Receptor mediated catabolism of plasminogen activators

Grimsley, Philip George, Medical Sciences, Faculty of Medicine, UNSW

January 2009

Humans have two plasminogen activators (PAs), tissue-type plasminogen activator (tPA) and urokinase-type plasminogen activator (uPA), which generate plasmin to breakdown fibrin and other barriers to cell migration. Both PAs are used as pharmaceuticals but their efficacies are limited by their rapid clearance from the circulation, predominantly by parenchymal cells of the liver. At the commencement of the work presented here, the hepatic receptors responsible for mediating the catabolism of the PAs were little understood. tPA degradation by hepatic cell lines was known to depend on the formation of binary complexes with the major PA inhibitor, plasminogen activator inhibitor type-1 (PAI-1). Initial studies presented here established that uPA was catabolised in a fashion similar to tPA by the hepatoma cell line, HepG2. Other laboratories around this time found that the major receptor mediating the binding and endocytosis of the PAs is Low Density Lipoprotein Receptor-related Protein (LRP1). LRP1 is a giant 600 kDa protein that binds a range of structurally and functionally diverse ligands including, activated α2 macroglobulin, apolipoproteins, β amyloid precursor protein, and a number of serpin-enzymes complexes, including PA??PAI-1 complexes. Further studies for the work presented here centred on this receptor. By using radiolabelled binding assays, ligand blots, and Western blots on cultured cells, the major findings are that: (1) basal LRP1 expression on HepG2 is low compared to a clone termed, HepG2a16, but appears to increase in long term culture; (2) a soluble form of LRP1, which retains ligand-binding capacity, is present in human circulation; (3) soluble LRP1 is also present in cerebral spinal fluid where its role in neurological disorders such as Alzheimer??s disease is a developing area of interest; and (4) the release of LRP1 is a mechanism conserved in evolution, possibly as distantly as molluscs. The discovery, identification, and characterisation of soluble LRP1 introduces this protein in the human circulation, and presents a possible further level of regulation for its associated receptor system.

LRP1

Soluble receptor

Soluble LRP1

Radioisotopes

Western blotting

Tissue-type plasminogen activator

Monoclonal antibodies

Recombinant protein production

SDS-PAGE electrophoresis

Flow cytometry

Ligand blotting

tPA

Urokinase-type plasminogen activator

Alzheimer's disease

uPA

Clearance

Endocytosis

Degradation

Evolutionary conservation

HepG2 hepatoma cell line

Plasminogen activator inhibitor type-1

PAI-1

Serpin enzyme complexes

Fibrinolysis

Atherosclerosis

Vascular biology

Haemostatic markers and cardiovascular function in black and white South Africans : the SABPA study / Leandi Lammertyn

