Global ETD Search

61	Mobilisering i akutskedet efter stroke : effekter på patientens funktionsnivå: en litteraturöversikt / Mobilisation in the acute stages after stroke : effects on the patient's functional outcome: a literature review Crantz, Karin, Sjöberg, Louise January 2020 (has links) Mobilisation in the acute stages of stroke is a complex subject where the nurse must considerseveral confounding variables. There is an insufficient state of evidence around when andhow the first mobilisation should occur after stroke, and there is often uncertainty in thedecision making. The aim was to describe how early mobilisation in the acute stages of stroke affects thepatient’s level of functioning. The method used was a general literature review with an integrated analysis. Results: 17 articles analysing the effect of early mobilisation on nursing-related outcomemeasures, published between 2015–2019, were included in the literature review. Sample,interventions and outcome measures varied between the different articles. Three of the articlesshowed results suggesting that early mobilisation could be negative for the patient’sfunctional outcome after stroke. Among the remaining articles there was an even distributionof positive effects of early mobilisation and results not showing any effect on functionaloutcome. The results of this literature review imply that early mobilisation to some extentmay contribute to improved basic functions as in managing the toilet, dressing and also moreinstrumental features as cooking and driving. Early mobilisation appears to be a safe nursingintervention in most cases, as long as the patient is considered medically stable. The conclusion to be drawn from this literature review is that nurses, through their mainresponsibility for nursing care can influence the patient’s functional outcome through the decisions made regarding the first mobilisation in patients hit by acute stroke. / Mobilisering i akutskedet efter stroke är ett komplext ämne där sjuksköterskan måste ta ställning till ett flertal samverkande faktorer. Evidensläget kring när och hur den första mobiliseringen bör ske efter stroke är otillräckligt, och ofta uppstår en osäkerhet i beslutsfattandet. Syftet var att beskriva hur tidig mobilisering i akutskedet efter stroke påverkar patientens funktionsnivå. Metoden som användes var en allmän litteraturöversikt med integrerad analys. Resultat: 17 artiklar som analyserat effekten av tidig mobilisering på omvårdnadsrelaterade utfallsmått, publicerade från 2015–2019, inkluderades i litteraturöversikten. Urval, interventioner och utfallsmått varierade mellan de olika artiklarna. Tre av artiklarna visade på resultat som talar för att tidig mobilisering skulle kunna vara negativt för patientens funktionsutfall efter stroke. Bland övriga artiklar sågs en jämn fördelning bland positiv effekt av tidig mobilisering och resultat som inte visat någon påverkan på funktionsutfallet. Resultatet i denna litteraturöversikt tyder på att tidig mobilisering i viss mån kan bidra till förbättrade basala funktioner såsom att klara av toalettbesök, på- och avklädning och även mer instrumentella funktioner som att laga mat och köra bil. Tidig mobilisering ter sig vara en säker omvårdnadsåtgärd i de flesta fall, så länge patienten bedöms som medicinskt stabil. Slutsatsen som kan dras av litteraturöversikten är att sjuksköterskan genom sitt huvudansvar för omvårdnad kan påverka patientens funktionsutfall genom de beslut som fattas kring den första mobiliseringen av patienter som drabbats av akut stroke. Ytterligare forskning avseende tidpunkt och mobiliseringens intensitet behövs för att kunna avgöra när och hur den första mobiliseringen skall påbörjas efter att en patient drabbats av stroke. Acute ischemic stroke Early mobilisation Functional outcome Intracerebral hematoma Level of functioning Akut ischemisk stroke Funktionsnivå Funktionsutfall Intracerebralt hematom Tidig mobilisering Nursing Omvårdnad
62	Avaliação da autorregulação cerebral dinâmica através da reatividade cerebrovascular em suíno com volume expansivo por balão simulando aumento de hematoma intracerebral / Evaluation of dynamic cerebral autoregulation through cerebrovascular reactivity in a swine model with expansive volume of a balloon simulating an increase of a intracerebral hematoma Patriota, Gustavo Cartaxo 15 September 2017 (has links) INTRODUÇÃO: A autorregulação cerebral representa um dos mecanismos fisiopatológicos incertos na hemorragia intracerebral espontânea, cujo comprometimento pode influenciar no resultado prognóstico e terapêutico. O objetivo deste trabalho é avaliar a autorregulação cerebral dinâmica em modelo suíno de hemorragia intracerebral espontânea através do índice de reatividade pressórica cerebrovascular e determinar a eficácia das intervenções clínicas e cirúrgicas. MÉTODOS: Foram estudados 21 suínos híbridos machos com idade de 3 meses. O modelo experimental simulou o efeito expansivo de uma hemorragia intracerebral espontânea de grande volume quando comparado ao cérebro humano. Foram avaliados volumes de expansão diferentes, distribuídos em três grupos com sete suínos