta" data-classname="equation" data-title="" />) activates N-methyl-d-aspartate (NMDA)-receptors leading to prolonged excitotoxity, causing neuronal death and subsequently glial scarring. Cross-linked-hyaluronic acid gel and interleukin-1 receptor antagonist (IL-1RA) are believed to have a neuroprotective effect. The major aim of this study was to evaluate neuroprotection in the central neural system. Briefly, spinal cord slice cultures from mice (p9-12) were chemically injured with NMDA and treated with two hyaluronic acid-based gels with integrated, or added, IL1RA. RNA was extracted and transcripted to cDNA. The gene expression of Neuronal nuclear protein, <img src="http://www.diva-portal.org/cgi-bin/mimetex.cgi?%5Cbeta" data-classname="equation" data-title="" />-aktin and IL-1<img src="http://www.diva-portal.org/cgi-bin/mimetex.cgi?%5Cbeta" data-classname="equation" data-title="" /> were studies with RT-qPCR. Results showed that gel integrated with IL1RA had significant therapeutic effect, resembling undamaged cultures. Furthermore, axonal outgrowth was investigated in dorsal root ganglion (DRG) in which two preparations of the method were evaluated. Results demonstrated that changing medium every other day was more preferred, compared to adding 20 µl medium every day. In conclusion, gels integrated with IL1RA have neuroprotective properties and in DRG preparations, medium should be changed every other day for optimal results.
|
Page generated in 0.1132 seconds