Lammertyn, Leandi

January 2015

Motivation In the black population of South Africa, cardiovascular disease (CVD) is rapidly increasing due to urbanisation. Stroke is usually accompanied by a prothrombotic haemostatic profile. Changing lifestyle factors that accompany the urbanisation process could have a negative impact on the haemostatic profile of black South Africans. Elevated levels of pro-coagulant factors, von Willebrand factor (vWF), fibrinogen and fibrin D-dimer have been reported in the black population, which could increase the black population’s susceptibility to CVD. However, low levels of plasminogen activator inhibitor-1 (PAI-1) previously reported in the black population could contribute towards a pro-fibrinolytic state, which may counteract the hypercoagulant state. This may have a beneficial effect on the haemostatic profile of the black population. More investigation into the haemostatic profile of black South Africans is therefore needed to determine if an altered haemostatic profile exists in this group, and if so, to what extent these alterations may relate to cardiovascular dysfunction. This study included markers of both the coagulation (vWF, fibrinogen, fibrin D-dimer) and fibrinolytic (PAI-1, fibrin D-dimer and fibrinolytic potential) systems in an attempt to investigate the haemostatic profile of the black population of South Africa, and for comparison purposes that of the white population as well. The relationship of these markers’ with selected markers of cardiovascular function was also examined to determine if they could possibly contribute to an increase in cardiovascular risk, especially in the black population. Aims The aims of this study were to first compare coagulation and fibrinolysis markers in the black and white populations of South Africa. Furthermore, to determine if associations exist between the selected components of the haemostatic system and markers of cardiovascular function, especially in the black population of South Africa, who tends to be at a higher cardiovascular risk due to altered metabolic and haemostatic profiles. Methodology The Sympathetic activity and Ambulatory Blood Pressure in Africans (SABPA) study was a prospective cohort study that consisted of 409 participants at baseline (2008-2009) that were equally distributed according to both ethnicity (200 black; 209 white) and gender (black, 101 men, 99 women; white, 101 men, 108 women). At follow-up (2011/2012) the cohort totalled 359 participants (170 black, 88 men and 82 women; 189 white, 93 men and 96 women). Data from baseline measurements were used for the first two manuscripts (chapters 2 and 3), while followup data was used for the third manuscript (chapter 4). vWF, fibrinogen, PAI-1, fibrin D-dimer, CLT, serum peroxides, glutathione, glutathione peroxidase and reductase activity were determined, and ambulatory blood pressure and the retinal vessel calibres were measured. The groups were stratified by ethnicity as specified by statistical interaction terms. T-tests and chi-square tests were used to compare means and proportions, respectively. Pearson and partial regression analyses were used to determine correlations between the components of the haemostatic system and cardiovascular function markers. This was followed by multiple linear regression analyses to investigate whether independent associations exist between the variables in both ethnic groups. P-values ≤0.050 were deemed significant. Results and conclusion of each manuscript The first manuscript (chapter 2) compares the haemostatic profiles of the black and white population to determine whether ambulatory blood pressure is related to components of the haemostatic system. The black participants displayed a prothrombotic profile with significantly higher vWF, fibrinogen, PAI-1, fibrin D-dimer and a longer CLT than their white counterparts. Furthermore, partial and multiple linear regression analyses showed a positive association of systolic and diastolic blood pressure with fibrin D-dimer in the black population, while a negative association existed between ambulatory blood pressure and CLT in the white population. These associations suggest that fibrin D-dimer may contribute, at least in part, to the high prevalence of hypertension in the black population. The second manuscript (chapter 3) determined associations between markers of the haemostatic and oxidant-antioxidant systems in the black and white populations. In addition to the prothrombotic profile that exists in the black population, this group also had significantly higher serum peroxides (oxidative stress) and lower glutathione peroxidase activity (antioxidant) levels. Multiple linear regression analyses indicated positive associations between fibrinogen and serum peroxides in both populations. In the white population, an additional positive association was found between serum peroxide and CLT. In the black population, vWF and CLT were negatively associated with GPx activity. The results suggest that there are ethnic-specific relationships between the haemostatic and oxidant-antioxidant systems. The third manuscript (chapter 4) investigated the relationships between the retinal vessel calibres and components of the haemostatic system in the black and white population. The investigation focussed specifically on arteriolar diameters in the lower median, since a narrow arteriolar diameter is known to be associated with elevated blood pressure. In both ethnic groups, a narrower arteriolar calibre was accompanied by narrower venular calibres. Independent positive associations were found between the central retinal vein equivalent (CRVE) and fibrinogen in the black population, as well as vWF and CLT in the white population. In addition, independent negative associations were found between the central retinal artery equivalent and CLT in the black population and with vWF in the white population. The results suggest that haemostatic alterations are linked to early vascular changes that may differ between ethnicities. General conclusion Ethnic-specific relationships between the components of the haemostatic system and measures of cardiovascular function are evident. The prothrombotic profile that is observed in the black population, together with the adverse associations of the haemostatic components with blood pressure, a compromised oxidant-antioxidant profile, and retinal vessel calibres may contribute, at least in part, to the high cardiovascular and cerebrovascular risk evident in this population group. / PhD (Physiology), North-West University, Potchefstroom Campus, 2015

Black

African

Ethnicity

Cardiovascular

von Willebrand factor

Fibrinogen

Plasminogen activator inhibitor-1

Fibrin D-dimer

Clot lysis time

Blood pressure

Oxidative stress

Antioxidant capacity

Retinal vessel calibres

Haemostatic markers and cardiovascular function in black and white South Africans : the SABPA study / Leandi Lammertyn