cada. O protocolo anestésico incluiu uma monitoração hemodinâmica invasiva associada a preservação da autorregulação cerebral. Os experimentos foram submetidos a monitoração neurológica multimodal e divididos em 5 fases. O índice de reatividade pressórica cerebrovascular estimou a autorregulacão cerebral durante todas as fases, sendo as três primeiras sem intervenções terapêuticas e as duas últimas para avaliar a eficácia das intervenções salina hipertônica e cirurgia. RESULTADOS: Os grupos avaliados foram homogêneos e sem diferença estatística quanto ao comprometimento da autorregulação cerebral comparando os diferentes volumes e tempos de compressão durante as duas primeiras horas da expansão do volume intracraniano. O comprometimento do índice de reatividade pressórica cerebrovascular ocorreu em alguns experimentos influenciando nas fases de tratamento subsequentes, salina hipertônica e cirurgia. CONCLUSÕES: Volumes expansivos elevados podem comprometer a autorregulação cerebral dinâmica e apresentar desfecho terapêutico desfavorável. A intervenção clínica e cirúrgica tem benefício nos experimentos com preservação do índice de reatividade pressórica cerebrovascular / INTRODUCTION: Cerebral autoregulation represents one of the uncertain pathophysiological mechanisms in spontaneous intracerebral hemorrhage, whose impairment may influence prognostic and therapeutic outcome. The aim of this study was to evaluate the dynamic cerebral autoregulation in the swine model of spontaneous intracerebral hemorrhage through the cerebrovascular reactivity index and to determine the efficacy of clinical and surgical interventions. METHODS: Twenty-one male hybrid pigs aged 3 months were studied. The experimental model simulated the expansive effect of a large intracerebral hemorrhage when compared to the human brain. Different volumes were evaluated, distributed in three groups with seven pigs each. Each experiment was divided in five phases. The anesthetic protocol included invasive hemodynamic monitoring associated with the preservation of cerebral autoregulation. Multimodallity monitoring was realised in all experiments. The cerebrovascular reactivity index estimated the cerebral autoregulation during all phases. The first three phases were without therapeutic interventions, and the last two phases were with therapeutic intervention of hypertonic saline solution and neurosurgery respectively. RESULTS: The evaluated groups were homogeneous and without statistical difference regarding the impairment of the cerebral autoregulation comparing different volumes and compression times during the first two hours of the intracranial volume expansion. CONCLUSIONS: Elevated expansive volumes may compromise dynamic cerebral autoregulation and have unfavorable therapeutic outcome. Clinical and surgical intervention had benefit in the experiments with preservation of cerebrovascular reactivity index Autorregulação cerebral Hemorragia intracerebral espontânea Hipertensão intracraniana Intracranial hypertension Monitoração multimodal Neurocirurgia Neurosurgical procedures Reatividade cerebrovascular Solução salina hipertônica Spontaneous intracranial hemorrhage
63	Nichtinvasive Magnetresonanz-Perfusionsmessung des Gehirns mittelsMagnetischer Blutbolusmarkierung(Spin-Labeling) Warmuth, Carsten 20 June 2003 (has links) Die magnetische Blutbolusmarkierung (Spin-Labeling) ermöglicht die nichtinvasive quantitative Messung des Blutflusses im Gewebe. Beim Spin-Labeling wird arterielles Blut durch Radiofrequenzpulse magnetisch markiert und der Transport der Markierung MR-tomographisch gemessen. Am Modell einer unter physiologischen Bedingungen perfundierten extrakorporalen Schweineniere konnte die Quantifizierbarkeit der Messmethode nachgewiesen werden. In einer Studie an 36 Hirntumorpatienten wurde das Verfahren mit der kontrastmittelbasierten First-Pass-Bolus-Methode zur nicht-quantitativen Perfusionsmessung verglichen. Es zeigte sich eine sehr gute Übereinstimmung zwischen beiden Methoden, der lineare Korrelationskoeffizient des relativen Blutflusses in der Tumorregion lag bei R=0,83. Die mittels Spin-Labeling ermittelten Absolutwerte des Blutflusses spielen bei der Beurteilung des Tumorgrades eine untergeordnete Rolle, da die mittlere Perfusion individuell sehr verschieden ist. Ein zweiter Anwendungsbereich für das Spin-Labeling ist die Darstellung großer Arterien. Spin-Labeling ermöglicht die nichtinvasive dynamische Angiographie (Dynamische Spin-Labeling-Angiographie - DSLA). Analog zur digitalen Subtraktionsangiographie kann damit der Einstromvorgang des Blutes in den Gefäßbaum zeitaufgelöst gemessen werden, jedoch mit wesentlich höherer zeitlicher Auflösung und frei wählbarer Projektionsrichtung. In einer Studie an 18 Patienten mit einseitigen Carotisstenosen wurden die Zeitdifferenzen der Anflutung der zerebralen Gefäße zwischen der betroffenen und der nicht stenosierten Seite bestimmt. Die im Carotis-Siphon gemessenen Zeitdifferenzen korrelieren signifikant mit dem Stenosegrad, steigen aber erst ab einer Lumeneinengung oberhalb von 80 Prozent deutlich an. Im Vergleich zu den etablierten Methoden