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Bath Salts Induced Severe Reversible CardiomyopathySivagnanam, Kamesh, Chaudari, Dhara, Lopez, Pablo, Sutherland, Michael E., Ramu, Vijay K. 08 August 2013 (has links)
Objective: Unusual clinical course Background: "Bath salts" is the street name for a group of recently identified and increasingly abused stimulant synthetic cathinones that are associated with multiple systemic effects. We present a case of a patient who developed reversible dilated cardiomyopathy secondary to their use. Case Report: A 27 year old male with no past medical history was brought to emergency department with agitation. He had been inhaling and intravenously injecting "bath salts", containing a mephedrone/Methylenedioxypyrovalerone (MDPV) combination. On presentation, he was tachycardic, hypotensive and febrile. His initial labs showed an elevated white count, creatinine and creatinine phosphokinase levels. His erythrocyte sedimentation rate; C-reactive protein; urinalysis; urine drug screen; Human Immunodeficiency Virus, hepatitis, coxsackie, and influenza serology were normal. EKG showed sinus tachycardia. An echocardiogram was done which showed dilated cardiomyopathy with an ejection fraction (EF) of 15-20% and global hypokinesia. A left heart catheterization was done and was negative for coronary artery disease. At a 20 week follow up, he had stopped abusing bath salts and was asymptomatic. A repeat echocardiogram showed an EF of 52%. Cocnlusions: Bath salts (MDPV, mephedrone) are synthetic cathinones with amphetamine/cocaine like properties with potential cardiotoxic effects. Cardiovascular manifestations reported include tachycardia, hypertension, myocardial infarction, arrhythmias and cardiac arrest. "Bath salts" can also cause severe reversible dilated cardiomyopathy. Prior to diagnosis, other causes of cardiomyopathy including ischemic, infectious, familial, immunological, metabolic and cytotoxic may need to be ruled out; as was done in our patient.
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Bath Salts Induced Severe Reversible CardiomyopathySivagnanam, Kamesh, Chaudari, Dhara, Lopez, Pablo, Sutherland, Michael E., Ramu, Vijay K. 08 August 2013 (has links)
Objective: Unusual clinical course Background: "Bath salts" is the street name for a group of recently identified and increasingly abused stimulant synthetic cathinones that are associated with multiple systemic effects. We present a case of a patient who developed reversible dilated cardiomyopathy secondary to their use. Case Report: A 27 year old male with no past medical history was brought to emergency department with agitation. He had been inhaling and intravenously injecting "bath salts", containing a mephedrone/Methylenedioxypyrovalerone (MDPV) combination. On presentation, he was tachycardic, hypotensive and febrile. His initial labs showed an elevated white count, creatinine and creatinine phosphokinase levels. His erythrocyte sedimentation rate; C-reactive protein; urinalysis; urine drug screen; Human Immunodeficiency Virus, hepatitis, coxsackie, and influenza serology were normal. EKG showed sinus tachycardia. An echocardiogram was done which showed dilated cardiomyopathy with an ejection fraction (EF) of 15-20% and global hypokinesia. A left heart catheterization was done and was negative for coronary artery disease. At a 20 week follow up, he had stopped abusing bath salts and was asymptomatic. A repeat echocardiogram showed an EF of 52%. Cocnlusions: Bath salts (MDPV, mephedrone) are synthetic cathinones with amphetamine/cocaine like properties with potential cardiotoxic effects. Cardiovascular manifestations reported include tachycardia, hypertension, myocardial infarction, arrhythmias and cardiac arrest. "Bath salts" can also cause severe reversible dilated cardiomyopathy. Prior to diagnosis, other causes of cardiomyopathy including ischemic, infectious, familial, immunological, metabolic and cytotoxic may need to be ruled out; as was done in our patient.
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Overexpressing Dominant Negative MyD88 Induces Cardiac Dysfunction in Transgenic MiceChen, Wei Q., Li, Chuan Fu, Jiang, Xuan, Ruan, Hai B., Qi, Xin, Liu, Li, Zhao, Qing S., Gao, Xiang 01 November 2010 (has links)
Myeloid differentiation protein-88 (MyD88) is a crucial adaptor protein in the innate immune response. A protective role for MyD88 in normal cardiac function has been proposed in a surgical hypertrophic model. To assess the in vivo role of MyD88 in cardiac remodeling, we generated transgenic mice with cardiac-restricted expression of a dominant negative mutant of MyD88 (dnMyD88). Surprisingly, dnMyD88 transgenic mice displayed characteristic features of heart failure; including heart weight increase, cardiomyocytes enlargement, interstitial fibrosis, and re-expression of "fetal" genes. Echocardiographic examination of dnMyD88 hearts revealed dilated chamber volume and reduced cardiac contractility. DnMyD88 mice died from heart failure before they were 7 months old, as shown by Kaplan-Meier analysis. Additionally, the heart failure phenotype of dnMyD88 mice was associated with abnormal activation of the Akt/GSK-3β signaling pathway. These data provide the first evidence that normal MyD88 signaling is crucial for maintaining the physiological function of the adult heart.
