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41	Dieta com sobrecarga de cálcio e fósforo leva à diminuição do volume ósseo de ratos urêmicos / Dietary overload of calcium and phosphorus is associated with low trabecular volume in uremic rats Batista, Daniella Guimarães 17 January 2011 (has links) As alterações do metabolismo mineral ocorrem precocemente nos pacientes com doença renal e podem interferir na formação, reabsorção e mineralização óssea comprometendo a integridade do esqueleto. Recentemente demonstramos que animais com sobrecarga de fósforo desenvolvem lesões ósseas semelhantes à osteoporose. O controle da hiperfosfatemia se faz com restrição de fósforo na dieta, e com o uso de quelantes. Um dos quelantes mais utilizados são os sais de cálcio. Estudos demonstraram que o uso desses quelantes favorece a progressão de calcificações arteriais nos pacientes com doença renal crônica. O objetivo desse estudo foi avaliar o efeito isolado do cálcio e do cálcio/fósforo no tecido ósseo e cardiovascular de ratos urêmicos submetidos a nefrectomia 5/6 (Nx) e paratireoidectomia (PTX),variando o conteúdo de cálcio e de cálcio/fósforo na dieta desses animais. Os níveis de paratormônio (PTH) foram restaurados com implante de mini-bombas osmóticas para infusão do 1-34 PTH de rato na dose de 0.022 g/100 g/h (fisiológica), ou de veículo (2% cisteina). Imediatamente após a Nefrectomia ou Sham Nx, os animais foram divididos em grupos de acordo com a dieta que continha Ca/P: 0,7%(Grupo Sham), Ca 1,2% (Grupo Nx RCa) e Ca/P: 1,2%/ 1,2% (Grupo Nx RCa/P). Após 2 meses, os animais foram sacrificados e foram realizadas as análises bioquímicas e histomorfométricas. Os animais nefrectomizados desenvolveram doença renal moderada, elevação da pressão arterial, assim como hiperfosfatemia, enquanto que apenas os animais Nx RCa/P cursaram com hipocalcemia. A infusão de 1-34 PTH foi efetiva, e os animais Nx RCa/P cursaram com elevação do FGF 23 e diminuição do calcitriol. Os animais que ingeriram dieta RCa e RCa/P apresentaram diminuição do volume trabecular (BV/TV), com diminuição dos parâmetros de formação(OS/BS e Ob.S/BS). Os animais que ingeriram dieta rica em cálcio e em cálcio/fósforo apresentaram maior apoptose de osteoblastos. A expressão gênica da TRAP foi maior nos animais Nx. Não detectamos calcificação vascular no tecido cardíaco e aorta dos animais. Em conclusão a sobrecarga de cálcio e de cálcio/fósforo associada à infusão fisiológica de PTH levam a diminuição do volume ósseo de animais urêmicos, conseqüente ao aumento da apoptose dos osteoblastos levando menor formação óssea; assim como maior atividade dos osteoclastos avaliada pela TRAP e não promoveu calcificação vascular nestes animais. O modelo animal que utilizamos reflete condições clínicas encontradas em pacientes com DRC / Bone and mineral metabolism disturbances occur early in patients with chronic kidney disease (CKD) and may interfere in bone formation, resorption or mineralization, compromising skeletal integrity. We previously have shown that phosphate (P) overload in uremic rats leads to decreased bone volume. In the clinical setting, the therapy for hyperphosphatemia includes dietary P restriction, as well as P binders, including calcium (Ca) salts. Previous studies have shown that Ca-based P binders favor the progression of vascular calcification in CKD patients. The current study evaluated the isolated effect of Ca or Ca and P overload on bone and cardiovascular tissues from uremic rats that were submitted to 5/6 nephrectomy (Nx) and parathyroidectomy (PTx), manipulating the Ca and P content in their diets. Parathormone (PTH) serum levels were kept in a normal range using miniosmotic pumps delivering rat 1-34 PTH or using vehicle. After Nx, animals were divided into three groups according to the diet: 0.7% Ca, 0.7% P (Sham Group); 1.2% Ca, 0.7% P (Nx HCa Group) and 1.2% Ca, 1.2% P (Nx HCa/P Group). After two months, animals were killed and biochemical and histomorphometric analyses were performed. Nx animals developed moderate CKD, arterial hypertension, as well as hyperphosphatemia, whereas only Nx HCa/P animals showed hypocalcemia. Osmotic infusion of PTH was effective, as confirmed by serum PTH levels. Nx HCa/P animals showed elevated serum FGF 23, as well as decreased serum calcitriol. Animals that were submitted to Ca or Ca/P overload showed decrease trabecular volume and a reduction in bone formation parameters, such as osteoid and osteoblastic surfaces. A significant increase in osteoblast apoptosis was seen in Nx HCa and Nx HCa/P Groups. The TRAP expression was higher in Nx animals. We could not observe vascular calcification in these animals. In conclusion, Ca or Ca/P overload associated with physiologic PTH infusion was associated with lower bone volume in uremic animals, explained by a increased osteoblastic apoptosis leads to decreased bone formation, and increased osteoclastic activity assessed by TRAP. This model resembles clinical conditions that are commonly observed in CKD patients Apoptose Apoptosis Calcificação vascular Falência renal crônica Hipercalcemia Hiperfosfatemia Hormônio paratireóideo Hypercalcemia Hyperphosphatemia Kidney failure chronic Osteodistrofia renal Parathyroid hormone Ratos Wistar Renal steodystrophy Vascular calcification Wistar rats
42	Rôle du monoxyde d'azote dans la calcification vasculaire et la rigidité artérielle dans un modèle d'hypertension systolique isolée Gilbert, Liz-Ann 12 1900 (has links) L’hypertension systolique isolée (HSI) est le résultat de changements au niveau de la paroi vasculaire qui ont pour conséquence d’augmenter la rigidité artérielle. Ces modifications surviennent surtout au niveau des grosses artères comme l’aorte et sont associées au vieillissement. La fragmentation des fibres élastiques, leur calcification (élastocalcinose) et la fibrose font partie des changements majeurs observés avec l’âge. En plus de ces changements, le vieillissement vasculaire provoque des modifications au niveau des cellules qui composent la paroi. Les cellules endothéliales sécrètent moins de monoxyde d’azote (NO) provoquant une dysfonction endothéliale et les cellules musculaires lisses vasculaires (CMLVs) synthétisent maintenant des protéines matricielles et osseuses. Situé entre le sang et les CMLVs, l’endothélium contrôle le tonus vasculaire par la sécrétion de plusieurs substances vasoactives qui interagissent entre elles afin de maintenir l’homéostasie du système vasculaire. Parmi celles-ci, on note l’endothéline (ET), un puissant vasoconstricteur et le NO, un gaz vasorelaxants. Ce dernier est aussi reconnu pour bloquer la production d’ET par un mécanisme dépendant du guanosine monophosphate cyclique (GMPc). Comme il y a une interaction entre le NO et l’ET, et que cette dernière est impliquée dans la calcification artérielle, le NO pourrait être impliqué dans la modulation de l’élastocalcinose et de la rigidité artérielle par l’inhibition de l’ET et la modification de la composition de la paroi. Cet effet, qui se produirait au delà des effets vasorelaxants du NO, offre un potentiel thérapeutique intéressant pour l’HSI. Afin d’évaluer l’implication du NO dans la calcification vasculaire et la rigidité artérielle, un modèle animal d’HSI a été utilisé (modèle warfarine vitamine K, WVK). Ce modèle d’élastocalcinose est basé sur l’inhibition de la maturation d’une protéine anti-calcifiante, la matrix Gla protein (MGP), par la warfarine. Afin de déterminer l’implication physiologique du NO dans l’initiation et la progression de l’élastocalcinose, sa production a été inhibée par un analogue de la L-arginine, le L-NG-nitroarginine methyl ester (L-NAME). Lors des processus d’initiation de la calcification, le L-NAME a prévenu l’élastocalcinose sans toutefois modifier la vitesse de l’onde de pouls (PWV). Suite au traitement L-NAME, l’expression de la NO synthase inductible (iNOS) a