werden die Möglichkeiten und Grenzen der DSLA dargestellt. / Arterial spin labeling methods allow to determine quantitative tissue blood flow values noninvasively. Arterial blood is labelled by an inversion pulse and the distribution of this intrinsic tracer is measured using magnetic resonance imaging. Experiments using an extra corporal in-vitro porcine kidney in a MR compatible set-up were carried out to determine the accuracy of blood flow values calculated from arterial spin labeling measurements. In a study of 36 brain tumor patients, spin labeling was compared to non-quantitative contrast-enhanced dynamic susceptibility-weighted perfusion imaging. Relative blood flow values determined with both methods were in good agreement, the linear regression coefficient in the tumor region was R=0.83. Due to the variable individual perfusion state, quantitative blood flow values determined using spin labeling play a minor role in the assessment of tumor grade. Application of spin labeling to angiography of major arteries was investigated. Dynamic spin labeling angiography (DSLA) sequences were implemented and tested on a clinical scanner. This technique allows time-resolved depiction of blood flow in large vessels with very high temporal resolution. As opposed to digital subtraction angiography, the method allows arbitrary projection directions. In a study, 18 patients with one-sided carotid stenoses were examined. In these patients the time differences of blood bolus arrival at both hemispheres were determined. Time differences measured in the carotid siphon show a significant correlation with the degree of stenosis. However, a clear increase is not seen until 80% narrowing of a carotid. Possibilities and limitations of the DSLA method are discussed in comparison to established techniques. Hirntumoren arterielles Spin-Labeling Perfusionmessung dynamische MR-Angiographie Carotisstenosen intrazerebrale Kollateralisierung brain tumors arterial spin labeling perfusion measurement dynamic MR-angiography carotid artery stenosis intracerebral collateralization 610 Medizin 33 Medizin XG 2100 XD 3200 XH 8550 YR 2500 ddc:610
64	Développement d’un modèle in vitro de Barrière Hémato-Encéphalique humaine pour des études pharmacologiques : Interactions avec les anticoagulants oraux directs / Development of an in vitro model of a human Blood Brain Barrier for pharmacological studies : Interactions with directs oral anticoagulants Puech, Clémentine 13 December 2018 (has links) La barrière hémato-encéphalique (BHE) contrôle le passage des médicaments, en partie par la présence d’ATP Binding Cassette (ABC) transporteurs. Dans de nombreuses pathologies cérébrales, la BHE est altérée. Parmi elles, les hémorragies intracérébrales (HIC), qui sont un effet iatrogène des anticoagulants. Des analyses cliniques montrent que les patients sous Anticoagulants Oraux Directs (AODs) présentent moins d’HIC que les patients traités avec les anticoagulants de référence, les anti-vitamine K (AVK), sans que les mécanismes cellulaires soient élucidés. Une des différences entre les AODs et les AVK résident dans leur profil pharmacocinétique, effectivement, les AODs sont des substrats des ABC transporteurs contrairement aux AVKs. Au cours des HIC, la thrombine est activée et entraine une altération de la BHE par clivage et des récepteurs protease activated receptor (PAR). Les objectifs de ce travail de thèse ont été de mettre en place un modèle in vitro de BHE afin d’étudier les interactions des médicaments avec les ABC transporteurs. Ensuite, le modèle est utilisé pour étudier les interactions des AODs en condition pathologique. Le modèle développé est basé sur la lignée HBEC-5i, peu décrite dans la littérature. Les cellules ont été cultivées en monocouche sur insert avec milieu conditionné issu d’astrocytes humains. Le modèle permet l’étude de l’interaction de thérapeutiques avec des ABC transporteurs par des mesures d’efflux ratios. Le modèle a été validé par des études de transport de molécules pharmacologiques. Ensuite, nous avons comparé, sur notre modèle, les effets de l’exposition à la thrombine avec ou sans prétraitement d’anticoagulants (rivaroxaban, dabigatran, apixaban, warfarine et héparine). Les AODs limitent l’ouverture de la BHE induite par la thrombine contrairement aux autres anticoagulants. Nos résultats ont montré que l’altération de la BHE est médiée par le clivage du récepteur PAR-1 par la thrombine. Ce clivage n’est pas le même en fonction de la classe d’anticoagulants utilisée, les AODs minimisant ce clivage. L’ensemble de ce travail de thèse a permis de donner des premières explications cellulaires quant aux mécanismes d’ouverture de la BHE consécutifs aux HIC sous AODs. / The blood-brain barrier (BBB) controls the passage of drugs, in part through the expression of the ATP Binding Cassette (ABC) transporters. In many brain diseases, the BBB is altered. Among them, intracerebral haemorrhages (ICH), which are an iatrogenic effect of anticoagulants. Clinical analyses show that patients with Direct Oral Anticoagulants (DOACs) treatment have less HIC than patients treated with the reference