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Cognitive Impairments after Hemorrhagic Brain Injury: Therapeutic Potential of Cofilin InhibitionAli, Mohammad January 2021 (has links)
No description available.
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Risk-benefit of Antithrombotic Treatment in Patients with Hemorrhage-prone Cerebral Small Vessel DiseaseBalali, Pargol January 2023 (has links)
Balali_Pargol_MSc thesis_Neuroscience department_2023Sep / Background: Cerebral microbleeds are asymptomatic neuroimaging markers of small
vessel disease (SVD), visualized as small hypointensities on blood-sensitive magnetic
resonance imaging (MRI) sequences. Patients with ischemic stroke and microbleeds are
at a higher risk of future ischemic stroke and intracranial hemorrhage. Antithrombotic
therapies, the mainstay treatment of secondary stroke prevention, are associated with an
increased risk of bleeding. This raises concerns surrounding the net benefit of
antithrombotic therapies in these hemorrhage-prone patients. The overarching aim of this
thesis is to determine the safety of antithrombotic treatments in patients with hemorrhage-prone SVD marked by microbleeds on MRI or prior intracerebral hemorrhage (ICH). I
aimed to characterize the association between baseline microbleeds and the risk of future
clinical outcomes in patients with ischemic stroke and whether there exists treatment
effect modification of different anticoagulants on clinical outcomes according to
microbleeds presence, location, and number.
Methods: We performed post hoc analyses on two multicenter previously conducted
randomized trials in patients with non-cardioembolic ischemic stroke. For the PACIFIC-STROKE trial, we used multivariable regression models to determine the contribution of
microbleeds to the risk of new microbleeds, hemorrhagic transformation (HT), ischemic
stroke, intracranial hemorrhage, and death. We assessed the treatment effect of
asundexian, a factor XIa inhibitor, vs. placebo on these clinical outcomes, stratified by
microbleeds presence, location, and number.
I was trained on standardized rating of microbleeds on MRI, achieved excellent interrater
reliability, and rated all DATAS-II participant MRIs. I used multivariable logistic
regression models to identify the association between microbleeds and HT and 90-day
excellent functional outcome. I assessed the interaction between treatment with
dabigatran, a direct thrombin inhibitor, vs. aspirin and microbleeds for these outcomes.
Separately, I performed a review of the literature and wrote an editorial discussing the
optimum timing of antiplatelet re-initiation after ICH.
Results: The PACIFIC-STROKE post hoc analyses showed that microbleeds are
associated with a 1.6-fold and 4.4-fold higher risk of HT and new microbleeds,
respectively. The DATAS-II exploratory analyses demonstrated no association between
the risk of outcomes and microbleeds presence. We found no interaction between
treatment assignment and microbleed presence for any of the clinical outcomes
investigated in either of these studies. Based on the totality of evidence, we concluded
that early resumption of antiplatelets in ICH survivors is likely to be safe.
Conclusion: Our findings do not support existing concerns surrounding the use of
anticoagulants in patients with acute ischemic stroke and microbleeds on MRI, nor for the
early resumption of antiplatelets in ICH survivors. / Thesis / Master of Science (MSc) / Diseases of small brain blood vessels can lead to strokes due to blockage or
bleeding. Small, asymptomatic brain bleeds on MRIs (microbleeds) are common among
affected patients. Patients with clot-induced stroke and microbleeds have a higher risk of
both types of strokes. Blood thinners are standard treatments to prevent future clotting
events after clot-induced stroke. However, their potential to increase the risk of brain
bleeding has raised concerns regarding their use in patients with microbleeds or bleeding-induced stroke.
We assessed information from two large, previously completed randomized trials
to evaluate the safety of strong blood thinners (anticoagulants) in patients with clot-induced
stroke and microbleeds. Additionally, we evaluated the risk vs. benefit of
restarting milder blood thinners (antiplatelets) early after bleeding-induced stroke.