été diminuée alors qu’elle a été augmentée lors du traitement WVK. Elle pourrait donc être impliquée dans les processus de calcification vasculaire. De plus, la NO synthase endothéliale (eNOS) semble également impliquée puisqu’elle a été augmentée dans le modèle WVK. Cette hausse pourrait être bénéfique pour limiter l’élastocalcinose alors que l’expression de la iNOS serait délétère. Lors de la progression de la calcification, le L-NAME a augmenté l’élastocalcinose et le PWV. Dans ce contexte, l’ET serait impliquée dans l’amplification de la calcification vasculaire entrainant une hausse de la rigidité artérielle. Comme le NO endogène limite la progression de la calcification et conséquemment la rigidité artérielle, il semble être protecteur. L’efficacité d’une modulation de la voie du NO dans le modèle WVK a été étudiée par l’administration d’un donneur de NO, le sinitrodil, ou d’un inhibiteur de la phosphosdiestérase 5 (PDE5), le tadalafil. La modulation de la voie du NO semble être bénéfique sur la rigidité artérielle, mais seulement de façon aiguë. En effet, le sinitrodil a modifié de transitoirement la rigidité au niveau de l’aorte possiblement par la modulation du tonus vasculaire sans toutefois avoir des effets sur la composition de la paroi. Comme le modèle WVK n’affecte pas la fonction endothéliale, les concentrations endogènes de NO semblent être optimales puisque le sinitrodil provoque une augmentation de l’élastocalcinose possiblement par le développement d’une tolérance. Tout comme le sinitrodil, le tadalafil a modulé de manière aiguë la rigidité artérielle sans modifier la composition de la paroi. Globalement, ces travaux ont permis de mettre en évidence les effets bénéfiques du NO endogène pour limiter le développement de l’HSI, suggérant qu’une dysfonction endothéliale, tel qu’observé lors du vieillissement, a un impact négatif sur la maladie. / Isolated systolic hypertension (ISH) is the result of complex changes in the vascular wall and consequently the increase of arterial stiffness. These modifications occur mainly in conductance arteries, like the aorta, and are associated with aging. The fragmentation of elastic fibers, calcification (elastocalcinosis), and fibrosis are major changes with age. In addition to these changes in the extracellular matrix, vascular aging also induces vascular cell wall modifications. These include decreased production of nitric oxide (NO) by endothelial cells, which induces endothelial dysfunction, and the production of matrix and bone proteins by vascular smooth muscle cells (VSMCs). Located between the blood and VSMCs, the endothelium controls vascular tone by secreting various vasoactive factors. These factors interact with each other to maintain the hemodynamic of the vascular system. Among these factors, the vasoconstrictor endothelin (ET) and the vasodilator NO. The latter has been shown to block ET production via a cyclic guanosine monophosphates-(cGMP) dependent mechanism, whereas ET has been implicated in arterial calcification. Therefore, NO might be involved in the modulation of elastocalcinosis and arterial stiffness by inhibiting ET and modifying the vascular wall composition. This effect of NO could offer interesting therapeutic potential for ISH. To evaluate the implication of NO in the vascular calcification and arterial stiffness, an animal model of ISH was used. This model of elastocalcinosis is based on the inhibition of the maturation of the anti-calcific protein, matrix Gla protein (MGP), by warfarin (WVK model). To gain insight into the physiological role of endogenous NO in the initiation and progression of elastocalcinosis, its production was inhibited by the administration of L-NAME. Interestingly, elastocalcinosis was prevented by L-NG-nitroarginine methyl ester (L-NAME) administration without any modifications of the pulse wave velocity (PWV) during the initiation of the calcification processes. After the L-NAME treatment, the expression of inducible NO synthase (iNOS) was decreased, whereas upon treatment with warfarin alone the expression of iNOS was increased, which could be implicated in vascular calcification and arterial stiffness. In addition, endothelial NO synthase (eNOS) seems to be implicated in this process as its expression was also increased upon WVK treatment. This increase could be beneficial to limit elastocalcinosis, whereas the increase in iNOS expression could be harmful. L-NAME administration during the progression of calcification increased elastocalcinosis and PWV. In an endothelial dysfunction context, ET has been shown to be involved in the amplification process of vascular calcification causing an increase in arterial stiffness. As NO limits the progression of calcification and consequently arterial stiffness, endogenous NO seems to be protective in the aorta. The efficacy of exogenous modulation of the NO pathway in the WVK model was studied upon administration of the NO donor, sinitrodil, or the phosphodiesterase type 5 inhibitor (PDE5), tadalafil. The exogenous modulation of the NO pathway seemed to be beneficial for arterial stiffness, but only in an acute manner. Indeed, sinitrodil modified the acute stiffness in the aorta potentially by vascular tone modulation, without having any effect on vascular wall composition. Since endothelial function was not affected upon WVK model, endogenous NO concentrations seem to be optimal. Thus, exogenous NO potentially caused an increase of elastocalcinosis by inducing tolerance to NO. As well as sinitrodil, tadalafil modulated the arterial stiffness in an acute manner without modifying the composition of the vascular wall. Broadly, these studies provide evidence that endogenous NO can limit ISH development, suggesting that endothelial dysfunction, as observed in aging, has a negative impact on this pathology. monoxyde d’azote rigidité artérielle donneurs de NO inhibiteur de phosphodiestérases calcification vasculaire hypertension systolique isolée vitesse de l’onde de pouls nitric oxide aortic stiffness phosphodiesterase inhibitors NO donors vascular calcification isolated systolic hypertension pulse wave velocity
43	Mecanismos fisiopatológicos do remodelamento vascular associado à calcificação em camundongos com obesidade e resistência à insulina / Mechanisms of vascular remodeling associated with calcification in obesity and insulin resistance Carmo, Luciana Simão do 12 December 2017 (has links) O remodelamento vascular é uma resposta adaptativa a estímulos específicos, participando da fisiopatologia de diversas doenças cardiovasculares. Devido à intersecção de fatores de risco cardiovasculares relacionados tanto ao remodelamento vascular como à calcificação vascular (CV), propomos a investigação de mecanismos que inter-relacionam tais condições. Postulamos que camundongos ob/ob com obesidade e resistência à insulina têm resposta exacerbada de remodelamento vascular associado à CV quando comparado aos camundongos controles C57BL/6 (C57) após estímulo com vitamina D3 (VD) in vivo. Camundongos C57 e ob/ob (OB) machos foram injetados com 8x103 UI/kg de vitamina D3 intraperitoneal (IP) ou solução fisiológica (CT) durante 14 dias (n=6). Houve aumento da circunferência da lâmina elástica externa da aorta, determinando aumento da área circunferencial do vaso em camundongos OBVD. A hipervitaminose D aumentou o comprimento da lâmina elástica interna da aorta, aumentando o lúmen vascular em camundongos OBVD. Ocorreu também diminuição da espessura da parede do vaso em camundongos OBVD, caracterizando remodelamento vascular positivo hipotrófico. Observamos ainda maior deposição de colágeno na parede do vaso e elastólise em camundongos OBVD. O remodelamento vascular positivo em camundongos OBVD se correlacionou diretamente com o aumento da calcificação na aorta (R2=0,8; p < 0,003). Aortas de camundongos OBVD apresentaram aumento na expressão de espécies