Lammertyn, Leandi

January 2015

Motivation In the black population of South Africa, cardiovascular disease (CVD) is rapidly increasing due to urbanisation. Stroke is usually accompanied by a prothrombotic haemostatic profile. Changing lifestyle factors that accompany the urbanisation process could have a negative impact on the haemostatic profile of black South Africans. Elevated levels of pro-coagulant factors, von Willebrand factor (vWF), fibrinogen and fibrin D-dimer have been reported in the black population, which could increase the black population’s susceptibility to CVD. However, low levels of plasminogen activator inhibitor-1 (PAI-1) previously reported in the black population could contribute towards a pro-fibrinolytic state, which may counteract the hypercoagulant state. This may have a beneficial effect on the haemostatic profile of the black population. More investigation into the haemostatic profile of black South Africans is therefore needed to determine if an altered haemostatic profile exists in this group, and if so, to what extent these alterations may relate to cardiovascular dysfunction. This study included markers of both the coagulation (vWF, fibrinogen, fibrin D-dimer) and fibrinolytic (PAI-1, fibrin D-dimer and fibrinolytic potential) systems in an attempt to investigate the haemostatic profile of the black population of South Africa, and for comparison purposes that of the white population as well. The relationship of these markers’ with selected markers of cardiovascular function was also examined to determine if they could possibly contribute to an increase in cardiovascular risk, especially in the black population. Aims The aims of this study were to first compare coagulation and fibrinolysis markers in the black and white populations of South Africa. Furthermore, to determine if associations exist between the selected components of the haemostatic system and markers of cardiovascular function, especially in the black population of South Africa, who tends to be at a higher cardiovascular risk due to altered metabolic and haemostatic profiles. Methodology The Sympathetic activity and Ambulatory Blood Pressure in Africans (SABPA) study was a prospective cohort study that consisted of 409 participants at baseline (2008-2009) that were equally distributed according to both ethnicity (200 black; 209 white) and gender (black, 101 men, 99 women; white, 101 men, 108 women). At follow-up (2011/2012) the cohort totalled 359 participants (170 black, 88 men and 82 women; 189 white, 93 men and 96 women). Data from baseline measurements were used for the first two manuscripts (chapters 2 and 3), while followup data was used for the third manuscript (chapter 4). vWF, fibrinogen, PAI-1, fibrin D-dimer, CLT, serum peroxides, glutathione, glutathione peroxidase and reductase activity were determined, and ambulatory blood pressure and the retinal vessel calibres were measured. The groups were stratified by ethnicity as specified by statistical interaction terms. T-tests and chi-square tests were used to compare means and proportions, respectively. Pearson and partial regression analyses were used to determine correlations between the components of the haemostatic system and cardiovascular function markers. This was followed by multiple linear regression analyses to investigate whether independent associations exist between the variables in both ethnic groups. P-values ≤0.050 were deemed significant. Results and conclusion of each manuscript The first manuscript (chapter 2) compares the haemostatic profiles of the black and white population to determine whether ambulatory blood pressure is related to components of the haemostatic system. The black participants displayed a prothrombotic profile with significantly higher vWF, fibrinogen, PAI-1, fibrin D-dimer and a longer CLT than their white counterparts. Furthermore, partial and multiple linear regression analyses showed a positive association of systolic and diastolic blood pressure with fibrin D-dimer in the black population, while a negative association existed between ambulatory blood pressure and CLT in the white population. These associations suggest that fibrin D-dimer may contribute, at least in part, to the high prevalence of hypertension in the black population. The second manuscript (chapter 3) determined associations between markers of the haemostatic and oxidant-antioxidant systems in the black and white populations. In addition to the prothrombotic profile that exists in the black population, this group also had significantly higher serum peroxides (oxidative stress) and lower glutathione peroxidase activity (antioxidant) levels. Multiple linear regression analyses indicated positive associations between fibrinogen and serum peroxides in both populations. In the white population, an additional positive association was found between serum peroxide and CLT. In the black population, vWF and CLT were negatively associated with GPx activity. The results suggest that there are ethnic-specific relationships between the haemostatic and oxidant-antioxidant systems. The third manuscript (chapter 4) investigated the relationships between the retinal vessel calibres and components of the haemostatic system in the black and white population. The investigation focussed specifically on arteriolar diameters in the lower median, since a narrow arteriolar diameter is known to be associated with elevated blood pressure. In both ethnic groups, a narrower arteriolar calibre was accompanied by narrower venular calibres. Independent positive associations were found between the central retinal vein equivalent (CRVE) and fibrinogen in the black population, as well as vWF and CLT in the white population. In addition, independent negative associations were found between the central retinal artery equivalent and CLT in the black population and with vWF in the white population. The results suggest that haemostatic alterations are linked to early vascular changes that may differ between ethnicities. General conclusion Ethnic-specific relationships between the components of the haemostatic system and measures of cardiovascular function are evident. The prothrombotic profile that is observed in the black population, together with the adverse associations of the haemostatic components with blood pressure, a compromised oxidant-antioxidant profile, and retinal vessel calibres may contribute, at least in part, to the high cardiovascular and cerebrovascular risk evident in this population group. / PhD (Physiology), North-West University, Potchefstroom Campus, 2015

Black

African

Ethnicity

Cardiovascular

von Willebrand factor

Fibrinogen

Plasminogen activator inhibitor-1

Fibrin D-dimer

Clot lysis time

Blood pressure

Oxidative stress

Antioxidant capacity

Retinal vessel calibres

Haemostatic variables in African adolescents : the PLAY study / Cornelie Nienaber