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Cardiac Troponin T Mutation in Familial Cardiomyopathy With Variable Remodeling and Restrictive PhysiologyMenon, S., Michels, V. V., Pellikka, P. A., Ballew, J. D., Karst, M. L., Herron, K. J., Nelson, S. M., Rodeheffer, R. J., Olson, Timothy M. 21 October 2008 (has links)
We identified a unique family with autosomal dominant heart disease variably expressed as restrictive cardiomyopathy (RCM), hypertrophic cardiomyopathy (HCM), and dilated cardiomyopathy (DCM), and sought to identify the molecular defect that triggered divergent remodeling pathways. Polymorphic DNA markers for nine sarcomeric genes for DCM and/ or HCM were tested for segregation with disease. Linkage to eight genes was excluded, but a cardiac troponin T (TNNT2) marker cosegregated with the disease phenotype. Sequencing of TNNT2 identified a heterozygous missense mutation resulting in an I79N substitution, inherited by all nine affected family members but by none of the six unaffected relatives. Mutation carriers were diagnosed with RCM (n = 2), non-obstructive HCM (n = 3), DCM (n = 2), mixed cardiomyopathy (n = 1), and mild concentric left ventricular hypertrophy (n = 1). Endomyocardial biopsy in the proband revealed non-specific fibrosis, myocyte hypertrophy, and no myofibrillar disarray. Restrictive Doppler filling patterns, atrial enlargement, and pulmonary hypertension were observed among family members regardless of cardiomyopathy subtype. Mutation of a sarcomeric protein gene can cause RCM, HCM, and DCM within the same family, underscoring the necessity of comprehensive morphological and physiological cardiac assessment in familial cardiomyopathy screening.
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Studies of Human Mutations in Phospholamban and Heat Shock Protein 20Liu, Guan-Sheng January 2015 (has links)
No description available.
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Genotype-Phenotype Association Analysis of Dilated Cardiomyopathy in Becker Muscular DystrophyKaspar, Rita Wen 26 August 2009 (has links)
No description available.
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Multiparametric cardiovascular magnetic resonance for the assessment of cardiac function and metabolism in hypertrophy and heart failureMahmod, Masliza January 2013 (has links)
Both hypertrophied and failing hearts are characterised by pathological left ventricular (LV) remodelling, impaired myocardial energy status and alteration in substrate metabolism. Cardiac magnetic resonance imaging (CMR) and magnetic resonance spectroscopy (MRS) are powerful tools in the characterisation of these disease conditions. More recent techniques have allowed assessment of myocardial steatosis using <sup>1</sup>H-MRS and tissue oxygenation using blood oxygen level dependent (BOLD) CMR. In hypertrophy and heart failure, studies on steatosis and the relationship with other parameters such as myocardial function and fibrosis, especially in humans are limited. I therefore investigated the presence of steatosis in severe aortic stenosis (AS) and dilated cardiomyopathy (DCM), and further assessed its relation to contractile function. This study found that myocardial triglyceride (TG) content is increased in both symptomatic and asymptomatic AS patients (lipid/water ratio 0.89±0.42% in symptomatic AS; 0.75±0.36% in asymptomatic AS vs. controls 0.45±0.17%, both p<0.05) and DCM patients (lipid/ratio 0.64±0.44% vs. controls 0.40±0.13%, p=0.03). Circumferential strain was lower in both AS (-16.4±2.5% in symptomatic AS; -18.9±2.9% in asymptomatic AS vs. controls 20.7±2.0%, both p<0.05) and DCM patients (-12.3±3.4% vs. controls -20.9±1.7%, p<0.001). In AS, myocardial contractility is related to the degree of steatosis, and were both reversible following aortic valve replacement (AVR), lipid/water ratio 0.92±0.41% vs. pre AVR 0.45±0.17%, p=0.04 and circumferential strain -17.2±2.0% vs. pre AVR -19.5±3.2%, p=0.04. A novel finding of this study was significant correlation of MRS-measured TG content with histological staining of TG of the myocardium, taken from endomyocardial biopsy during AVR. In DCM, myocardial TG was independently associated with LV dilatation and correlated significantly with hepatic TG, which suggests that both cardiac and hepatic steatosis might be a common feature in the failing heart. Additionally, although the hypertrophied heart is characterised by impaired perfusion, it is unknown if this is severe enough to translate into tissue deoxygenation and ischaemia. I assessed this by using adenosine vasodilator stress test and BOLD-CMR in patients with severe AS. It was found that AS patients had reduced perfusion (myocardial perfusion reserve index-MPRI 1.0±0.3 vs. controls 1.7±0.3, p<0.001), and blunted tissue oxygenation (blood-oxygen level dependent-BOLD signal intensity-SI change 4.8±9.6% vs. controls 18.2±11.6%, p=0.001) during stress. Importantly, there was a substantial improvement in perfusion and oxygenation towards normal after AVR, MPRI 1.5±0.4, p=0.005 vs. pre AVR and BOLD SI change 16.4±7.0%, p=0.014 vs. pre AVR. Overall, the work in this thesis supports the powerful role of CMR in assessing LV function and elucidating metabolic mechanisms in the hypertrophied and failing heart.