Bleeding was more prevalent in patients with microbleeds; however, the effect of
the anticoagulants tested on bleeding outcomes was not modified by microbleed
presence. Overall, our findings suggest that blood thinners are safe in patients with clot-induced stroke and microbleeds, and that early resumption of antiplatelets seems safe in
patients with bleeding-induced stroke.
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Nitroxidative Stress Induced Neurodegeneration In Intracerebral Hemorrhagic Stroke-a Nanomedical ApproachMadajka, Maria H. January 2007 (has links)
No description available.
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Estrogen signaling in stroke : genetic and experimental studiesStrand, Magnus January 2007 (has links)
Stroke is a common and multifactorial disease influenced by genetic and environmental risk factors. It is a highly heterogeneous entity consisting of two main types, ischemic (80%) and hemorrhagic (20%) stroke. The most common form of hemorrhagic stroke is intracerebral hemorrhage (ICH). Ischemic stroke mainly results from thrombotic or embolic events, while ICH is caused by the rupture of an artery in the brain. The mean age of first-ever stroke is 75 years (73 vs. 78 years, for men and women, respectively) and the age-specific stroke incidence is higher for men as compared to women, suggesting that hormonal factors confer protection. A large body of experimental and observational studies shows that estrogens exert beneficial effects in the cardiovascular system. However, large, recent, clinical randomized trials have failed to demonstrate a lower risk of stroke with hormone replacement therapy (HRT) in elderly postmenopausal women. It is possible that HRT may only protect a subgroup of women. Here, genetic predisposition might be involved. Stroke incidence is 50% higher in northern compared to southern Sweden, suggesting a genetic predisposition in this population. This relatively homogeneous population displays founder effects, making it well suited for genetic studies. Since 1985, the MONICA and VIP projects have conducted large-scale cardiovascular health surveys in this population. Information about conventional stroke risk determinants and also DNA have been collected, and two prospective, nested case-referent cohorts (113 cases and 226 controls; 275 cases and 549 controls) have been sampled. To investigate whether genes of the estrogen signaling system may be important in stroke development, we performed genetic association studies, including specific functional single nucleotide polymorphisms in the genes for estrogen receptor alpha (ERα, ESR1), and its target genes osteoprotegerin (OPG, TNFRS11B) and interleukin-6 (IL-6, IL6). We found a significant association between the common c.454-397T/T genotype in ESR1 and ICH, remaining after adjustments for conventional stroke risk factors. The c.454-397T/T genotype also associated with increased systolic (SBP) and diastolic blood pressure (DBP). The combination of c.454- 397T/T and either hypertension, increased SBP, or increased DBP boosted this association substantially and significant synergistic effects on ICH risk between this genotype and increased blood pressure were demonstrated. In a second study, we found a similar association between the common OPG-1181C/C genotype and ICH. Cognitive impairments, including spatial memory and learning deficiencies, are common after stroke. Estrogens improve cognitive functions, including memory and learning processes, in postmenopausal women and ovariectomized rodents. Post-ischemic housing of rats in an enriched environment (EE) improves recovery of spatial memory and learning impairments. Both estrogen and EE induce neuroplasticity in the hippocampus. We hypothesized that 17β- estradiol combined with EE would accelerate recovery after experimental focal brain ischemia in ovariectomized rats and that such improvements could be related to expression of nerve growth factor-induced gene A (NGFI-A) in the hippocampus. Five to six weeks after middle cerebral artery occlusion, 17β-estradiol–treated rats housed in an EE showed significant improvements in cognitive function (i.e., shorter latency and path in the Morris water maze task) and significantly higher NGFI-A mRNA expression in bilateral cornu ammonis 1 (CA1) and ipsilateral dentate gyrus (DG) compared to placebo-treated animals in EE. In conclusion, we present evidence for the association between polymorphic variants in the ESR1 and TNFRS11B genes and ICH and show that 17β-estradiol in combination with EE accelerates cognitive functions in a rat stroke model, putatively through upregulation of NGFI-A in hippocampal subregions. These findings may contribute to an increased understanding of the underlying genetic etiology of ICH and may be informative for the primary prevention of this disease. They also provide hope for 17β-estradiol combined with early environmental enrichment as a novel therapeutic option following ischemic stroke.