Nienaber, Cornelie

January 2006

Cardiovascular disease (CVD) is a major cause of adult morbidity and mortality in developed as well as in developing countries. In black population groups, stroke is more prominent than ischaemic heart disease. This may be attributed to a combination of risk factors seen in this population group inter alia raised haemostatic markers, which favour the development of stroke since it is well known that a disturbance in the haemostatic balance (a hypercoagulable and a hypofibrinolytic state) predisposes to CVD. It is generally accepted that childhood genetic, environmental and behavioural factors lay the groundwork for the manifestation of adult CVD. Therefore, one of the studies that form part of this dissertation was a cross-sectional study to determine whether haemostatic abnormalities are already present in black African adolescents and to determine whether high risk groups exist [in relation to the following haemostatic markers: fibrinogen, factor VIII (FVIII), plasminogen activator inhibitor type 1 activity (PAI-Iact), and thrombin anti-thrombin complex (TAT)] for the development of CVD later in life. The population subdivisions were made according to gender, body fat %, maturity status, height for age Z-score, and habitual PA levels. Since behavioural factors [diet, physical activity (PA), smoking and drinking habits] are controllable determinants, it could be possible to improve CVD risk to a certain degree. Therefore, the second study that forms part of this dissertation attempted to establish whether a PA programme will successfully reduce haemostatic variables in a subset of the study population used in the first study. The reader is referred to the abstracts at the beginning of each separate study manuscript (Chapters 3 and 4), for a description of the subjects, study design and methods used in each study. The results of the cross-sectional study showed that in African adolescents (a) gender independently contributed to the variability in PAI-Iact, but that the gender difference in fibrinogen and TAT could be explained by the significant differences in fat mass and PA levels observed between the genders; (b) fibrinogen was significantly higher in the stunted compared to the non-stunted children indicating that childhood chronic malnutrition may possibly predispose independently to CVD; (c) fitness influences TAT concentrations positively and that (d) no significant differences in FVIII could be found between any of the subdivisions. As these determinants seem to be modifiable through behavioural changes and optimal nutrition status through early life, it raises a sense of urgency to develop strategies for the prevention and treatment of these risk factors. The results of the intervention study showed that an 11-week outdoor PA intervention programme had no significant effect on the haemostatic markers of African adolescents, but the results of this study should be interpreted with caution since (a) seasonal variations could have clouded the effect of the PA intervention as baseline measurements were taken in the summer and end measurements in the winter; (b) attendance of the PA sessions does not necessarily implicate compliance to the exercises given; (c) baseline values seem to play a prominent role in the changes that could be expected during an intervention and, therefore, improvements in the haemostatic profile would most likely be more significant in individuals with raised baseline levels. Similar research on African children is warranted since studies investigating PA's effect on haemostatic variables remain a topic of debate and speculation and data on African population groups are scanty. / Thesis (M.Sc. (Nutrition))--North-West University, Potchefstroom Campus, 2007

Cardiovascular disease

Factor VIII

Fibrinogen

Fitness

Haemostasis

Overfatness

Physical activity

Plasminogen activator inhibitor type 1

South Africa

Stunting

Thrombin antithrombin complex

Modélisation et traitement des accidents vasculaires cérébraux ischémiques / Modelisation and treatment of ischemic stroke disease

Macrez, Richard

14 September 2010

L’injection intraveineuse de l’activateur tissulaire du plasminogène (tPA) est le seul traitement aigu de l’ischémie cérébrale autorisé chez l’Homme. Cependant, la thrombolyse présente des limites d’utilisation, comme son étroite fenêtre thérapeutique, un risque hémorragique et une efficacité de recanalisation malgré tout relativement peu élevée. De plus, la littérature suggère fortement que non seulement le tPA endogène, mais aussi exogène (capable de traverser la barrière hémato-encéphalique), a des effets pro-excitotoxiques. Nous avons proposé que cet effet résulte du clivage de la sous unité NR1 du récepteur NMDA. Malgré un effort important de la communauté scientifique pour chercher de nouveaux traitements, tous les espoirs se sont avérés être des échecs. Sur ces bases, ces travaux de thèse ont consisté à : 1) Améliorer les approches précliniques en développant un nouveau modèle d’ischémie cérébrale chez la souris et en incluant dans les études un des principaux facteur de risque des AVC, le vieillissement ; 2) Développer une stratégie d’immunothérapie visant l’interaction tPA/ récepteur NMDA. J’ai ainsi montré qu’il existe une diminution du volume de lésion ischémique corrélée à l’âge et que cette diminution de tPA est due à une diminution d’expression du facteur de transcription D-Site Albumin Binding Protein (DBP). J’ai également développé un modèle innovant d’ischémie thrombo-embolique chez la souris, dans lequel la reperfusion par le tPA est bénéfique, si tant est qu’elle soit réalisée de manière précoce. Sur ce modèle, j’ai apporté par une stratégie d’immunisation active la preuve in vivo du clivage du domaine amino-terminal de la sous-unité NR1 des récepteurs NMDA. Enfin, j’ai produit un anticorps médicament, capable d’empêcher l’interaction du tPA avec la sous-unité NR1 des récepteurs NMDA, dont une injection unique permet de réduire les lésions ischémiques, mais aussi d’augmenter la fenêtre thérapeutique de la thrombolyse, conférant alors une récupération fonctionnelle à long terme. Cette stratégie pourrait donc accroître la proportion de patients traitables après un AVC ischémique aiguë / Reperfusion with tissue plasminogen activator (tPA) is the only approved treatment for ischemic stroke. However, thrombolysis has some limitations, including a narrow therapeutic window, an elevated risk of hemorrhage transformation and a low level of effective recanalization. Moreover, there is a growing body of evidence that both endogenous and exogenous tPA (able to cross the blood-brain barrier) could mediated pro-excitotoxic effects. We have proposed that this noxious effect results from the cleavage of the NR1 subunit of the NMDA receptor. My thesis work consisted in: 1) Improving pre-clinic approaches by developing a new model of thrombo-embolic ischemia in mice and by taking into account a major risk factor for stroke, aging; 2) Developing a strategy of immunotherapy targeting the interaction between tPA and NMDA receptor. I have thus shown that ischemic lesions decrease as a function of age, due to reduced levels of tPA. Moreover, I have identified DBP (D-site albumin Binding Protein), as being the transcription factor responsible for the control of tPA levels as a function of age. I have also developed a new model of thrombo-embolic ischemia in mice, in which tPA-induced thrombolysis is beneficial, provided it is performed soon enough. In this model, I have demonstrated by using a strategy of active immunization the in vivo occurrence of the cleavage of the NMDA receptor NR1 subunit by tPA. Finally, I have produced an antibody able to prevent the interaction between tPA and the NMDA receptor subunit, of which a single injection confers long lasting brain protection and neurological recovery and can also increase the therapeutic window of thrombolysis. This strategy could thus significantly increase the proportion of treatable ischemic stroke patients