reativas de oxigênio (ERO), que foi associado a aumento da atividade de metaloproteinases de matriz (MMP). Estes resultados fornecem evidências que camundongos obesos, insulino-resistentes, e com diabetes tipo 2 desenvolveram remodelamento vascular positivo hipotrófico correlacionado diretamente com calcificação vascular em camundongos OBVD após estímulo com vitamina D3. O desenvolvimento de remodelamento vascular positivo hipotrófico neste modelo murino é possivelmente mediado pela ativação de MMP na parede da aorta e a geração de ERO pode ter contribuído para a ativação de MMP no nosso modelo / Vascular remodeling is a vessel response to mechanical and hemodynamic stimuli, which is a major determinant of changes in vessel lumen caliber. The mechanisms that influence arterial remodeling include calcification. We hypothesized that ob/ob mice develop positive vascular remodeling associated with calcification. We quantify and assess mechanisms of vascular remodeling and vascular calcification in ob/ob mice (OB) after vitamin D3 stimulation (VD) or phosphate buffered saline (CT), compared with (C57BL/6) mice. Both ob/ob (OBVD) and C57BL/6 (C57VD) mice received 8x103 IU/day of (IP) vitamin D3 for 14 days. Control ob/ob (OBCT) and C57BL/6 (C57CT) mice received IP phosphate buffered saline (PBS) for 14 days (n=6). Hypervitaminosis D increased the external and internal elastic length in aortas from OB mice, resulting in increased total vascular area and lumen vascular area respectively, which characterizes positive vascular remodeling. OBVD mice decreased the aortic wall thickness, resulting in hypotrophic vascular remodeling. We demonstrated increases in collagen deposition, elastolysis and calcification in the aortas of OBVD mice. These results showed a positive correlation between expansive vascular remodeling and vascular calcification in OBVD mice (R2=0,8; p < 0,003). Furthermore, aorta from OBVD increased oxidative stress, coincidently with augmented metalloproteinase activity. Our data provide evidence that obese type 2 diabetes mellitus and insulin-resistant mice (ob/ob) developed positive hypotrophic vascular remodeling correlated directly with increased vascular calcification in OBVD mice after chronic vitamin D3 stimulation. The development of positive hypotrophic vascular remodeling in this mouse model is possibly mediated by the activation in the aortic wall of MMP and ROS may have contributed to the activation of MMP in our model Calcificação vascular Camundongos obesos Colecalciferol Diabetes mellitus tipo 2 Diabetes mellitus type 2 Estresse oxidativo Insulin resistance Metaloproteinases da matriz Mice Obese Obesidade Obesity Oxidative stress Remodelação vascular Resistência à insulina Vacular remodeling Vascular calcification
44	Avaliação do efeito isolado do fósforo e do paratormônio sobre o tecido cardíaco de ratos urêmicos paratireoidectomizados / Evaluation of the isolated effect of phosphorus and parathyroid hormone on the cardiac tissue of parathyroidectomized uremic rats Custódio, Melani Ribeiro 13 December 2007 (has links) A doença cardiovascular (DCV) é a principal causa de mortalidade nos pacientes com doença renal crônica (DRC) e a hipertrofia de ventrículo esquerdo (HVE), a alteração mais freqüente. A remodelação cardíaca (RC) patológica ocorre em resposta a agressões como sobrecarga de volume ou de pressão e é influenciada por ativação neurohormonal, fatores locais, inflamação, isquemia, necrose e apoptose celular. Os miócitos são as principais células envolvidas na RC. Avaliamos o papel da hiperfosfatemia e do paratormônio (PTH) em animais urêmicos. Trinta e dois ratos Wistar machos foram submetidos à paratireoidectomia (PTX) e nefrectomia (Nx), com reposição contínua de PTH em concentração fisiológica (PTHf= 0,022 ug/100g/h) ou elevada (PTHe=0,11 ug/100g/h). Os animais sham (N=16) foram operados e recebiam infusão de veículo. Apenas o conteúdo de fósforo nas dietas era diferente, ou seja: pobre=0,2% (pP) ou rica em fósforo=1,2% (rP). Dividimos os animais em 6 grupos: Sham: Sham-pP (G1), Sham-rP (G2); PTX+Nx: PTHf-pP (G3), PTHf-rP (G4), PTHe-pP (G5), PTHe-rP (G6). Semanalmente determinamos o peso e a pressão arterial caudal. Creatinina, fósforo, cálcio PTH e hematócrito foram analisados. Após 8 semanas os animais foram sacrificados. A hipertrofia e fibrose miocárdicas foram analisadas com o sistema digital Leica. O peso do coração corrigido por 100g peso corporal foi maior nos grupos G5 e G6 e apresentou uma correlação positiva com hipertrofia e fibrose miocárdica. A hipertrofia e fibrose foram menores no G3, quando comparado aos grupos Nx. A hipertrofia miocárdica foi maior no G6, evidenciando o papel do P neste processo. A fibrose mocárdica ocorreu principalmente em subendocárdio e foi mais intensa no G6. Analisamos a expressão do fator transformador de crescimento (TGF-beta) e angiotensina II que foram mais intensas nos grupos G5 e G6. As lesões das artérias coronarianas foram avaliadas de forma semi-quantitativa e os animais G5 e G6 mostraram calcificações de camada média. A expressão da alfa-actina se correlacionou negativamente com as lesões coronarianas. Nossos resultados demonstraram a importância do fósforo e PTH na fisiopatologia da DCV, sendo necessário um melhor controle destes elementos para prevenção de mortalidade nos pacientes com DRC. / Cardiovascular disease (CVD) is the leading cause of mortality in patients with chronic kidney disease (CKD), and left ventricular hypertrophy (LVH) is the most common alteration. Pathologic cardiac remodeling (CR) occurs in response to injuries such as volume or pressure overload, and it is influenced by neurohormonal activation, local factors, inflammation, ischemia, necrosis and cellular apoptosis. Myocytes are the principal cells involved in CR. We evaluated the role of hyperphosphatemia and parathyroid hormone (PTH) in uremic animals. Thirty-two male Wistar rats were submitted to parathyroidectomy (PTX) and nephrectomy (Nx), with PTH continuous replacement in physiologic concentration (PTHf=0.022ug/100g/h) or elevated (PTHe=0.11ug/100g/h). The sham animals (N=16) were operated and received vehicle infusion. Only the phosphorus content in diets was different, that is: poor = 0.2% (pP) or rich in phosphorus = 1.2% (rP). We divided the animals into 6 groups: Sham: Sham-pP (G1), Sham-rP (G2); PTX+Nx: PTHf-pP (G3), PTHf-rP (G4), PTHe-pP (G5), PTHe-rP (G6). We determined the weight and caudal blood pressure weekly. Creatinine, phosphorus, PTH calcium and hematocrit were analyzed. After 8 weeks, the animals were sacrificed. Myocardial hypertrophy and fibrosis were analyzed using Leica digital system. The weight of the heart corrected for 100g body weight was greater in groups G5 and G6 and presented a positive correlation with myocardial hypertrophy and fibrosis. Hypertrophy and fibrosis were lower in G3, when compared to Nx groups. Myocardial hypertrophy was higher in G6, determining the role of P in this process. Myocardial fibrosis occurred mainly in subendocardium and was more intense in G6. We analyzed the expression of transforming growth factor (TGF-alfa) and angiotensin II, which were more intense in groups G5 and G6. Coronary artery lesions were evaluated semiquantitatively and G5 and G6 animals showed middle layer calcifications. Expression of alfa-actin correlated negatively with coronary lesions. Our results demonstrated the importance of phosphorus and PTH in the pathophysiology of CVD; therefore, a better control of these elements is required in order to prevent mortality in patients with CKD. Angiotensin II Angiotensina II Calcificação vascular. Cardiac remodeling Cardiovascular disease Doença cardiovascular Fibrose Fibrosis Hiperfosfatemia Hipertrofia de ventrículo esquerdo Hyperphosphatemia Left ventricular hypertrophy Parathyroid hormone Paratormônio Remodelação cardíaca Vascular calcification.