anticoagulants, Vitamin K Antagonist (VKA), without understanding the cellular mechanisms. One of the differences between DOACs and VKA lies in their pharmacokinetic profile, indeed, DOACs are substrates of ABC transporters unlike VKA. During HIC, thrombin, is activated and causes alterations in the BBB by the cleavage of the protease activated receptor (PAR). The objectives of this thesis work were first to set up an in vitro model of the BBB in order to study the passage of drugs and their interactions with ABC transporters. In a second step, the model is used to study the interactions of DOACs in pathological conditions. The model developed is based on the HBEC-5i cell line seldom described in the literature. The cells were cultured in monolayer on insert with conditioned medium from human astrocytes. It allows the study of the interaction of therapeutics with ABC transporters by measuring efflux ratios. The model has been validated by transport studies of pharmacological molecules. In order to meet our second objective, we compared the effect of thrombin exposure with or without pretreatment with anticoagulants (rivaroxaban, dabigatran, apixaban, warfarin and heparin sodium) on our model. DOACs limit the BBB damage induced by the thrombin unlike other anticoagulants. Our results showed that alteration of the BBB is mediated by the cleavage of the PAR-1 receptor by thrombin. This cleavage is not the same depending on the class of anticoagulants used, DOACs minimizing this cleavage. All this thesis work made it possible to provide the first cellular explanations of the opening mechanisms of the BBB following HIC under DOACs. Barrière hémato-encéphalique ABC transporteurs Anticoagulants oraux directs Protease activated receptor-1 Hémorragies intracérébrales Modèle in vitro Blood-brain barrier ABC transporters Direct Oral Anticoagulants Protease activated receptor-1 Intracerebral haemorrhages In vitro model
65	Interferindo com oscila??es de alta frequ?ncia no hipocampo epil?ptico: consequ?ncias para as crises espont?neas Farias, Kelly Soares 21 September 2012 (has links) Made available in DSpace on 2014-12-17T15:28:52Z (GMT). No. of bitstreams: 1 KellySF_DISSERT.pdf: 3939064 bytes, checksum: 5be69492fa857ba043776a01195d92b4 (MD5) Previous issue date: 2012-09-21 / Conselho Nacional de Desenvolvimento Cient?fico e Tecnol?gico / Crises epil?pticas s?o eventos parox?sticos do sistema nervoso central (SNC) caracterizadas por uma descarga el?trica neuronal anormal, com ou sem perda de consci?ncia e com sintomas cl?nicos variados. Nas epilepsias do lobo temporal as crises tem in?cio focal, em estruturas do sistema l?mbico. Dados cl?nicos e experimentais mostram que essas regi?es apresentam morte neuronal (esclerose hipocampal), reorganiza??o sin?ptica (brotamento aberrante das fibras musgosas) e gliose reativa, sendo esses marcadores biol?gicos da zona epileptog?nica. Registros extracelulares mostram que al?m das altera??es anat?micas mencionadas acima, a zona epileptog?nica tamb?m apresenta oscila??es de alta frequ?ncia patol?gicas (pOAF). As pOAF s?o oscila??es transientes (50 100 ms de dura??o), de baixa amplitude (200 μV - 1.5 mV) e de frequ?ncias vari?veis (80 800 Hz). A rela??o entre essas oscila??es e a g?nese das crises espont?neas ainda ? desconhecida. O objetivo do presente trabalho foi avaliar os efeitos da estimula??o el?trica intracerebral (EIC) nas pOAF e frequ?ncia de crises espont?neas de animais cronicamente epil?pticos (modelo da epilepsia do lobo temporal). Atualmente, a EIC ? utilizada no tratamento de dist?rbios do movimento (e.g., doen?a de Parkinson) e em alguns casos de dor cr?nica, e experimentalmente, no tratamento das epilepsias de dif?cil controle. A hip?tese de trabalho dessa disserta??o ? de que a indu??o de depress?o de longa dura??o por EIC, ao reduzir a excitabilidade neuronal local, modular? as pOAF, bem como a frequ?ncia de crises espont?neas. Para isso, comparamos as caracter?sticas espectrais das pOAF e a frequ?ncia de crises espont?neas antes e depois de um protocolo de 12 horas de estimula??o el?trica de baixa frequ?ncia (0,2 Hz) aplicado na via perforante. De fato, esse protocolo reduziu a amplitude do potencial de a??o coletivo registrado no giro denteado (GD) do hipocampo dorsal em 45% (amplitude m?dia da primeira e da ?ltima hora de estimula??o: 7,3 ? 3,0 mV e 4,1 ? 1,5 mV, respectivamente; p<0,05; teste t). O monitoramento cont?nuo do potencial de campo local, realizado no GD e em CA3 simultaneamente, mostrou que o protocolo de estimula??o empregado foi eficaz em (i) aumentar a dura??o (64,6 ? 9,3 ms vs. 70,5 ? 11,5 ms) e reduzir (ii) a entropia (3,72 ? 0,28 vs. 3,58 ? 0,30), (iii) o ?ndice pOAF (0,20 ? 0,08 vs. 0,15 ? 0,07) e (iv) o modo espectral (237,5 ? 15,8 Hz vs. 228,7 ? 15,2 Hz) das pOAF (valores do GD, expressos como m?dia ? desvio-padr?o, para os per?odos pr? e p?s estimula??o respectivamente; p<0,05; teste t). Ainda, este protocolo reduziu significativamente a frequ?ncia de crises espont?neas (1,8 ? 0,4 vs. 1,0 ? 0,3 crises/hora; pr? e p?s estimula??o, respectivamente; p<0,05; teste t). Curiosamente, observamos um aumento na dura??o m?dia das crises espont?neas ap?s o t?rmino do protocolo (39,7 ? 6,0 vs. 51,6 ? 12,5 s; pr? e p?s estimula??o respectivamente; p<0,05; teste t). Estes resultados sugerem que a redu??o da excitabilidade neuronal, por meio de protocolos de estimula??o el?trica, altera o perfil espectral das pOAF. Esse efeito foi acompanhado de redu??o na frequ?ncia de crises espont?neas. Apesar de preliminar, o presente trabalho contribui para o refinamento de terapias baseadas em EIC para indiv?duos com epilepsia