Activateur tissulaire du plasminogène

Barrière hémato-encéphalique

Ischémie cérébrale

Immunothérapie

Modèles expérimentaux

Vieillissement

Thrombolyse

Tissue plasminogen activator

Blood-brain barrier

Brain ischemia

Immunotherapy

Experimental models

Aging

Thrombolysis

616.81

Mecanismos moleculares envolvidos no fenótipo endotelial em resposta a estímulos físicos e químicos / Molecular mechanisms involved in endothelial phenotype in response to physical and chemical stimuli

Silva, Thaís Girão da

01 August 2018

O endotélio reveste a parede vascular e possui função essencial na manutenção da homeostase. A célula endotelial é capaz de perceber estímulos extracelulares, como fatores químicos e mecânicos, transmitir a informação para dentro da célula e regular sua função e fenótipo. Neste sentido, investigamos os mecanismos moleculares associados as células endoteliais em dois contextos importantes de intervenções vasculares 1) nos stents farmacológicos, onde a rapamicina exerce funções antiproliferativas e pró-trombogênicas, e 2) na revascularização cardíaca por ponte de safena, onde o alto estiramento mecânico exerce grande impacto no remodelamento vascular e no fenótipo da célula endotelial. A rapamicina pertence à classe de drogas limus, bastante utilizadas nos stents farmacológicos usados no procedimento de desobstrução vascular. Além de sua função antiproliferativa, exploramos os efeitos deletérios associados a pró-trombogênese. Os dados demonstraram que a rapamicina ativa o receptor de TGF independentemente de seu ligante TGFbeta, promovendo aumento na expressão da PAI-1 (pró-trombogênica), alteração no fenótipo endotelial (Transição endotélio-mesenquimal - EndMT) e na formação de fibras de estresse. Os efeitos observados são dependentes da ativação de Smad2 e independentes da via clássica antiproliferativa por mTOR. Experimentos in vivo mostraram que o tratamento com inibidor do receptor de TGF diminui os efeitos pró-trombogênicos e a expressão de PAI-1 induzidos pela rapamicina em artérias carótidas de camundongos. A ponte de safena é um procedimento bastante utilizado na cirurgia de revascularização cardíaca e a arterialização do segmento venoso submetido ao estresse hemodinâmico arterial resulta em remodelamento vascular, que influencia o sucesso do procedimento. Nossos dados demonstram que a célula endotelial humana de veia safena humana (hSVEC), susceptível as modificações do tipo EndMT induzido quimicamente (estímulo pró-fibrótico e pró-inflamatório), não expressou o mesmo comportamento em resposta ao aumento de estiramento mecânico que ocorre durante a arterialização venosa. Entretanto, detectamos uma pronunciada redução dos filamentos de actina, modulação no padrão de ativação da cofilina e na proporção de actina glomerular (G-actina) entre citoplasma e núcleo, com redução da biodisponibilidade de NO. De modo interessante, demonstramos que a redução no filamento de actina é específica para a célula endotelial venosa, não sendo observado em células endoteliais de origem arterial de aorta e coronária. Em conjunto, os dados mostram que 1) efeitos pró-trombogênicos associados a rapamicina são mediados por ativação do receptor de TGF independente do seu ligante e da atividade antiproliferativa da droga e 2) a adaptação da célula endotelial venosa ao estiramento mecânico envolve modulação da síntese/degradação de filamentos de actina e redução na biodisponibilidade de NO. Estes novos elementos sobre o mecanismo de transdução de estímulos químicos e físicos pelo endotélio poderão ser explorados terapeuticamente para modular a plasticidade endotelial em disfunções cardiovasculares / Endothelium is the inner layer in vascular wall and displays an essential role in the maintenance of cardiovascular homeostasis. Endothelial cell senses the extracellular stimuli, such as chemical and mechanical factors, transduce and process these signals to regulate cell function and phenotype. Here, we investigated molecular underpinning of the endothelial cells under two important scenarios: 1) in drug-eluting stents, where rapamycin exerts antiproliferative and undesirable prothrombogenic functions, and 2) in vein graft bypass surgery, where increased stretch modulates vascular remodeling and endothelial cell phenotype. Rapamycin belongs to the class of limus drugs and is widely used in drug eluting stents (DES) to vascular restenosis. In addition to its antiproliferative function, we explore the deleterious effects associated with prothrombogenesis. Our data demonstrated that rapamycin activates TGF receptor independent of its ligand TGFbeta, in concert with promotion of PAI-1 expression (prothrombogenic), changes in endothelial phenotype (Endothelial to Mesenchymal Transition - EndMT) and stress fibers induction. These effects are Smad2 dependent and independent of the classical antiproliferative mTOR pathway of rapamycin. Our in vivo experiments showed that TGF receptor inhibitor treatment decreases prothrombogenic effects and PAI-1 expression induced by rapamycin in mice carotid arteries. Saphenous vein is widely used in coronary artery bypass surgery (CABG) and the vein arterialization remodeling in response to the increased stress influences graft patency. Our data demonstrated that human saphenous vein endothelial cell (hSVEC) is susceptible to chemically induced endothelial-to-mesenchymal transition (EndMT) by pro-fibrotic and pro-inflammatory stimuli. On the other hand, physical stimulus associated with high stretch failed to induce EndMT. However, we detected a pronounced decrease of actin filaments, modulation of the cofilin activation, changes in the proportion of glomerular actin (G-actin) between cytoplasm and nucleus, and reduction of NO bioavailability. Interestingly, the reduction of actin fibers by high stretch is specific to venous endothelial cell since arterial endothelial cells from aorta, and coronary artery failed to display the response. Altogether, our data show that 1) the thrombogenic effects of rapamycin are mediated by TGF receptor activation independent of its ligand and independent of the antiproliferative pathway of the drug, and 2) the adaptation of venous endothelial cell to mechanical stretch involves synthesis/degradation of actin filaments and reduced NO bioavailability. These new elements on signal transduction of endothelial cells in response to chemical and physical stimuli may be therapeutically explored to modulate endothelial plasticity in cardiovascular disorders