45	Efeito do carbonato de cálcio e do carbonato de sevelamer na remodelação óssea e na calcificação arterial em um modelo experimental de uremia com doença óssea adinâmica / Effects of calcium carbonate and sevelamer carbonate in bone remodeling and arterial calcification in a model of experimental uremia with adynamic bone disease Ferreira, Juliana Cunha 12 April 2013 (has links) INTRODUÇÃO: Há poucos modelos experimentais de doença óssea adinâmica (DOA) e os mecanismos fisiopatológicos dessa doença não são completamente compreendidos. Além disso, os efeitos dos quelantes de fósforo (P) na DOA têm sido pouco estudados. Este estudo objetivou estabelecer um modelo de DOA e avaliar os efeitos da terapia com carbonato de cálcio (Ca) e carbonato de sevelamer (sevelamer) sobre os distúrbios do metabolismo mineral e ósseo da doença renal crônica (DMO-DRC), no modelo estabelecido. MÉTODOS: Experimento 1: A DOA e a DRC foram induzidas por nefrectomia 5/6 (Nx) e paratireoidectomia (PTx) em ratos Wistar, que após a cirurgia foram divididos em 2 grupos: Nx+PTx e sham (sham Nx+PTx). Experimento 2: ratos Wistar foram submetidos à Nx e à PTx e após a cirurgia, foram divididos em outros 2 grupos: Nx+PTx+Ca (CaCO3 a 3%); Nx+PTx+Sev (sevelamer a 3%). A dieta de todos os animais após a cirurgia foi rica em P (1,2%) à base de grãos, exceto o grupo sham, que recebeu dieta padrão com 0,6% de P. Após oito semanas, os animais foram sacrificados. Foram realizadas análises bioquímicas, ósseas e de calcificação vascular. RESULTADOS: Experimento 1: A Nx e a PTx foram efetivas, confirmadas pela elevação da creatinina, com diminuição do clearance de creatinina e dos níveis de cálcio iônico, nos animais Nx+PTx comparados aos animais sham. O modelo foi eficaz na indução da DOA, confirmada pela diminuição do turnover ósseo nos animais Nx+PTx, comparados ao grupo sham. Experimento 2: A terapia com quelantes de P não alterou o P sérico, mas reduziu a fração de excreção de P (FeP). A diminuição dos níveis de FGF-23 e PTH nos animais Nx+PTx foram independentes da terapia com quelantes e não houve diferença nos valores entre os grupos. A esclerostina sérica não foi diferente entre os grupos, mas os animais Nx+PTx+Sev apresentaram menor expressão gênica de SOST e menor taxa de apoptose de osteócitos que os outros grupos. Ambos os quelantes de P diminuíram a expressão gênica do Dickkopf-1 e do fator de crescimento ?1 (TGF-?1). Os animais Nx+PTx+Ca apresentaram maior superficie de reabsorção e maior conteúdo de Ca do ventrículo esquerdo (VE) que os animais Nx+PTx, enquanto os animais Nx+PTx+Sev mostraram diminuição do conteúdo de Ca de VE, comparado aos demais grupos. CONCLUSÕES: o modelo experimental desenvolvido é útil para o estudo da DRC com DOA. A FeP parece ser parâmetro mais fidedigno que o P sérico para avaliar o poder dos quelantes de P. A diminuição do FGF-23 esteve relacionada à diminuição dos níveis de PTH e à hipocalcemia. Os animais tratados com Ca apresentaram sobrecarga desse elemento, traduzida por maior calciúria, maior conteúdo de cálcio de VE e maior superfície de reabsorção óssea. Os mecanismos subjacentes à ação do sevelamer na diminuição da expressão da SOST foram independentes do PTH, do P séricos, da função renal e da expressão gênica de TGF-?1. Mais estudos são necessários para melhor compreensão desses mecanismos / INTRODUCTION: There are few experimental models of adynamic bone disease (ABD) and the pathophysiology of this disease is not fully understood. In addition, the effects of different phosphate (P) binders on ABD have not been evaluated. This study aimed to establish a model of ABD and evaluate the effects of therapy with calcium carbonate (Ca) and sevelamer carbonate (sevelamer) on disorders of bone and mineral metabolism in chronic kidney disease (CKD-MBD), on the established model. METHODS: Experiment 1: ABD and CKD were induced by 5/6 nephrectomy (Nx) and parathyroidectomy (PTx) in Wistar rats, which after surgery, were divided into 2 groups: Nx+PTx and sham (sham Nx+PTx). Experiment 2: Wistar rats underwent Nx and PTx and after surgery were divided into 2 more groups: Nx+PTx+Ca(3% Ca-treated) and Nx+PTx+Sev (3% Sev-treated). All animals were fed a high P (1.2%), grain-based diet, except the sham group which was fed a standard P (0,6%) diet. After 8 weeks, the animals were sacrificed. Biochemical, bone and vascular calcification analyses were performed. RESULTS: Experiment 1: Nx and PTx were effective, confirmed by higher creatinina with decreased creatinine clearance and decreased ionized calcium levels respectively, in Nx+PTx animals compared to sham animals. The model was effective in inducing ABD confirmed by decreased bone turnover in animals Nx+PTx compared to sham group. Phosphate binders administration did not change serum P, but decreased the fractional excretion of phosphate (FeP) in treated animals. FGF-23 and PTH levels were reduced in all Nx+PTx animals independent of the therapy with P binders and these levels were not different among groups. Serum sclerostin was not different among groups, however, Nx+PTx+Sev animals had lower SOST gene expression and lower osteocytes apoptotic rate than the other animals. Both P binders decreased Dickkopf-1 and transforming growing factor ?1 (TGF-?1) gene expression. Nx+PTx+Ca animals showed higher eroded surface and higher left ventricle (LV) calcium content than Nx+PTx animals, whereas Nx+PTx+Sev animals showed a decrease in LV calcium content, compared to the other groups. CONCLUSIONS: This experimental model is useful to study CKD with ABD. The FeP seems to be a more reliable parameter than serum P to evaluate the effectiveness of P binders. Decreased FGF-23 levels were related to decreased PTH levels and hypocalcemia. Ca-treated animals showed Ca overload, as seen by higher calciuria, higher LV calcium content and higher eroded surface. The underlying mechanisms involved in sevelamer actions of decreased SOST expression were independent of PTH, serum P, renal function and TGF-?1 gene expression. Further studies are needed to a better understanding of these mechanisms Apoptose Apoptosis Calcificação vascular Cálcio Calcium Chelating agents Expressão gênica Fósforo Gene expression Insuficiência renal crônica Modelos animais Models animal Osteodistrofia renal Phosphorus Quelantes Renal insufficiency chronic Renal osteodystrophy Vascular calcification
46	Integração do estudo anatômico coronariano através da angiotomografia/escore de cálcio ao estudo funcional de perfusão miocárdica pelo PET-CT utilizando rubídio na investigação da doença arterial coronariana / Integration of the coronary anatomy study through angiotomography/coronary artery calcium score to the functional study of myocardial perfusion by PET-CT using rubidium in the investigation of coronary artery disease Fahel, Mateus Guimarães 20 October 2017 (has links) Introdução: A doença arterial coronariana (DAC) persiste com alta morbimortalidade. Várias modalidades diagnósticas não-invasivas estão disponíveis para sua avaliação, incluindo escore de cálcio coronariano (EC), angiotomografia coronariana (AngioTC) e tomografia por emissão de pósitrons com rubídio (PET-CT82Rb), com ótimas sensibilidade e especificidade. A integração destes métodos em um exame híbrido permite delinear extensão anatômica e funcional da aterosclerose, possibilitando diagnósticos mais corretos. Objetivo: Avaliar anatomia coronariana e perfusão miocárdica de pacientes suspeitos ou portadores de DAC com tecnologia híbrida (PETCT82Rb e AngioTC/EC), testando a hipótese da maior acurácia do método híbrido em relação aos métodos isolados, correlacionando com desfecho de IAM/óbito cardíaco após 24 meses. Métodos: Foram incluídos 54 pacientes dos ambulatórios de cardiologia do Instituto do Coração (InCor-HCFMUSP), que realizaram estudo híbrido no departamento de Medicina Nuclear do InCor entre maio e outubro de 2013. A carga aterosclerótica coronariana foi contabilizada pelo escore de cálcio; a quantidade de lesões coronarianas, o grau de redução luminal e a composição das placas foram avaliados através da AngioTC; isquemia/fibrose pelo PET-CT82Rb foi contabilizada através do SDS (summed difference score) do estresse e repouso e a reserva de fluxo coronariana (RFC) foi considerada reduzida quando menor que 2mL/min/g. Após 24 