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Efeito cerebroprotetor do pré-condicionamento isquêmico sobre aspectos celulares e funcionais no modelo de hemorragia intracerebral focal em ratos Wistar adultosDelgado, Thamiris Fenalti January 2017 (has links)
O Acidente Vascular Encefálico (AVE) Hemorrágico representa mais de 10% de todos os casos de AVE e possui altas taxas de morbidade e de mortalidade. Os pacientes que sobrevivem a este evento permanecem com alguma disfunção motora, que algumas vezes é incapacitante. O extravasamento de sangue em um AVE hemorrágico ocorre, geralmente, em regiões onde há bifurcação de pequenas arteríolas penetrantes, como na região dos núcleos da base. O estriado, importante componente dessa região, está relacionado a funções motoras superiores, como o planejamento e a execução do movimento. Alguns estudos demonstram que o pré-condicionamento (PC) isquêmico pode gerar a tolerância a outros eventos que acometem o sistema nervoso. O PC é definido como fenômeno decorrente da exposição de um tecido ou órgão a um insulto sub-letal capaz de resultar em adaptações determinantes para a tolerância tecidual. Isso ocorre mesmo quando esses dois estímulos são de origens diferentes; neste caso diz-se que o PC desenvolveu tolerância cruzada. Desta forma, o presente estudo dedicou-se ao estudo de efeitos celulares e funcionais do pré-condicionamento isquêmico, por oclusão bilateral das artérias carótidas durante 10 minutos, sobre o modelo de hemorragia intracerebral (HIC), por administração intraestriatal de colagenase do tipo IV-S em ratos. A hipótese de trabalho era de que o PC causaria tolerância cruzada para a HIC, e consequente neuroproteção avaliada por testes motores, volume de lesão, com envolvimento de astrocitose e de micróglia reativa Foram usados 67 ratos machos Wistar adultos, divididos em 4 grupos: Sham (controle cirúrgico), PC, HIC, PC+HIC. Assim, os animais dos grupos PC e PC+HIC foram submetidos ao pré-condicionamento e 24 horas depois os animais HIC e PC+HIC receberam a injeção de colagenase, enquanto os animais Sham e PC receberam uma injeção de salina. A avaliação motora dos animais foi realizada a partir dos testes do cilindro e do Staircase. Trinta e quatro dias após a HIC os animais foram perfundidos e o estriado ipsilateral à injeção foi dissecada para obtenção de amostras teciduais necessárias à avaliação da perda tecidual e quantificação de intensidade de fluorescência de GFAP (proteína glial fibrilar ácida) e OX-42, importantes marcadores de astrócitos e microglia, respectivamente. Os resultados demonstram que: a) a HIC causa deficits motores em ambos os testes realizados, e que o PC reverte este efeito; b) a HIC causa lesão estriatal que não é revertido pelo pré-condicionamento; c) a HIC causa aumento da intensidade de fluorescência para GFAP e para OX-42, e o PC reverte apenas a reatividade da micróglia. Em conjunto, sugere-se que o pré-condicionamento isquêmico causa tolerância cruzada com a hemorragia intracerebral experimental, resultando em proteção funcional, mas não morfológica, possivelmente associada a uma diminuição da reatividade da microglia após o evento hemorrágico. / Hemorrhagic Vascular Stroke (EVA) represents more than 10% of all stroke cases with high rates of morbidity and mortality. Patients who survive this event, remain with some motor dysfunction, which is sometimes disabling. The extravasation of blood in a hemorrhagic stroke occurs, generally, in regions where there is bifurcation of small vessels, as in the region of striatum. The striatum is related to the higher motor functions, such as the planning and execution of the movement. Some studies have shown that preconditioning (PC) can generate a tolerance to other events that accompany the nervous system. The PC is presented as the source of the exposure of a sub-lethal, resulting in an adaptation of determinants to a tissue tolerance. Thus, the present study aimed shows the ischemic preconditioning effects, by bilateral occlusion of the carotid arteries for 10 minutes, on the intracerebral hemorrhage (ICH) model, by intra- striatum administration of type IV S collagenase