Actin cytoskeleton

Cell transdifferentiation

Células endoteliais

Citoesqueleto de actina

Endothelial cells

Inibidor 1 de ativador de plasminogênio

Plasminogen activator inhibitor 1

Proteínas smad

Signal transduction

Smad proteins

Transdiferenciação celular

Transdução de sinais

Tradução, adaptação transcultural, validade e confiabilidade das escalas Cincinnati Prehospital Stroke Scale e Los Angeles Prehospital Stroke Screen

Almeida, Priscila Masquetto Vieira de.

January 2019

Orientador: Alessandro Lia Mondelli / Resumo: Introdução: O Acidente Vascular Cerebral (AVC) é uma das principais causas de morte e sequelas neurológicas no mundo. O reconhecimento precoce e a pré-notificação hospitalar por serviços de atendimento pré-hospitalar têm sido relacionados com o aumento nas taxas de tratamento adequado. Sendo assim, a American Heart Association e a European Stroke Organisation recomendam o uso de escalas de avaliação pelas equipes do atendimento pré-hospitalar. Objetivo: Traduzir para o idioma português do Brasil, realizar a adaptação transcultural das escalas Cincinnati Prehospital Stroke Scale e Los Angeles Prehospital Stroke Screen e avaliar a confiabilidade e validade na população brasileira. Material e Métodos: Trata-se de um estudo metodológico, transversal e prospectivo realizado em 2 etapas: a primeira constituída pelos processos de tradução e adaptação transcultural das escalas e a segunda pela aplicação das mesmas, que ocorreu entre julho de 2016 e dezembro de 2017. Resultados e Discussão: A Cincinnati Prehospital Stroke Scale ficou denominada de “Escala de Avaliação pré-hospitalar do AVC – Cincinnati”. Os resultados mostraram um Coeficiente de alpha de Cronbach foi de 0,39 e uma alta confiabilidade interobservador do instrumento final, evidenciada pelo alto valor do índice de Kappa, principalmente nos itens “queda do braço” e “fala” que obtiveram o valor máximo. A escala apresentou acurácia de 93% (IC 95% 87,76, – 98,24%), sensibilidade de 92,42% (IC 95%, 86,03 – 98,80% / VPP = 71,7... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Introduction: Strokes are one of the leading causes of death and neurological disability in the world. Early recognition and prehospital notification may increase rates of thrombolysis with recombinant tissue plasminogen activator (rt-PA). Therefore, the American Heart Association and the European Stroke Organization recommend the use of assessment scales by prehospital care teams. Objective: To translate the Cincinnati Prehospital Stroke Scale (CPSS) and the Los Angeles Prehospital Stroke Screen to Portuguese, make a cross-cultural adaptation to Brazilian culture, and validate and verify its reliability in a Brazilian population. Material and Methods: This was a cross-sectional and prospective methodological study carried out in two stages: the first one consisted of the translation and crosscultural adaptation of the original scale and the second involved the application of the final instrument, which occurred between July 2016 and December 2017. Results and discussion: The final version of the Cincinnati Prehospital Stroke Scale was called the “Escala de Avaliação pré-hospitalar do AVC – Cincinnati”. The results showed Cronbach's alpha was 0,39 and a high interobserver reliability of the final instrument, evidenced by the high value of the Kappa index, especially in the items "arm drop" and "speech," which exhibited the maximum values. The scale showed accuracy of 93% (95% CI 87.76 - 98.24%), sensitivity of 92.42% (CI 95% 86.03 - 98.80% / PPV = 71.76) and specificity of 4%... (Complete abstract click electronic access below) / Doutor