meses, foi realizado contato telefônico e avaliação do prontuário dos pacientes, sendo pesquisado infarto agudo do miocárdio/óbito cardíaco como desfecho clínico principal. Resultados: Dentre os participantes, houve predomínio de homens (61,3%), com idade média de 55,5 ± 12,3 anos. A maioria apresentava sobrepeso/obesidade (76%), hipertensão arterial sistêmica (70,4%) e/ou dislipidemia (61,1%). O protocolo durou uma média de 52,2 ± 3,5 min e a dose total média de radiação foi 12,29 ± 2,88 mSv. A média do EC total foi 127,3 ± 249,0, sendo que 24% da amostra possuíam EC maior que 100. Houve predomínio de placas de ateroma mistas (51,3%), com 13% dos pacientes apresentando lesões angiograficamente significativas ( >= 50%). Oito pacientes apresentaram resultado alterado na análise perfusional qualitativa/semiquantitativa (14,8%), metade com isquemia e metade com fibrose. A RFC estava reduzida globalmente em 18,5% dos pacientes e de forma segmentar em 5,6%. Após 24 meses, 9,3% dos pacientes apresentaram infarto, 60% destes fatais. Houve concordância no máximo moderada dos métodos avaliados com a RFC (Kappa = 0,514; p= 0,001). Quanto ao desempenho dos métodos para ocorrência de IAM em 24 meses, foi demonstrada elevada acurácia da RFC para tal finalidade, com AUROC de 0,963 (IC95% 0,912 - 1,000; p= 0,001), com melhor ponto de corte de 1,975 mL/min/g. Não foi identificada alteração na sensibilidade ou no valor preditivo negativo quando a RFC foi agregada aos outros métodos, inclusive houve redução do valor preditivo positivo e da especificidade em relação à RFC isoladamente. Conclusão: O método híbrido não apresentou maior acurácia que a RFC pelo PET-CT82Rb isoladamente na predição de IAM em dois anos de acompanhamento, todavia, a tomografia cardíaca agrega informações importantes capazes de influenciar a conduta clínica nos pacientes não isquêmicos e possivelmente modifica desfechos em médio/longo prazo / Introduction: Coronary artery disease (CAD) persists with high morbidity and mortality. Several non-invasive diagnostic imaging modalities are available for its evaluation, including coronary calcium score (CS), coronary CT angiography (AngioCT) and positron emission tomography with rubidium (82Rb PET-CT), with excellent sensitivity and specificity. The integration of these methods into a hybrid examination allows delineating the anatomical and functional impact of atherosclerosis, enabling more accurate diagnoses. Objective: To evaluate coronary anatomy and myocardial perfusion of patients with suspected or known CAD with hybrid technology (82Rb PET-CT and AngioCT/CS), testing the hypothesis of the greater accuracy of the hybrid method in relation to the isolated methods, correlating with myocardial infarction/cardiac death outcome after 24 months. Methods: Fifty-four consecutive patients referred from the Cardiology outpatient clinics of the Heart Institute (InCor-HCFMUSP) to perform CAD assessment in a hybrid study in the Department of Nuclear Medicine of InCor, between May and October 2013, were enrolled. The coronary atherosclerotic burden was accounted by CS; the amount of coronary lesions, stenosis severity and plaque composition were evaluated through AngioCT; 82Rb PET-CT perfusional analysis was evaluated through the rest and dipyridamole stress summed difference score (SDS) and the coronary flow reserve (CFR) was considered impaired when < 2mL/min/g. After 24 months, the composite outcome of myocardial infarction and cardiac death was evaluated through telephone contact and patient\'s medical records. Results: From the 54 enrolled patients, mean age was 55.5 ± 12.3 years and 61% were male. Most patients presented overwheight/obesity (76%), systemic arterial hypertension (70%) and/or dyslipidemia (61%). The protocol lasted an average of 52.2 ± 3,5 min and mean radiation dose was 12.29 ± 2,88 mSv. The mean total CS was 127.3 ± 249.0, and 24% of the patients were above 100. There was a predominance of patients with mixed atheroma plaques (51.3%) and 13% presented angiographically significant lesions ( >= 50%). Eight patients presented perfusion impairment in the qualitative/semi-quantitative perfusion analysis (14.8%), half with ischemia and half with fibrosis. The CFR was globally reduced in 18.5% of the sample and in a segmental manner in 5.6%. After 24 months of follow-up, 9.3% of the patients had a myocardium infarction, 60% of these were fatal. A maximum of moderate agreement was found between the methods and CFR (Kappa = 0.514, p= 0.001). Regarding the performance of the different methods for predicting infarction in 24 months, CFR reached high accuracy, with AUROC of 0.963 (95% CI 0.912 - 1.0; p= 0.001), with a cutoff point of 1.975 mL/min/g. No variation in neither sensitivity nor negative predictive value was identified when the other methods were added to CFR, instead, there was a reduction in positive predictive value and specificity in relation to unaided CFR. Conclusion: There was no incremental value of the hybrid method when compared to isolated CFR 82Rb PET-CT for the prediction of myocardial infarction in two years follow-up. However, cardiac CT aggregates important information capable of influencing clinical management of nonischemic patients and possibly modifies medium/long-term cardiac outcomes Calcificação vascular Computed tomography angiography Coronary artery disease Doença da artéria coronariana Imagem de perfusão do miocárdio Myocardial perfusion imaging Radioisótopos de rubídio Rubidium radioisotopes Vascular calcification
47	Rôle du monoxyde d'azote dans la calcification vasculaire et la rigidité artérielle dans un modèle d'hypertension systolique isolée Gilbert, Liz-Ann 12 1900 (has links) L’hypertension systolique isolée (HSI) est le résultat de changements au niveau de la paroi vasculaire qui ont pour conséquence d’augmenter la rigidité artérielle. Ces modifications surviennent surtout au niveau des grosses artères comme l’aorte et sont associées au vieillissement. La fragmentation des fibres élastiques, leur calcification (élastocalcinose) et la fibrose font partie des changements majeurs observés avec l’âge. En plus de ces changements, le vieillissement vasculaire provoque des modifications au niveau des cellules qui composent la paroi. Les cellules endothéliales sécrètent moins de monoxyde d’azote (NO) provoquant une dysfonction endothéliale et les cellules musculaires lisses vasculaires (CMLVs) synthétisent maintenant des protéines matricielles et osseuses. Situé entre le sang et les CMLVs, l’endothélium contrôle le tonus vasculaire par la sécrétion de plusieurs substances vasoactives qui interagissent entre elles afin de maintenir l’homéostasie du système vasculaire. Parmi celles-ci, on note l’endothéline (ET), un puissant vasoconstricteur et le NO, un gaz vasorelaxants. Ce dernier est aussi reconnu pour bloquer la production d’ET par un mécanisme dépendant du guanosine monophosphate cyclique (GMPc). Comme il y a une interaction entre le NO et l’ET, et que cette dernière est impliquée dans la calcification artérielle, le NO pourrait être impliqué dans la modulation de l’élastocalcinose et de la rigidité artérielle par l’inhibition de l’ET et la modification de la composition de la paroi. Cet effet, qui se produirait au delà des effets vasorelaxants du NO, offre un potentiel thérapeutique intéressant pour l’HSI. Afin d’évaluer l’implication du NO dans la calcification vasculaire et la rigidité artérielle, un modèle animal d’HSI a été utilisé (modèle warfarine vitamine K, WVK). Ce modèle d’élastocalcinose est basé sur l’inhibition de la maturation d’une protéine anti-calcifiante, la matrix Gla protein (MGP), par la warfarine. Afin de déterminer l’implication physiologique du NO dans l’initiation et la progression de l’élastocalcinose, sa production a été inhibée par un analogue de la L-arginine, le L-NG-nitroarginine methyl ester (L-NAME). Lors des processus d’initiation de la calcification, le L-NAME a prévenu l’élastocalcinose sans toutefois modifier la vitesse de l’onde de pouls (PWV). Suite au traitement L-NAME, l’expression de la NO synthase inductible (iNOS) a été diminuée alors qu’elle a été augmentée lors du traitement WVK. Elle pourrait donc être impliquée dans les processus de calcification vasculaire. De plus, la NO synthase endothéliale (eNOS) semble également