in rats. The working hypothesis was tolerance to HIC, and consequent neuroprotection by motor function, lesion volume, astrocytosis and reactive microglia. A total of 84 male Wistar adult rats were divided into 4 groups: Sham (surgical control), PC, HIC, PC + HIC Thus, the animals of the PC and PC + HIC groups were introduced to the preconditioning and 24 hours later, the HIC and PC + HIC animals received a collagenase injection, while the Sham and PC animals received a saline injection. The evaluation of the animal function was performed from cylinder and Staircase tests. Thirty-four days after the surgery, the striatum was dissected and prepared to lesion volume analysis and fluorescence intensity of GFAP quantification (acid glial fibrillary protein) and OX-42, important astrocyte and microglia markers respectively. The results demonstrate that: a) an HIC causes motor deficits in both tests performed, and that the PC reverses this effect; b) an ICH causes a striatal lesion that is not reversed by preconditioning; c) an HIC promoted high fluorescence intensity for GFAP and OX-42, and PC reverses the microglia reactivity. Taken together, we suggest that ischemic preconditioning combined with experimental intracerebral hemorrhage, promotes functional but not morphological protection, being associated with the microglial reactivity decrease after the hemorrhagic event.
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Efeito cerebroprotetor do pré-condicionamento isquêmico sobre aspectos celulares e funcionais no modelo de hemorragia intracerebral focal em ratos Wistar adultosDelgado, Thamiris Fenalti January 2017 (has links)
O Acidente Vascular Encefálico (AVE) Hemorrágico representa mais de 10% de todos os casos de AVE e possui altas taxas de morbidade e de mortalidade. Os pacientes que sobrevivem a este evento permanecem com alguma disfunção motora, que algumas vezes é incapacitante. O extravasamento de sangue em um AVE hemorrágico ocorre, geralmente, em regiões onde há bifurcação de pequenas arteríolas penetrantes, como na região dos núcleos da base. O estriado, importante componente dessa região, está relacionado a funções motoras superiores, como o planejamento e a execução do movimento. Alguns estudos demonstram que o pré-condicionamento (PC) isquêmico pode gerar a tolerância a outros eventos que acometem o sistema nervoso. O PC é definido como fenômeno decorrente da exposição de um tecido ou órgão a um insulto sub-letal capaz de resultar em adaptações determinantes para a tolerância tecidual. Isso ocorre mesmo quando esses dois estímulos são de origens diferentes; neste caso diz-se que o PC desenvolveu tolerância cruzada. Desta forma, o presente estudo dedicou-se ao estudo de efeitos celulares e funcionais do pré-condicionamento isquêmico, por oclusão bilateral das artérias carótidas durante 10 minutos, sobre o modelo de hemorragia intracerebral (HIC), por administração intraestriatal de colagenase do tipo IV-S em ratos. A hipótese de trabalho era de que o PC causaria tolerância cruzada para a HIC, e consequente neuroproteção avaliada por testes motores, volume de lesão, com envolvimento de astrocitose e de micróglia reativa Foram usados 67 ratos machos Wistar adultos, divididos em 4 grupos: Sham (controle cirúrgico), PC, HIC, PC+HIC. Assim, os animais dos grupos PC e PC+HIC foram submetidos ao pré-condicionamento e 24 horas depois os animais HIC e PC+HIC receberam a injeção de colagenase, enquanto os animais Sham e PC receberam uma injeção de salina. A avaliação motora dos animais foi realizada a partir dos testes do cilindro e do Staircase. Trinta e quatro dias após a HIC os animais foram perfundidos e o estriado ipsilateral à injeção foi dissecada para obtenção de amostras teciduais necessárias à avaliação da perda tecidual e quantificação de intensidade de fluorescência de GFAP (proteína glial fibrilar ácida) e OX-42, importantes marcadores de astrócitos e microglia, respectivamente. Os resultados demonstram que: a) a HIC causa deficits motores em ambos os testes realizados, e que o PC reverte este efeito; b) a HIC causa lesão estriatal que não é revertido pelo pré-condicionamento; c) a