Serviços médicos de emergência.

Acidente vascular cerebral.

Sinais e Sintomas

Tradução

Reprodutibilidade dos testes.

Prehospital Emergency Care

Acidente vascular cerebral.

Signs and Symptoms

Tissue Plasminogen Activator

Reprodutibilidade dos testes.

Značaj perfuzione kompjuterizovane tomografije endokranijuma u primeni intravenske trombolitičke terapije kod bolesnika sa akutnim ishemijskim moždanim udarom

Georgievski-Brkić Biljana

24 December 2015

<p>UVOD: Akutni ishemijski moždani udar (AIMU) je poremećaj moždane funkcije nastao usled vaskularnih o&scaron;tećenja, uzrokovane okluzijom ili embolijom krvnog suda. Za razliku od standardnog CT pregleda endokranijuma, CT perfuzija (CTP) je napredna dijagnostička procedura koja može u prvim satima od početka simptoma AIMU pružiti precizne informacije o lokalizaciji i veličini infarkta mozga, a u okviru infarkta, razlikovati srž i ishemijsku penumbru. Samim tim, CTP predstavlja svojevrsnu pomoć u selekciji pacijenata za intravensku primenu rekombinantnog tkivnog plazminogen aktivatora (rtPA). CILJ RADA: Cilj istraživanja je bio da se primenom CTP ispita koliko iznosi: optimalna veličina srži, zatim minimalni i optimalan odnos penumbre i srži infarkta pogodnih za primenu rtPA, maligni profil srži infarkta koji je nepogodan za primenu rtPA i % simptomatske hemoragije kao komplikacije nakon rtPA. MATERIJAL I METODE: Istraživanje je obavljeno u Specijalnoj bolnici &bdquo;Sveti Sava&ldquo; u Beogradu kao petogodi&scaron;nja retrospektivna studija. Studija je obuhvatila ukupno 130 pacijenata sa AIMU kod kojih je primenjena CTP. Eksperimentalnu grupu je sačinjavalo 100 pacijenata kojima je aplikovana rtPA, a kontrolnu grupu 30 pacijenata, koji nisu primili rtPA. Svim ispitanicima su načinjeni: standardni CT pregled glave i CT perfuzija odmah nakon prijema i kontrolni standardni CT pregled endokranijuma 24 h nakon prijema u bolnicu. Pregledi su obavljeni sa 16-slajsnom MSCT aparatu, pri čemu je pokrivenost CTP iznosila 2 cm. &bdquo;Mismatch&ldquo; postoji ukoliko je perfuziona lezija na CBF mapi veća od perfuzionog deficita na CBV mapi (srţ infarkta). REZULTATI: Rezultati studije su pokazali da pacijenti oboleli od AIMU sa mismatchom manjim od 20% nisu imali koristi od primenjene rtPA, a pacijenti sa 20% i vi&scaron;e mismatch-om su imali ili umeren ili značajan neurolo&scaron;ki oporavak. Optimalni mismatch, kojim se postiže visoka uspe&scaron;nost nakon rtPA je iznosio ˃ 101% penumbre. Pacijenti sa povr&scaron;inom perfuzionog deficita na CBV mapi manjom od 1175 mm2 su imali bolji neurolo&scaron;ki oporavak, u odnosu na pacijente savećim lezijama, a samim tim su bili pogodni za primenu rtPA. Perfuzioni deficit na CBV mapi veći od 3000 mm2 (60ml) je predstavljao maligni profil infarkta, usled povećanog rizika od nastanka simptomatske hemoragije i smrtnog ishoda. Simptomatska hemoragija u eksperimentalnoj grupi je iznosila svega 3%, &scaron;to predstavlja nizak procenat komplikacija nakon reperfuzione terapije. ZAKLJUČAK: CT perfuzija je urgentna i brza tehnika, koja nam daje jedinstvene informacije o AIMU, pomaže u dono&scaron;enju odluke o terapijskom pristupu i može poslužiti kao surogat biomarker u predikciji kliničkog ishoda.</p> / <p>INTRODUCTION: Acute ischemic stroke (AIS) is functional brain disorder, which is happened due to vascular damaged, caused by vessel occlusion or embolism. Unlike to noncontrast brain CT, CT perfusion (CTP) is advanced diagnostic procedure, which could give accurate information about localization and extent of AIS in the first hours of symptom onset, and also differentiate infarct cor and ischemic penumbra. Thus, CTP helps in selection patients for administration intravenous recombinant tissue plasminogen activator (rtPA) AIM: The aims of study were to estimate: the size of optimal infarct cor, minimal and optimal ratio between penumbra and infarct core which is suitable for rtPA, malignant profile of infarct core which is not suitable for rtPA and percentage of symptomatic intracerebral hemorrhage as compli-cation after rtPA using CTP. MATERIAL AND METHODS: The investigation was performed in Stroke hospital &bdquo;Sveti Sava&rdquo; in Belgrade as five years retrospective study. Study included 130 patients with AIS with performed CT perfusion. One hundred patients from experimental group were treated with rtPA and thirty patients from control group were not treated with rtPA. All patients underwent baseline noncontrast CT of brain, CT perfusion and control 24 hours follow-up noncontrast brain CT. Examinations were done on 16-slice MSCT and CTP covered an area of 20 mm of brain tissue. &bdquo;Mismatch &ldquo;was defined as a perfusion lesion (CBF lesion) larger than the core lesion (CBV). RESULTS: Results of study showed that the patients with AIS and mismatch less than 20%, had no benefit from rtPA, but patients with &ge; 20% of mismatch had good or excellent clinical outcome. Optimal mismatch, which provided favorable response after rtPA, was ˃101% of penumbra. Patients with cor perfusion lesion (CBV) less than 1175 mm2, are suitable for rtPAand had better clinical outcome, then the patients with larger lesions. Perfusion cor lesions (CBV) larger than 3000 mm2 (60ml) was malignantprofile, because of high risk of symptomatic intracerebral hemorrhage and mortality. Symptomatic hemorrhage in experimental group was only 3%, as a low percentage of complications after reperfusion therapy.<br />CONCLUSION: CTP is emergency and rapid technique, which provides unique information about AIS, helps with clinical decision making and could be surrogate biomarker in prediction of clinical outcome.</p>