impliquée puisqu’elle a été augmentée dans le modèle WVK. Cette hausse pourrait être bénéfique pour limiter l’élastocalcinose alors que l’expression de la iNOS serait délétère. Lors de la progression de la calcification, le L-NAME a augmenté l’élastocalcinose et le PWV. Dans ce contexte, l’ET serait impliquée dans l’amplification de la calcification vasculaire entrainant une hausse de la rigidité artérielle. Comme le NO endogène limite la progression de la calcification et conséquemment la rigidité artérielle, il semble être protecteur. L’efficacité d’une modulation de la voie du NO dans le modèle WVK a été étudiée par l’administration d’un donneur de NO, le sinitrodil, ou d’un inhibiteur de la phosphosdiestérase 5 (PDE5), le tadalafil. La modulation de la voie du NO semble être bénéfique sur la rigidité artérielle, mais seulement de façon aiguë. En effet, le sinitrodil a modifié de transitoirement la rigidité au niveau de l’aorte possiblement par la modulation du tonus vasculaire sans toutefois avoir des effets sur la composition de la paroi. Comme le modèle WVK n’affecte pas la fonction endothéliale, les concentrations endogènes de NO semblent être optimales puisque le sinitrodil provoque une augmentation de l’élastocalcinose possiblement par le développement d’une tolérance. Tout comme le sinitrodil, le tadalafil a modulé de manière aiguë la rigidité artérielle sans modifier la composition de la paroi. Globalement, ces travaux ont permis de mettre en évidence les effets bénéfiques du NO endogène pour limiter le développement de l’HSI, suggérant qu’une dysfonction endothéliale, tel qu’observé lors du vieillissement, a un impact négatif sur la maladie. / Isolated systolic hypertension (ISH) is the result of complex changes in the vascular wall and consequently the increase of arterial stiffness. These modifications occur mainly in conductance arteries, like the aorta, and are associated with aging. The fragmentation of elastic fibers, calcification (elastocalcinosis), and fibrosis are major changes with age. In addition to these changes in the extracellular matrix, vascular aging also induces vascular cell wall modifications. These include decreased production of nitric oxide (NO) by endothelial cells, which induces endothelial dysfunction, and the production of matrix and bone proteins by vascular smooth muscle cells (VSMCs). Located between the blood and VSMCs, the endothelium controls vascular tone by secreting various vasoactive factors. These factors interact with each other to maintain the hemodynamic of the vascular system. Among these factors, the vasoconstrictor endothelin (ET) and the vasodilator NO. The latter has been shown to block ET production via a cyclic guanosine monophosphates-(cGMP) dependent mechanism, whereas ET has been implicated in arterial calcification. Therefore, NO might be involved in the modulation of elastocalcinosis and arterial stiffness by inhibiting ET and modifying the vascular wall composition. This effect of NO could offer interesting therapeutic potential for ISH. To evaluate the implication of NO in the vascular calcification and arterial stiffness, an animal model of ISH was used. This model of elastocalcinosis is based on the inhibition of the maturation of the anti-calcific protein, matrix Gla protein (MGP), by warfarin (WVK model). To gain insight into the physiological role of endogenous NO in the initiation and progression of elastocalcinosis, its production was inhibited by the administration of L-NAME. Interestingly, elastocalcinosis was prevented by L-NG-nitroarginine methyl ester (L-NAME) administration without any modifications of the pulse wave velocity (PWV) during the initiation of the calcification processes. After the L-NAME treatment, the expression of inducible NO synthase (iNOS) was decreased, whereas upon treatment with warfarin alone the expression of iNOS was increased, which could be implicated in vascular calcification and arterial stiffness. In addition, endothelial NO synthase (eNOS) seems to be implicated in this process as its expression was also increased upon WVK treatment. This increase could be beneficial to limit elastocalcinosis, whereas the increase in iNOS expression could be harmful. L-NAME administration during the progression of calcification increased elastocalcinosis and PWV. In an endothelial dysfunction context, ET has been shown to be involved in the amplification process of vascular calcification causing an increase in arterial stiffness. As NO limits the progression of calcification and consequently arterial stiffness, endogenous NO seems to be protective in the aorta. The efficacy of exogenous modulation of the NO pathway in the WVK model was studied upon administration of the NO donor, sinitrodil, or the phosphodiesterase type 5 inhibitor (PDE5), tadalafil. The exogenous modulation of the NO pathway seemed to be beneficial for arterial stiffness, but only in an acute manner. Indeed, sinitrodil modified the acute stiffness in the aorta potentially by vascular tone modulation, without having any effect on vascular wall composition. Since endothelial function was not affected upon WVK model, endogenous NO concentrations seem to be optimal. Thus, exogenous NO potentially caused an increase of elastocalcinosis by inducing tolerance to NO. As well as sinitrodil, tadalafil modulated the arterial stiffness in an acute manner without modifying the composition of the vascular wall. Broadly, these studies provide evidence that endogenous NO can limit ISH development, suggesting that endothelial dysfunction, as observed in aging, has a negative impact on this pathology. monoxyde d’azote rigidité artérielle donneurs de NO inhibiteur de phosphodiestérases calcification vasculaire hypertension systolique isolée vitesse de l’onde de pouls nitric oxide aortic stiffness phosphodiesterase inhibitors NO donors vascular calcification isolated systolic hypertension pulse wave velocity
48	Integração do estudo anatômico coronariano através da angiotomografia/escore de cálcio ao estudo funcional de perfusão miocárdica pelo PET-CT utilizando rubídio na investigação da doença arterial coronariana / Integration of the coronary anatomy study through angiotomography/coronary artery calcium score to the functional study of myocardial perfusion by PET-CT using rubidium in the investigation of coronary artery disease Mateus Guimarães Fahel 20 October 2017 (has links) Introdução: A doença arterial coronariana (DAC) persiste com alta morbimortalidade. Várias modalidades diagnósticas não-invasivas estão disponíveis para sua avaliação, incluindo escore de cálcio coronariano (EC), angiotomografia coronariana (AngioTC) e tomografia por emissão de pósitrons com rubídio (PET-CT82Rb), com ótimas sensibilidade e especificidade. A integração destes métodos em um exame híbrido permite delinear extensão anatômica e funcional da aterosclerose, possibilitando diagnósticos mais corretos. Objetivo: Avaliar anatomia coronariana e perfusão miocárdica de pacientes suspeitos ou portadores de DAC com tecnologia híbrida (PETCT82Rb e AngioTC/EC), testando a hipótese da maior acurácia do método híbrido em relação aos métodos isolados, correlacionando com desfecho de IAM/óbito cardíaco após 24 meses. Métodos: Foram incluídos 54 pacientes dos ambulatórios de cardiologia do Instituto do Coração (InCor-HCFMUSP), que realizaram estudo híbrido no departamento de Medicina Nuclear do InCor entre maio e outubro de 2013. A carga aterosclerótica coronariana foi contabilizada pelo escore de cálcio; a quantidade de lesões coronarianas, o grau de redução luminal e a composição das placas foram avaliados através da AngioTC; isquemia/fibrose pelo PET-CT82Rb foi contabilizada através do SDS (summed difference score) do estresse e repouso e a reserva de fluxo coronariana (RFC) foi considerada reduzida quando menor que 2mL/min/g. Após 24 meses, foi realizado contato telefônico e avaliação do prontuário dos pacientes, sendo pesquisado infarto agudo do miocárdio/óbito cardíaco como desfecho clínico principal. Resultados: Dentre os participantes, houve predomínio de homens (61,3%), com idade média de 55,5 ± 12,3 anos. A maioria apresentava sobrepeso/obesidade (76%), hipertensão arterial sistêmica (70,4%) e/ou dislipidemia (61,1%). O protocolo durou uma média de 52,2 ± 3,5 min e a dose