HIC causa aumento da intensidade de fluorescência para GFAP e para OX-42, e o PC reverte apenas a reatividade da micróglia. Em conjunto, sugere-se que o pré-condicionamento isquêmico causa tolerância cruzada com a hemorragia intracerebral experimental, resultando em proteção funcional, mas não morfológica, possivelmente associada a uma diminuição da reatividade da microglia após o evento hemorrágico. / Hemorrhagic Vascular Stroke (EVA) represents more than 10% of all stroke cases with high rates of morbidity and mortality. Patients who survive this event, remain with some motor dysfunction, which is sometimes disabling. The extravasation of blood in a hemorrhagic stroke occurs, generally, in regions where there is bifurcation of small vessels, as in the region of striatum. The striatum is related to the higher motor functions, such as the planning and execution of the movement. Some studies have shown that preconditioning (PC) can generate a tolerance to other events that accompany the nervous system. The PC is presented as the source of the exposure of a sub-lethal, resulting in an adaptation of determinants to a tissue tolerance. Thus, the present study aimed shows the ischemic preconditioning effects, by bilateral occlusion of the carotid arteries for 10 minutes, on the intracerebral hemorrhage (ICH) model, by intra- striatum administration of type IV S collagenase in rats. The working hypothesis was tolerance to HIC, and consequent neuroprotection by motor function, lesion volume, astrocytosis and reactive microglia. A total of 84 male Wistar adult rats were divided into 4 groups: Sham (surgical control), PC, HIC, PC + HIC Thus, the animals of the PC and PC + HIC groups were introduced to the preconditioning and 24 hours later, the HIC and PC + HIC animals received a collagenase injection, while the Sham and PC animals received a saline injection. The evaluation of the animal function was performed from cylinder and Staircase tests. Thirty-four days after the surgery, the striatum was dissected and prepared to lesion volume analysis and fluorescence intensity of GFAP quantification (acid glial fibrillary protein) and OX-42, important astrocyte and microglia markers respectively. The results demonstrate that: a) an HIC causes motor deficits in both tests performed, and that the PC reverses this effect; b) an ICH causes a striatal lesion that is not reversed by preconditioning; c) an HIC promoted high fluorescence intensity for GFAP and OX-42, and PC reverses the microglia reactivity. Taken together, we suggest that ischemic preconditioning combined with experimental intracerebral hemorrhage, promotes functional but not morphological protection, being associated with the microglial reactivity decrease after the hemorrhagic event.
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Efeito cerebroprotetor do pré-condicionamento isquêmico sobre aspectos celulares e funcionais no modelo de hemorragia intracerebral focal em ratos Wistar adultosDelgado, Thamiris Fenalti January 2017 (has links)
O Acidente Vascular Encefálico (AVE) Hemorrágico representa mais de 10% de todos os casos de AVE e possui altas taxas de morbidade e de mortalidade. Os pacientes que sobrevivem a este evento permanecem com alguma disfunção motora, que algumas vezes é incapacitante. O extravasamento de sangue em um AVE hemorrágico ocorre, geralmente, em regiões onde há bifurcação de pequenas arteríolas penetrantes, como na região dos núcleos da base. O estriado, importante componente dessa região, está relacionado a funções motoras superiores, como o planejamento e a execução do movimento. Alguns estudos demonstram que o pré-condicionamento (PC) isquêmico pode gerar a tolerância a outros eventos que acometem o sistema nervoso. O PC é definido como fenômeno decorrente da exposição de um tecido ou órgão a um insulto sub-letal capaz de resultar em adaptações determinantes para a tolerância tecidual. Isso ocorre mesmo quando esses dois estímulos são de origens diferentes; neste caso diz-se que o PC desenvolveu tolerância cruzada. Desta forma, o presente estudo dedicou-se ao estudo de efeitos celulares e funcionais do pré-condicionamento