66	Avaliação da autorregulação cerebral dinâmica através da reatividade cerebrovascular em suíno com volume expansivo por balão simulando aumento de hematoma intracerebral / Evaluation of dynamic cerebral autoregulation through cerebrovascular reactivity in a swine model with expansive volume of a balloon simulating an increase of a intracerebral hematoma Gustavo Cartaxo Patriota 15 September 2017 (has links) INTRODUÇÃO: A autorregulação cerebral representa um dos mecanismos fisiopatológicos incertos na hemorragia intracerebral espontânea, cujo comprometimento pode influenciar no resultado prognóstico e terapêutico. O objetivo deste trabalho é avaliar a autorregulação cerebral dinâmica em modelo suíno de hemorragia intracerebral espontânea através do índice de reatividade pressórica cerebrovascular e determinar a eficácia das intervenções clínicas e cirúrgicas. MÉTODOS: Foram estudados 21 suínos híbridos machos com idade de 3 meses. O modelo experimental simulou o efeito expansivo de uma hemorragia intracerebral espontânea de grande volume quando comparado ao cérebro humano. Foram avaliados volumes de expansão diferentes, distribuídos em três grupos com sete suínos cada. O protocolo anestésico incluiu uma monitoração hemodinâmica invasiva associada a preservação da autorregulação cerebral. Os experimentos foram submetidos a monitoração neurológica multimodal e divididos em 5 fases. O índice de reatividade pressórica cerebrovascular estimou a autorregulacão cerebral durante todas as fases, sendo as três primeiras sem intervenções terapêuticas e as duas últimas para avaliar a eficácia das intervenções salina hipertônica e cirurgia. RESULTADOS: Os grupos avaliados foram homogêneos e sem diferença estatística quanto ao comprometimento da autorregulação cerebral comparando os diferentes volumes e tempos de compressão durante as duas primeiras horas da expansão do volume intracraniano. O comprometimento do índice de reatividade pressórica cerebrovascular ocorreu em alguns experimentos influenciando nas fases de tratamento subsequentes, salina hipertônica e cirurgia. CONCLUSÕES: Volumes expansivos elevados podem comprometer a autorregulação cerebral dinâmica e apresentar desfecho terapêutico desfavorável. A intervenção clínica e cirúrgica tem benefício nos experimentos com preservação do índice de reatividade pressórica cerebrovascular / INTRODUCTION: Cerebral autoregulation represents one of the uncertain pathophysiological mechanisms in spontaneous intracerebral hemorrhage, whose impairment may influence prognostic and therapeutic outcome. The aim of this study was to evaluate the dynamic cerebral autoregulation in the swine model of spontaneous intracerebral hemorrhage through the cerebrovascular reactivity index and to determine the efficacy of clinical and surgical interventions. METHODS: Twenty-one male hybrid pigs aged 3 months were studied. The experimental model simulated the expansive effect of a large intracerebral hemorrhage when compared to the human brain. Different volumes were evaluated, distributed in three groups with seven pigs each. Each experiment was divided in five phases. The anesthetic protocol included invasive hemodynamic monitoring associated with the preservation of cerebral autoregulation. Multimodallity monitoring was realised in all experiments. The cerebrovascular reactivity index estimated the cerebral autoregulation during all phases. The first three phases were without therapeutic interventions, and the last two phases were with therapeutic intervention of hypertonic saline solution and neurosurgery respectively. RESULTS: The evaluated groups were homogeneous and without statistical difference regarding the impairment of the cerebral autoregulation comparing different volumes and compression times during the first two hours of the intracranial volume expansion. CONCLUSIONS: Elevated expansive volumes may compromise dynamic cerebral autoregulation and have unfavorable therapeutic outcome. Clinical and surgical intervention had benefit in the experiments with preservation of cerebrovascular reactivity index Autorregulação cerebral Hemorragia intracerebral espontânea Hipertensão intracraniana Monitoração multimodal Neurocirurgia Reatividade cerebrovascular Solução salina hipertônica Intracranial hypertension Neurosurgical procedures Spontaneous intracranial hemorrhage