total média de radiação foi 12,29 ± 2,88 mSv. A média do EC total foi 127,3 ± 249,0, sendo que 24% da amostra possuíam EC maior que 100. Houve predomínio de placas de ateroma mistas (51,3%), com 13% dos pacientes apresentando lesões angiograficamente significativas ( >= 50%). Oito pacientes apresentaram resultado alterado na análise perfusional qualitativa/semiquantitativa (14,8%), metade com isquemia e metade com fibrose. A RFC estava reduzida globalmente em 18,5% dos pacientes e de forma segmentar em 5,6%. Após 24 meses, 9,3% dos pacientes apresentaram infarto, 60% destes fatais. Houve concordância no máximo moderada dos métodos avaliados com a RFC (Kappa = 0,514; p= 0,001). Quanto ao desempenho dos métodos para ocorrência de IAM em 24 meses, foi demonstrada elevada acurácia da RFC para tal finalidade, com AUROC de 0,963 (IC95% 0,912 - 1,000; p= 0,001), com melhor ponto de corte de 1,975 mL/min/g. Não foi identificada alteração na sensibilidade ou no valor preditivo negativo quando a RFC foi agregada aos outros métodos, inclusive houve redução do valor preditivo positivo e da especificidade em relação à RFC isoladamente. Conclusão: O método híbrido não apresentou maior acurácia que a RFC pelo PET-CT82Rb isoladamente na predição de IAM em dois anos de acompanhamento, todavia, a tomografia cardíaca agrega informações importantes capazes de influenciar a conduta clínica nos pacientes não isquêmicos e possivelmente modifica desfechos em médio/longo prazo / Introduction: Coronary artery disease (CAD) persists with high morbidity and mortality. Several non-invasive diagnostic imaging modalities are available for its evaluation, including coronary calcium score (CS), coronary CT angiography (AngioCT) and positron emission tomography with rubidium (82Rb PET-CT), with excellent sensitivity and specificity. The integration of these methods into a hybrid examination allows delineating the anatomical and functional impact of atherosclerosis, enabling more accurate diagnoses. Objective: To evaluate coronary anatomy and myocardial perfusion of patients with suspected or known CAD with hybrid technology (82Rb PET-CT and AngioCT/CS), testing the hypothesis of the greater accuracy of the hybrid method in relation to the isolated methods, correlating with myocardial infarction/cardiac death outcome after 24 months. Methods: Fifty-four consecutive patients referred from the Cardiology outpatient clinics of the Heart Institute (InCor-HCFMUSP) to perform CAD assessment in a hybrid study in the Department of Nuclear Medicine of InCor, between May and October 2013, were enrolled. The coronary atherosclerotic burden was accounted by CS; the amount of coronary lesions, stenosis severity and plaque composition were evaluated through AngioCT; 82Rb PET-CT perfusional analysis was evaluated through the rest and dipyridamole stress summed difference score (SDS) and the coronary flow reserve (CFR) was considered impaired when < 2mL/min/g. After 24 months, the composite outcome of myocardial infarction and cardiac death was evaluated through telephone contact and patient\'s medical records. Results: From the 54 enrolled patients, mean age was 55.5 ± 12.3 years and 61% were male. Most patients presented overwheight/obesity (76%), systemic arterial hypertension (70%) and/or dyslipidemia (61%). The protocol lasted an average of 52.2 ± 3,5 min and mean radiation dose was 12.29 ± 2,88 mSv. The mean total CS was 127.3 ± 249.0, and 24% of the patients were above 100. There was a predominance of patients with mixed atheroma plaques (51.3%) and 13% presented angiographically significant lesions ( >= 50%). Eight patients presented perfusion impairment in the qualitative/semi-quantitative perfusion analysis (14.8%), half with ischemia and half with fibrosis. The CFR was globally reduced in 18.5% of the sample and in a segmental manner in 5.6%. After 24 months of follow-up, 9.3% of the patients had a myocardium infarction, 60% of these were fatal. A maximum of moderate agreement was found between the methods and CFR (Kappa = 0.514, p= 0.001). Regarding the performance of the different methods for predicting infarction in 24 months, CFR reached high accuracy, with AUROC of 0.963 (95% CI 0.912 - 1.0; p= 0.001), with a cutoff point of 1.975 mL/min/g. No variation in neither sensitivity nor negative predictive value was identified when the other methods were added to CFR, instead, there was a reduction in positive predictive value and specificity in relation to unaided CFR. Conclusion: There was no incremental value of the hybrid method when compared to isolated CFR 82Rb PET-CT for the prediction of myocardial infarction in two years follow-up. However, cardiac CT aggregates important information capable of influencing clinical management of nonischemic patients and possibly modifies medium/long-term cardiac outcomes Calcificação vascular Doença da artéria coronariana Imagem de perfusão do miocárdio Radioisótopos de rubídio Computed tomography angiography Coronary artery disease Myocardial perfusion imaging Rubidium radioisotopes Vascular calcification
49	Efeito do carbonato de cálcio e do carbonato de sevelamer na remodelação óssea e na calcificação arterial em um modelo experimental de uremia com doença óssea adinâmica / Effects of calcium carbonate and sevelamer carbonate in bone remodeling and arterial calcification in a model of experimental uremia with adynamic bone disease Juliana Cunha Ferreira 12 April 2013 (has links) INTRODUÇÃO: Há poucos modelos experimentais de doença óssea adinâmica (DOA) e os mecanismos fisiopatológicos dessa doença não são completamente compreendidos. Além disso, os efeitos dos quelantes de fósforo (P) na DOA têm sido pouco estudados. Este estudo objetivou estabelecer um modelo de DOA e avaliar os efeitos da terapia com carbonato de cálcio (Ca) e carbonato de sevelamer (sevelamer) sobre os distúrbios do metabolismo mineral e ósseo da doença renal crônica (DMO-DRC), no modelo estabelecido. MÉTODOS: Experimento 1: A DOA e a DRC foram induzidas por nefrectomia 5/6 (Nx) e paratireoidectomia (PTx) em ratos Wistar, que após a cirurgia foram divididos em 2 grupos: Nx+PTx e sham (sham Nx+PTx). Experimento 2: ratos Wistar foram submetidos à Nx e à PTx e após a cirurgia, foram divididos em outros 2 grupos: Nx+PTx+Ca (CaCO3 a 3%); Nx+PTx+Sev (sevelamer a 3%). A dieta de todos os animais após a cirurgia foi rica em P (1,2%) à base de grãos, exceto o grupo sham, que recebeu dieta padrão com 0,6% de P. Após oito semanas, os animais foram sacrificados. Foram realizadas análises bioquímicas, ósseas e de calcificação vascular. RESULTADOS: Experimento 1: A Nx e a PTx foram efetivas, confirmadas pela elevação da creatinina, com diminuição do clearance de creatinina e dos níveis de cálcio iônico, nos animais Nx+PTx comparados aos animais sham. O modelo foi eficaz na indução da DOA, confirmada pela diminuição do turnover ósseo nos animais Nx+PTx, comparados ao grupo sham. Experimento 2: A terapia com quelantes de P não alterou o P sérico, mas reduziu a fração de excreção de P (FeP). A diminuição dos níveis de FGF-23 e PTH nos animais Nx+PTx foram independentes da terapia com quelantes e não houve diferença nos valores entre os grupos. A esclerostina sérica não foi diferente entre os grupos, mas os animais Nx+PTx+Sev apresentaram menor expressão gênica de SOST e menor taxa de apoptose de osteócitos que os outros grupos. Ambos os quelantes de P diminuíram a expressão gênica do Dickkopf-1 e do fator de crescimento ?1 (TGF-?1). Os animais Nx+PTx+Ca apresentaram maior superficie de reabsorção e maior conteúdo de Ca do ventrículo esquerdo (VE) que os animais Nx+PTx, enquanto os animais Nx+PTx+Sev mostraram diminuição do conteúdo de Ca de VE, comparado aos demais grupos. CONCLUSÕES: o modelo experimental desenvolvido é útil para o estudo da DRC com DOA. A FeP parece ser parâmetro mais fidedigno que o P sérico para avaliar o poder dos quelantes de P. A diminuição do FGF-23 esteve relacionada à diminuição dos níveis de PTH e à hipocalcemia. Os animais tratados com Ca apresentaram sobrecarga desse elemento, traduzida por maior calciúria, maior conteúdo de cálcio de VE e maior superfície de reabsorção óssea. Os mecanismos subjacentes à ação do sevelamer na diminuição da expressão da SOST foram independentes do PTH, do P séricos, da função renal e da