isquêmico, por oclusão bilateral das artérias carótidas durante 10 minutos, sobre o modelo de hemorragia intracerebral (HIC), por administração intraestriatal de colagenase do tipo IV-S em ratos. A hipótese de trabalho era de que o PC causaria tolerância cruzada para a HIC, e consequente neuroproteção avaliada por testes motores, volume de lesão, com envolvimento de astrocitose e de micróglia reativa Foram usados 67 ratos machos Wistar adultos, divididos em 4 grupos: Sham (controle cirúrgico), PC, HIC, PC+HIC. Assim, os animais dos grupos PC e PC+HIC foram submetidos ao pré-condicionamento e 24 horas depois os animais HIC e PC+HIC receberam a injeção de colagenase, enquanto os animais Sham e PC receberam uma injeção de salina. A avaliação motora dos animais foi realizada a partir dos testes do cilindro e do Staircase. Trinta e quatro dias após a HIC os animais foram perfundidos e o estriado ipsilateral à injeção foi dissecada para obtenção de amostras teciduais necessárias à avaliação da perda tecidual e quantificação de intensidade de fluorescência de GFAP (proteína glial fibrilar ácida) e OX-42, importantes marcadores de astrócitos e microglia, respectivamente. Os resultados demonstram que: a) a HIC causa deficits motores em ambos os testes realizados, e que o PC reverte este efeito; b) a HIC causa lesão estriatal que não é revertido pelo pré-condicionamento; c) a HIC causa aumento da intensidade de fluorescência para GFAP e para OX-42, e o PC reverte apenas a reatividade da micróglia. Em conjunto, sugere-se que o pré-condicionamento isquêmico causa tolerância cruzada com a hemorragia intracerebral experimental, resultando em proteção funcional, mas não morfológica, possivelmente associada a uma diminuição da reatividade da microglia após o evento hemorrágico. / Hemorrhagic Vascular Stroke (EVA) represents more than 10% of all stroke cases with high rates of morbidity and mortality. Patients who survive this event, remain with some motor dysfunction, which is sometimes disabling. The extravasation of blood in a hemorrhagic stroke occurs, generally, in regions where there is bifurcation of small vessels, as in the region of striatum. The striatum is related to the higher motor functions, such as the planning and execution of the movement. Some studies have shown that preconditioning (PC) can generate a tolerance to other events that accompany the nervous system. The PC is presented as the source of the exposure of a sub-lethal, resulting in an adaptation of determinants to a tissue tolerance. Thus, the present study aimed shows the ischemic preconditioning effects, by bilateral occlusion of the carotid arteries for 10 minutes, on the intracerebral hemorrhage (ICH) model, by intra- striatum administration of type IV S collagenase in rats. The working hypothesis was tolerance to HIC, and consequent neuroprotection by motor function, lesion volume, astrocytosis and reactive microglia. A total of 84 male Wistar adult rats were divided into 4 groups: Sham (surgical control), PC, HIC, PC + HIC Thus, the animals of the PC and PC + HIC groups were introduced to the preconditioning and 24 hours later, the HIC and PC + HIC animals received a collagenase injection, while the Sham and PC animals received a saline injection. The evaluation of the animal function was performed from cylinder and Staircase tests. Thirty-four days after the surgery, the striatum was dissected and prepared to lesion volume analysis and fluorescence intensity of GFAP quantification (acid glial fibrillary protein) and OX-42, important astrocyte and microglia markers respectively. The results demonstrate that: a) an HIC causes motor deficits in both tests performed, and that the PC reverses this effect; b) an ICH causes a striatal lesion that is not reversed by preconditioning; c) an HIC promoted high fluorescence intensity for GFAP and OX-42, and PC reverses the microglia reactivity. Taken together, we suggest that ischemic preconditioning combined with experimental intracerebral hemorrhage, promotes functional but not morphological protection, being associated with the microglial reactivity decrease after the hemorrhagic event.