67	Suivi du métabolisme énergétique cérébral chez les patients victimes d'hémorragies sous-arachnoïdiennes graves : intérêt pour le pronostic individuel et le diagnostic des complications ischémiques / Monitoring of cerebral energy metabolism in patients experiencing severe subarachnoid hemorrhage : interest for the individual prognosis and for the diagnosis of ischemic complications Tholance, Yannick 16 October 2014 (has links) L'intérêt du suivi du métabolisme énergétique cérébral dans la prise en charge des patients victimes d'hémorragie sous-arachnoïdienne anévrismale (aSAH) grave reste actuellement controversé en raison de l'absence de valeurs seuils décisionnelles applicables en pratique. Ce travail avait pour objectif de réévaluer l'intérêt des paramètres biochimiques de trois techniques, la microdialyse intracérébrale (cMD), la mesure de la pression tissulaire cérébrale en oxygène (PbtO2) et le cathéter rétrograde jugulaire, pour prédire l’issue fonctionnelle de ces patients et diagnostiquer la survenue d'un infarctus. Il parait évident que ce suivi peut permettre de prédire à l'échelon individuel l'issue fonctionnelle à long terme. Le metabolic ratio (MR) ou l'association de ce MR avec des paramètres des deux autres techniques (ratio Lactate/Pyruvate >40, lactates hypoxiques) représentent des potentiels biomarqueurs pronostiques. Il est en revanche difficile de conclure sur l'intérêt de ce suivi pour diagnostiquer les complications ischémiques secondaires. Bien qu'il ait été montré que le MR peut être considéré comme un biomarqueur, il n'est pas possible de conclure actuellement sur les deux approches locales (cMD et PbtO2). Des règles d'implantation ont tout de même pu être identifiées et validées permettant leur application rapide en pratique courante. Au final, le suivi du métabolisme énergétique cérébral doit être envisagé dans la prise en charge des patients aSAH graves notamment pour prédire l'issue fonctionnelle à long terme car des valeurs seuils décisionnelles ont été identifiées et faciliteront ainsi l'utilisation de ce type de monitoring / The interest of cerebral energy metabolism monitoring in the care of patients suffering from aneurysmal subarachnoid hemorrhage (aSAH) currently remains controversial because of the absence of decision making thresholds applicable in practice. This work aimed to reassess the value of biochemical parameters from three techniques, intracerebral microdialysis (cMD), the measurement of brain tissue oxygen pressure (PbtO2), the retrograde jugular catheter to predict the functional outcome and diagnose the occurrence of secondary ischemia.It seems obvious that this monitoring can predict at the individual level the functional long-term outcome. The metabolic ratio (MR) or association of MR with the parameters of the two other techniques (lactate/pyruvate >40, hypoxic lactate) represent potential prognostic biomarkers.It is however difficult to conclude on the interest of such monitoring to diagnose secondary ischemic complications. Although it has been shown that the MR can be considered as a biomarker, it is currently not possible to conclude on the two local approaches (cMD and PbtO2). Nevertheless, implantation rules have been identified and validated for their rapid application in clinical practice.Finally, the monitoring of brain energy metabolism remains a reference technique in the care of serious aSAH patients, especially to predict functional long-term outcome because decision thresholds have been identified and thus will facilitate the use of this kind of monitoring Métabolisme énergétique cérébral Hémorragie sous-arachnoïdienne Issue fonctionnelle Microdialyse intracérébrale Lactate Glucose Cerebral energy metabolism Subarachnoid hemorrhage Functional outcome Intracerebral microdialysis Retrograde jugular catheter Lactates Glucose 612.8
68	Valeur pronostique du « monitoring » du métabolisme énergétique cérébral chez les patients victimes d’une hémorragie sous-arachnoïdienne grave / Pronostic value of the cerebral energetic metabolism monitoring in poor grade subarachnoid hemorrhage patients Keli Barcelos, Gleicy 21 December 2012 (has links) Le ratio métabolique (MR) est un marqueur du métabolisme cérébral. Dans notre travail, nous avons démontré sa valeur pronostique chez 68 patients victimes d’une hémorragie sous-arachnoïdienne anévrysmale grave. En effet, une diminution du MR sous le seuil de 3,35 traduit un phénomène d’hyperglycolyse relative, dont le nombre d’événement est prédictive d’un pronostic défavorable avec une excellente sensibilité et spécificité. L’obtention de ces résultats est rendue possible, notamment après une phase de validation dans un modèle animal de procédures permettant de limiter les effets de facteurs pré-analytiques critiques. Ces résultats permettent d’envisager une étude pour savoir si l’intégration de ce marqueur dans la stratégie de prise en charge du patient, permet de modifier son devenir fonctionnel. Après avoir validé analytiquement les mesures de pyruvate, glucose et lactate impliquant la technique de microdialyse, nous avons étudié sur une cohorte de patients graves aSAH, modeste (n=18 patients) s’il existait des phénomènes d’hyperglycolyse et leur corrélation avec le pronostic. Dans notre série, à la différence de l’approche globale (cathétérisme de la veine jugulaire), un phénomène d’hyperglycolyse conduirait vers un bon pronostic. En fait, l’approche