expressão gênica de TGF-?1. Mais estudos são necessários para melhor compreensão desses mecanismos / INTRODUCTION: There are few experimental models of adynamic bone disease (ABD) and the pathophysiology of this disease is not fully understood. In addition, the effects of different phosphate (P) binders on ABD have not been evaluated. This study aimed to establish a model of ABD and evaluate the effects of therapy with calcium carbonate (Ca) and sevelamer carbonate (sevelamer) on disorders of bone and mineral metabolism in chronic kidney disease (CKD-MBD), on the established model. METHODS: Experiment 1: ABD and CKD were induced by 5/6 nephrectomy (Nx) and parathyroidectomy (PTx) in Wistar rats, which after surgery, were divided into 2 groups: Nx+PTx and sham (sham Nx+PTx). Experiment 2: Wistar rats underwent Nx and PTx and after surgery were divided into 2 more groups: Nx+PTx+Ca(3% Ca-treated) and Nx+PTx+Sev (3% Sev-treated). All animals were fed a high P (1.2%), grain-based diet, except the sham group which was fed a standard P (0,6%) diet. After 8 weeks, the animals were sacrificed. Biochemical, bone and vascular calcification analyses were performed. RESULTS: Experiment 1: Nx and PTx were effective, confirmed by higher creatinina with decreased creatinine clearance and decreased ionized calcium levels respectively, in Nx+PTx animals compared to sham animals. The model was effective in inducing ABD confirmed by decreased bone turnover in animals Nx+PTx compared to sham group. Phosphate binders administration did not change serum P, but decreased the fractional excretion of phosphate (FeP) in treated animals. FGF-23 and PTH levels were reduced in all Nx+PTx animals independent of the therapy with P binders and these levels were not different among groups. Serum sclerostin was not different among groups, however, Nx+PTx+Sev animals had lower SOST gene expression and lower osteocytes apoptotic rate than the other animals. Both P binders decreased Dickkopf-1 and transforming growing factor ?1 (TGF-?1) gene expression. Nx+PTx+Ca animals showed higher eroded surface and higher left ventricle (LV) calcium content than Nx+PTx animals, whereas Nx+PTx+Sev animals showed a decrease in LV calcium content, compared to the other groups. CONCLUSIONS: This experimental model is useful to study CKD with ABD. The FeP seems to be a more reliable parameter than serum P to evaluate the effectiveness of P binders. Decreased FGF-23 levels were related to decreased PTH levels and hypocalcemia. Ca-treated animals showed Ca overload, as seen by higher calciuria, higher LV calcium content and higher eroded surface. The underlying mechanisms involved in sevelamer actions of decreased SOST expression were independent of PTH, serum P, renal function and TGF-?1 gene expression. Further studies are needed to a better understanding of these mechanisms Apoptose Calcificação vascular Cálcio Expressão gênica Fósforo Insuficiência renal crônica Modelos animais Osteodistrofia renal Quelantes Apoptosis Calcium Chelating agents Gene expression Models animal Phosphorus Renal insufficiency chronic Renal osteodystrophy Vascular calcification
50	Avaliação do efeito isolado do fósforo e do paratormônio sobre o tecido cardíaco de ratos urêmicos paratireoidectomizados / Evaluation of the isolated effect of phosphorus and parathyroid hormone on the cardiac tissue of parathyroidectomized uremic rats Melani Ribeiro Custódio 13 December 2007 (has links) A doença cardiovascular (DCV) é a principal causa de mortalidade nos pacientes com doença renal crônica (DRC) e a hipertrofia de ventrículo esquerdo (HVE), a alteração mais freqüente. A remodelação cardíaca (RC) patológica ocorre em resposta a agressões como sobrecarga de volume ou de pressão e é influenciada por ativação neurohormonal, fatores locais, inflamação, isquemia, necrose e apoptose celular. Os miócitos são as principais células envolvidas na RC. Avaliamos o papel da hiperfosfatemia e do paratormônio (PTH) em animais urêmicos. Trinta e dois ratos Wistar machos foram submetidos à paratireoidectomia (PTX) e nefrectomia (Nx), com reposição contínua de PTH em concentração fisiológica (PTHf= 0,022 ug/100g/h) ou elevada (PTHe=0,11 ug/100g/h). Os animais sham (N=16) foram operados e recebiam infusão de veículo. Apenas o conteúdo de fósforo nas dietas era diferente, ou seja: pobre=0,2% (pP) ou rica em fósforo=1,2% (rP). Dividimos os animais em 6 grupos: Sham: Sham-pP (G1), Sham-rP (G2); PTX+Nx: PTHf-pP (G3), PTHf-rP (G4), PTHe-pP (G5), PTHe-rP (G6). Semanalmente determinamos o peso e a pressão arterial caudal. Creatinina, fósforo, cálcio PTH e hematócrito foram analisados. Após 8 semanas os animais foram sacrificados. A hipertrofia e fibrose miocárdicas foram analisadas com o sistema digital Leica. O peso do coração corrigido por 100g peso corporal foi maior nos grupos G5 e G6 e apresentou uma correlação positiva com hipertrofia e fibrose miocárdica. A hipertrofia e fibrose foram menores no G3, quando comparado aos grupos Nx. A hipertrofia miocárdica foi maior no G6, evidenciando o papel do P neste processo. A fibrose mocárdica ocorreu principalmente em subendocárdio e foi mais intensa no G6. Analisamos a expressão do fator transformador de crescimento (TGF-beta) e angiotensina II que foram mais intensas nos grupos G5 e G6. As lesões das artérias coronarianas foram avaliadas de forma semi-quantitativa e os animais G5 e G6 mostraram calcificações de camada média. A expressão da alfa-actina se correlacionou negativamente com as lesões coronarianas. Nossos resultados demonstraram a importância do fósforo e PTH na fisiopatologia da DCV, sendo necessário um melhor controle destes elementos para prevenção de mortalidade nos pacientes com DRC. / Cardiovascular disease (CVD) is the leading cause of mortality in patients with chronic kidney disease (CKD), and left ventricular hypertrophy (LVH) is the most common alteration. Pathologic cardiac remodeling (CR) occurs in response to injuries such as volume or pressure overload, and it is influenced by neurohormonal activation, local factors, inflammation, ischemia, necrosis and cellular apoptosis. Myocytes are the principal cells involved in CR. We evaluated the role of hyperphosphatemia and parathyroid hormone (PTH) in uremic animals. Thirty-two male Wistar rats were submitted to parathyroidectomy (PTX) and nephrectomy (Nx), with PTH continuous replacement in physiologic concentration (PTHf=0.022ug/100g/h) or elevated (PTHe=0.11ug/100g/h). The sham animals (N=16) were operated and received vehicle infusion. Only the phosphorus content in diets was different, that is: poor = 0.2% (pP) or rich in phosphorus = 1.2% (rP). We divided the animals into 6 groups: Sham: Sham-pP (G1), Sham-rP (G2); PTX+Nx: PTHf-pP (G3), PTHf-rP (G4), PTHe-pP (G5), PTHe-rP (G6). We determined the weight and caudal blood pressure weekly. Creatinine, phosphorus, PTH calcium and hematocrit were analyzed. After 8 weeks, the animals were sacrificed. Myocardial hypertrophy and fibrosis were analyzed using Leica digital system. The weight of the heart corrected for 100g body weight was greater in groups G5 and G6 and presented a positive correlation with myocardial hypertrophy and fibrosis. Hypertrophy and fibrosis were lower in G3, when compared to Nx groups. Myocardial hypertrophy was higher in G6, determining the role of P in this process. Myocardial fibrosis occurred mainly in subendocardium and was more intense in G6. We analyzed the expression of transforming growth factor (TGF-alfa) and angiotensin II, which were more intense in groups G5 and G6. Coronary artery lesions were evaluated semiquantitatively and G5 and G6 animals showed middle layer calcifications. Expression of alfa-actin correlated negatively with coronary lesions. Our results demonstrated the importance of phosphorus and PTH in the pathophysiology of CVD; therefore, a better control of these elements is required in order to prevent mortality in patients with CKD. Angiotensina II Calcificação vascular. Doença cardiovascular Fibrose Hiperfosfatemia Hipertrofia de ventrículo esquerdo Paratormônio Remodelação cardíaca Angiotensin II Cardiac remodeling Cardiovascular disease Fibrosis Hyperphosphatemia Left ventricular hypertrophy Parathyroid hormone Vascular calcification.

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