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Recurrent stroke : risk factors, predictors and prognosisPennlert, Johanna January 2016 (has links)
Background Many risk factors for stroke are well characterized and might, at least to some extent, be similar for first-ever stroke and for recurrent stroke events. However, previous studies have shown heterogeneous results on predictors and rates of stroke recurrence. Patients who survive spontaneous intracerebral hemorrhage (ICH) often have compelling indications for antithrombotic (AT) treatment (antiplatelet (AP) and/or anticoagulant (AC) treatment), but due to controversy of the decision to treat, a large proportion of these patients are untreated. In the absence of evidence from randomized controlled trials (RCTs), there is need for more high- quality observational data on the clinical impact of, and optimal timing of AT in ICH survivors. The aims of this thesis were to assess time trends in stroke recurrence, to determine the factors associated with an increased risk of stroke recurrence – including socioeconomic factors – and to determine to what extent ICH survivors with and without atrial fibrillation (AF) receive AT treatment and to determine the optimal timing (if any) of such treatment. Methods The population-based Monitoring Trends and Determinants of Cardiovascular Disease (MONICA) stroke incidence register was used to assess the epidemiology and predictors of stroke recurrence after ischemic stroke (IS) and ICH from 1995 to 2008 in northern Sweden. Riksstroke, the Swedish stroke register, linked with the National Patient Register and the Swedish Dispensed Drug Register, made it possible to identify survivors of first-ever ICH from 2005 to 2012 with and without concomitant AF to investigate to what extent these patients were prescribed AP and AC therapy. The optimal timing of initiating treatment following ICH in patients with AF 2005–2012 was described through separate cumulative incidence functions for severe thrombotic and hemorrhagic events and for the combined endpoint “vascular death or non-fatal stroke”. Riksstroke data on first-ever stroke patients from 2001 to 2012 was linked to the Longitudinal Integration Database for Health Insurance and Labour market studies to add information on education and income to investigate the relationship between socioeconomic status and risk of recurrence. Results Comparison between the cohorts of 1995–1998 and 2004–2008 showed declining risk of stroke recurrence (hazard ratio: 0.64, 95% confidence interval (CI): 0.52-0.78) in northern Sweden. Significant factors associated with an increased risk of stroke recurrence were age and diabetes. Following ICH, a majority (62%) of recurrent stroke events were ischemic. The nationwide Riksstroke study confirmed the declining incidence, and it further concluded that low income, primary school as highest attained level of education, and living alone were associated with a higher risk of recurrence beyond the acute phase. The inverse effects of socioeconomic status on risk of recurrence did not differ between men and women and persisted over the study period. Of Swedish ICH-survivors with AF, 8.5% were prescribed AC and 36.6% AP treatment, within 6 months of ICH. In patients with AF, predictors of AC treatment were less severe ICH, younger age, previous anticoagulation, valvular disease and previous IS. High CHA2DS2-VASc scores did not seem to correlate with AC treatment. We observed both an increasing proportion of AC treatment at time of the initial ICH (8.1% in 2006 compared with 14.6% in 2012) and a secular trend of increasing AC use one year after discharge (8.3% in 2006 versus 17.2% in 2011) (p<0.001 assuming linear trends). In patients with high cardiovascular event risk, AC treatment was associated with a reduced risk of vascular death and non-fatal stroke with no significantly increased risk of severe hemorrhage. The benefit appeared to be greatest when treatment was started 7–8 weeks after ICH. For high-risk women, the total risk of vascular death or stroke recurrence within three years was 17.0% when AC treatment was initiated eight weeks after ICH and 28.6% without any antithrombotic treatment (95% CI for difference: 1.4% to 21.8%). For high-risk men, the corresponding risks were 14.3% vs. 23.6% (95% CI for difference: 0.4% to 18.2%). Conclusion Stroke recurrence is declining in Sweden, but it is still common among stroke survivors and has a severe impact on patient morbidity and mortality. Age, diabetes and low socioeconomic status are predictors of stroke recurrence. Regarding ICH survivors with concomitant AF, physicians face the clinical dilemma of balancing the risks of thrombosis and bleeding. In awaiting evidence from RCTs, our results show that AC treatment in ICH survivors with AF was initiated more frequently over the study period, which seems beneficial, particularly in high-risk patients. The optimal timing of anticoagulation following ICH in AF patients seems to be around 7–8 weeks following the hemorrhage.