par microdialyse donne une information sur le métabolisme énergétique localisé à l’implantation de la sonde, alors que le MR donne une information globale, ce qui est probablement le facteur le plus important expliquant la différence d’interprétation entre les 2 approches. En l’absence d’outils de traitement de données et d’algorithmes de décision clinique validés, la microdialyse ne donne pas à l’heure actuelle, une valeur individuelle diagnostique ou pronostique. Un des résultats très prometteurs de ce travail, est la mise en évidence d’un phénomène d’hyperglycolyse relative globale lors du vasospasme, rapidement réversible chez les patients ayant bien évolué, alors qu’il perdure de nombreuses heures après le vasospasme chez les patients ayant évolué de manière péjorative. Ces résultats nécessitent d’être reproduits sur un nombre plus significatifs de patients, ce qui permettrait une confirmation radiologique du vasospasme de manière plus précoce afin de confirmer son importance, sa localisation et l’éventualité de le traiter rapidement / The metabolic ratio (MR) is an index of the brain energetic metabolism. In our study, we have demonstrated its prognostic value for 68 poor grade patients aneurysmal subarachnoid hemorrhage (aSAH): a MR below the threshold value of 3.35 reflects a phenomenon of global cerebral hyperglycolysis which, if repeated, is predictive of a bad outcome. These results were made possible after validation step in an animal mode which allowed to control the critical pre-analytical factors. Our results pave the way for a clinical study aiming to determine if taking into account the MR will help to improve the functional outcome of the aSAH patients. In another approach, based on the use of cerebral microdialysis, we have studied, in an 18 patients cohort, and after an analytical validation of a new biochemical analysis, if such cerebral hyperglycolysis phenomenon was a encountered in this cohort, if these was a correlation with the patients’ outcome. In contrast with the previous 68 aSAH patients, this hyperglycolysis phenomenon appears linked to a good outcome. This apparent discrepancy may be due the difference in the anatomical giving a more localized information on the brain metabolism than the jugular approach used for the MR determination. The most interesting of our results is the correlation found between hyperglycolysis and cerebral vasospasm. If conformed with a larger cohort of aSAH patients, the use of MR could allow an earlier detection and treatment of cerebral vasospasm Hémorragie sous-arachnoïdienne Métabolisme énergétique cérébral Cathéter jugulaire rétrograde Microdialyse intracérébrale Ratio métabolique Lactate Glucose Pyruvate Subarachnoid hemorrhage Cerebral energetic metabolism Jugular catheter retrograde Intracerebral microdialysis Metabolic ratio Lactate Glucose Pyruvate 616.8
69	Identifying the Role of Cofilin Signaling in Hemorrhagic Brain Injury Almarghalani, Daniyah Abduljalil 11 July 2022 (has links) No description available. Neurobiology Neurosciences Aging Behavioral Sciences Molecular Biology Therapy Hemorrhagic brain injury Intracerebral hemorrhage (ICH) siRNA therapeutics Microglial activation, Neuroinflammation Post-stroke cognitive impairment (PSDT) Motor impairment Cofilin knockout Cofilin Knockdown
70	Effets motivationnels des cannabinoïdes dans un modèle animal de la schizophrénie Gallo, Alexandra 06 1900 (has links) Depuis quelques décennies, la consommation de cannabis et son usage thérapeutique sont le sujet de nombreux débats. Le cannabis est la drogue illicite la plus consommée au monde et cette consommation se trouve dix fois plus élevée chez les patients atteints de schizophrénie que dans la population générale. L’hypothèse d’une automédication initialement proposée afin d’expliquer la consommation élevée de cannabis chez les patients atteints de schizophrénie est maintenant remise en question. En effet, les rapports indiquant une aggravation des symptômes plutôt qu’une amélioration suite à une consommation à long terme sont de plus en plus nombreux. Sachant que le cannabis peut induire des effets soit plaisants soit aversifs, la question se pose à savoir si une prédominance de la valence motivationnelle positive ou une diminution de la valence négative du cannabis peut expliquer la consommation élevée parmi les individus ayant un diagnostic de schizophrénie? Bien qu’un grand nombre de recherches pré-cliniques aient été menées chez l’animal normal pour évaluer l’effet motivationnel du Δ9-tétrahydrocannabinol (THC) et autres cannabinoïdes synthétiques, aucune n’a abordé cette problématique dans un modèle animal de la schizophrénie. Cette lacune nous a donc amené à étudier la valence motivationnelle du THC et de l’agoniste cannabinoïde WIN55,212-2 (WIN) dans un modèle animal de la schizophrénie: la lésion néonatale de l’hippocampe ventral (NVHL). Dans le premier article, nous présentons les résultats de quatre expériences. Une première avait pour objectif de déterminer si la procédure expérimentale que nous avons utilisée permettait de reproduire des signes distinctifs du modèle animal de la schizophrénie. Par