Enzyme Encapsulation, Biosensing Endocrine Disrupting Chemicals, and Bio-therapeutic Expression Platforms Using Cell-Free Protein Synthesis

Yang, Seung Ook

01 June 2017

Cell-free protein synthesis (CFPS) is a powerful protein expression platform where protein synthesis machinery is borrowed from living organisms. Target proteins are synthesized in a reaction tube together with cell extract, amino acids, energy source, and DNA. This reaction is versatile, and dynamic optimizations of the reaction conditions can be performed. The "œopen" nature of CFPS makes it a compelling candidate for many technologies and applications. This dissertation reports new and innovative applications of CFPS including 1) enzyme encapsulation in a virus-like particle, 2) detection of endocrine disrupting chemicals in the presence of blood and urine, and 3) expression of a multi-disulfide bond therapeutic protein. Two major limitations of enzymes are their instability and recycling difficulty. To overcome these limitations, we report the first enzyme encapsulation in the CFPS by immobilizing in a virus-like particle using an RNA aptamer. This technique allows simple and fast enzyme production and encapsulation We demonstrate, for the first time, the Rapid Adaptable Portable In vitro Detection biosensor platform (RAPID) for detecting endocrine disrupting chemicals (EDCs) in human blood and urine samples. Current living cell-based assays can take a week to detect EDCs, but RAPID requires only 2 hours. It utilizes the versatile nature of CFPS for biosensor protein complex production and EDC detection. Biotherapeutic protein expression in E. coli suffers from inclusion body formation, insolubility, and mis-folding. Since CFPS is not restricted by a cell wall, dynamic optimization can take place during the protein synthesis process. We report the first expression of full-length tissue plasminogen activator (tPA) using CFPS. These research works demonstrate the powerful and versatile nature of the CFPS.

Seung Ook Yang

cell-free protein synthesis

enzyme encapsulation

enzyme immobilization

endocrine disrupting chemicals

RAPID

blood

urine

therapeutic protein

tissue plasminogen activator

Biochemistry

Haemostatic variables in African adolescents : the PLAY study / Cornelie Nienaber

Nienaber, Cornelie

January 2006

Thesis (M.Sc. (Nutrition))--North-West University, Potchefstroom Campus, 2007.

Cardiovascular disease

Factor VIII

Fibrinogen

Fitness

Haemostasis

Overfatness

Physical activity

Plasminogen activator inhibitor type 1

South Africa

Stunting

Thrombin antithrombin complex