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Studies on the role of Cofilin signaling in Hemin induced Microglial activationBin Sayeed, Muhammad Shahdaat 22 December 2016 (has links)
No description available.
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Estratégias de neuroproteção em diferentes modelos de acidente vascular encefálico: avaliação do dano neuromotor e estresse oxidativo estriatal / Neuroprotection strategies in different models of stroke: evaluation of neuromotor damage and striatal oxidative stressSosa, Priscila Marques, Sosa, Priscila Marques 15 March 2016 (has links)
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Previous issue date: 2016-03-15 / O AVE é uma das principais causas de morte e incapacidade funcional em todo mundo, sendo dividido em dois subtipos: isquêmico, causado pela diminuição do fluxo sanguíneo; e hemorrágico, caracterizado pelo extravasamento de sangue nos tecidos encefálicos. Considerando a alta taxa de mortalidade e a gravidade das sequelas pós AVE, torna-se de extrema importância a busca por alvos terapêuticos que visem diminuir as sequelas causadas pelos quadros isquêmico e hemorrágico. Sendo assim, este estudo investigou os efeitos neuroprotetores do exercício físico (8 semanas previamente à lesão) em um quadro de AVE isquêmico (através da oclusão bilateral das artérias carótidas comuns) e os efeitos neuroprotetores da apocinina (posteriormente à lesão – 2, 6 e 24h – na dose 0,5mg/kg) em um quadro de AVE hemorrágico (através da infusão de colagenase no corpo estriado) em ratos Wistar. Para avaliar a função motora dos animais, foram utilizados os testes de Campo Aberto (CA), Rotarod (RR) e Escala de Déficit Neurológico (NDS), e, para avaliar o balanço redox estriatal, avaliamos a presença de EROs, TBARS (espécies reativas ao ácido tiobarbitúrico) e capacidade antioxidante total (FRAP). Nossos resultados mostraram que o exercício físico é uma estratégia parcialmente eficaz de proteção em um modelo de AVE isquêmico. No entanto, a apocinina não se mostrou uma estratégia de neuroproteção eficaz em um modelo de AVE hemorrágico. Estes resultados revelam a possibilidade da utilização do exercício físico como estratégia de neuroproteção. A apocinina, por sua vez, precisa ser melhor estudada em casos de AVE hemorrágico, considerando a investigação do seu mecanismo, doses e tempos de administração. / The stroke is one of the leading causes of death and disability worldwide, and is divided into two subtypes: ischemic, caused by a decreased on blood flow; and hemorrhagic, characterized by leakage of blood in brain tissue. Considering the high mortality rate and severity of post stroke sequelae, it is extremely important to search for therapeutic targets aimed at reducing the consequences caused by ischemic and hemorrhagic frames. Thus, this study investigated the neuroprotective effects of physical exercise (8 weeks prior to injury) in an ischemic stroke modle (by bilateral occlusion of the common carotid arteries) and the neuroprotective effects of apocynin (after the injury - 2, 6 and 24 hours - at a dose 0.5 mg/kg) in a hemorrhagic stroke model (by collagenase infusion into the striatum) in Wistar rats. Open Field (OF), Rotarod (RR) and Neurologic Disabilities Scale (NDS) were used to evaluate the motor function of the animals. To the striatal redox balance evaluation we assessed the presence of ROS, TBARS (reactive species to thiobarbituric acid) and total antioxidant capacity (FRAP). Our results showed that physical exercise is a partially effective strategy to protect against ischemic stroke. However, apocynin was not an effective neuroprotective strategy in a experimental model of hemorrhagic stroke. These results show the possibility of using exercise as a neuroprotective strategy. The apocynin need to be better studied in cases of hemorrhagic stroke, whereas the investigation of its mechanism, dosages and times of administration.
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