la suite, nous avons évalué i) l’effet d’une dose de WIN sur l’activité locomotrice spontanée et ii) la valence motivationnelle du THC (0.5 mg/kg, i.p) et du WIN (1 mg/kg, i.p) chez les rats adolescents (jour post-natal 28-40, PD28-40) et adultes (PD56) au moyen du paradigme de préférence de place conditionnée (PPC). Tel qu’attendu, la réponse locomotrice à l’amphétamine (0.75 et 1.5 mg/kg) chez les rats NVHL adultes était supérieure à celle des rats contrôles (test distinctif du modèle). Le THC a induit une tendance aversive chez les rats contrôles adultes. Enfin, le WIN a stimulé l’activité locomotrice et induit une aversion significative chez les rats adultes NVHL. Dans un deuxième article, nous avons évalué la valence motivationnelle du THC (0.5 mg/kg), du WIN (1 et 3 mg/kg) et l’effet de l’amphétamine au moyen du paradigme d’autostimulation électrique intracérébrale (ASI). Les résultats montrent que : i) l’effet amplificateur de l’amphétamine sur l’ASI était de plus courte durée chez les rats NVHL; ii) le THC produit une légère atténuation de la récompense chez les rats contrôles tandis que le WIN a produit une atténuation plus prononcée de la récompense chez les rats NVHL, un effet qui a été bloqué par l’antagoniste aux récepteurs CB1, le AM251 (3 mg/kg). Pour la première fois les résultats suggèrent une altération du système endocannabinoïde dans un modèle animal de la schizophrénie. Ils indiquent qu’une exposition aigüe conduit à une prédominance de la valence négative. Bien qu’en apparente contradiction avec les études cliniques, ces résultats soulignent l’importance du contexte socio-environnemental pour expliquer les effets du cannabis chez les patients. De plus ils encouragent les futures études à évaluer cette valence sur un modèle d’exposition chronique. / Over the past few decades, the cannabis consumption and its therapeutic use have been the subject of many debates. Cannabis is the most widely used illicit drug and among patients with a diagnosis of schizophrenia, its consumption is ten times higher than in the general population. The self-medication hypothesis that has been initially proposed to account for the co-morbidity schizophrenia – cannabis is now questioned on the basis of several reports showing that long term cannabis consumption worsen schizophrenia symptoms in patients. Knowing that cannabis can provoke both rewarding and aversive effects in human and in animal, the following question can be raised: can co-morbidity schizophrenia – cannabis be explained by a salient positive or a blunted negative motivational valence of cannabis? Even though many pre-clinical studies have been carried out in normal animals on the motivational effects of Δ9-Tetrahydrocannabinol (THC) or other synthetic cannabinoids, none has measured these effects in an animal model of schizophrenia. On the basis of this, we undertook a series of studies on the motivational valence of THC and the cannabinoid agonist WIN55,212-2 (WIN) in an animal model of schizophrenia : the neonatal ventral hippocampus lesion (NVHL). In the first report, we present the results of four studies. The first was aimed at showing that the experimental procedures that we used reproduced some abnormal features of the animal model. Then we evaluated i) the effect of WIN (1 mg/kg) on spontaneous locomotor activity and ii) the motivational valence of THC (0.5 mg/kg) and WIN (1 mg/kg) in the young (post-natal day 28-40, PD28-40) and adult (PD56) rats with the conditioned place-preference paradigm (CPP). As expected, amphetamine produced a higher locomotor activity in NVHL rats, an effect observed at PD56 and not at PD35 (NVHL usual test). THC tended to induce an aversion in control rats at PD56 while WIN produced a significant aversion at PD56 in NVHL rats only. We also assessed, in a second report, the valence of THC (0.5 mg/kg) and WIN (1 and 3 mg/kg), and amphetamine (0.75 mg/kg) using the brain stimulation reward paradigm. Results show that i) the enhancement effect of amphetamine on reward was shorter in adult NVHL rats; ii) THC induced a weak reward attenuation in control rats while WIN produced a marked dose-dependent attenuation in NVHL rats; this effect of WIN was blocked by AM251 (3 mg/kg), an antagonist at CB1 receptors. For the first time, these results suggest that the endogenous cannabinoid system is altered in this animal model of schizophrenia. They indicate that an acute exposure leads to a predominance of negative valence. Even if this seems contradictory with clinical studies, these results highlight the interconnection between the drug and the socio-environment aspects. In addition, they encourage future studies to evaluate this valence on a chronic exposure paradigm with this animal model of schizophrenia. Delta-9-tetrahydrocannabinol WIN55,212-2 AM251 Récompense Locomotion Préférence de place conditionnée Auto-stimulation intracérébrale Schizophrénie Neonatal ventral hippocampus lesion Delta-9-tetrahydrocannabinol WIN55,212-2 AM251 Reward Locomotion Conditioned place preference Intracerebral self-stimulation Schizophrenia

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