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Estudo da sobrevida e de fatores prognósticos em cães com cardiomiopatia dilatada idiopática / Survival study and assessment of prognostic factors in dogs with idiopathic dilated cardiomyopathyYamaki, Fernanda Lie 30 August 2007 (has links)
Cardiomiopatia dilatada (CMD) é uma das doenças cardiovasculares adquiridas mais comuns em cães afetando principalmente cães de raças grandes e gigantes, além do Cocker Spaniel Inglês e Americano. A anormalidade primária é a diminuição da contratilidade miocárdica, com dilatação secundária das câmaras cardíacas, que pode evoluir para insuficiência cardíaca, apresentar arritmias (atrial e/ou ventricular) e resultar em óbito em qualquer estágio da doença (sendo a morte súbita relativamente comum). Poucos estudos em cães, sendo a maioria retrospectiva, têm o objetivo de determinar fatores prognósticos, e predizer o prognóstico em qualquer paciente continua a ser um desafio. Portanto, no presente trabalho objetivou-se estudar a sobrevida de cães com CMD, assim como observar possíveis fatores determinantes de sobrevida. Para tal, foram avaliados 50 cães com CMD por meio de exame físico, radiográfico de tórax, eletrocardiográfico (eletrocardiograma de repouso e monitorização Holter) e ecocardiográfico. Os animais foram acompanhados por pelo menos 150 dias ou até o óbito. Avaliou-se a influência da idade, raça, sexo, fração de encurtamento do ventrículo esquerdo (FE), da classe funcional da insuficiência cardíaca, da presença de ascite, efusão pleural, edema pulmonar, insuficiência cardíaca bilateral, fibrilação atrial (FA) ou de arritmias ventriculares na sobrevida. A sobrevida dos cães com CMD variou de cinco dias a 1021 dias, com tempo médio de 347 dias, e tempo mediano de sobrevida foi de 223 dias; a probabilidade de sobreviver por seis meses foi de 51%, por um ano foi de 37% e por dois anos foi de 13%. Os cães da raça Cocker Spaniel Inglês apresentaram maior sobrevida em relação aos cães da raça Doberman e aos cães de outras raças. A presença de FA (p<0,03) e de arritmias ventriculares (tanto de ectopias ventriculares no eletrocardiograma de repouso (p<0,02) como de taquicardia ventricular não sustentada (p<0,0001) na monitorização Holter) foram associadas a menor sobrevida, enquanto que a idade, FE, sexo, classe funcional da insuficiência cardíaca, presença de ascite, efusão pleural, edema pulmonar ou insuficiência cardíaca bilateral não estiveram associados a aumento da mortalidade. A sobrevida foi variável, mas o prognóstico em geral foi ruim. O melhor preditor diagnóstico foi a presença de taquicardia ventricular não sustentada na monitorização Holter. / Dilated cardiomyopathy (DCM) is one of the most common acquired cardiovascular disease of dogs, affecting mainly large and giant breeds, as well as English and American Cocker Spaniels. The primary abnormality is decrease in myocardial contractility with secondary cardiac chambers dilatation. The clinical presentation may include development of heart failure, arrhythmias (atrial and/or ventricular), and death in any phase of the disease (with sudden death relatively frequent). Few studies have been described in dogs with the purpose of determining prognostic indicators for DCM, and predicting prognosis in any given single patient continues to be a challenge. The aim of this study was to evaluate survival time, and if possible, to find factors influencing prognosis in dogs with dilated cardiomyopathy. Fifty dogs with DCM have been included in the study. The patients were prospectively evaluated by physical examination, ten-lead electrocardiography, thoracic radiography, 24-hour Holter monitoring, and echocardiography. The animals were followed-up for at least 150 days or until death. Studied variables were left ventricle shortening fraction, age, sex, breed, presence of ascite, subcutaneous edema, pulmonary edema, pleural effusion, biventricular heart failure, as well as, presence of atrial fibrillation and ventricular arrhythmias, including non-sustained ventricular tachycardia on Holter monitoring. The mean and median survival time were, respectively, 347 days and 223 days (range 5 to 1021 days). Probability of survival at six months was 51%, at 1 year was 37%, and at 2 year was 13%. The survival time was significantly longer in English Cocker Spaniel, versus Doberman Pinschers, or versus other breeds. Atrial fibrillation (p<0,03) and ventricular arrhthmias (ventricular ectopy on ten-lead electrocardiography (p<0,02) and non-sustained ventricular tachycardia (p<0,0001) on Holter monitoring) were associated with increased mortality. While age at the time of presentation, shortening fraction, gender, presence of ascites, pleural effusion, or pulmonary edema were not associated with increased mortality. Survival time was variable, but the prognosis was usually poor. The best prognostic indicator was the presence of non-sustained ventricular tachycardia in Holter monitoring.
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Correlação entre os níveis sangüíneos da proteína S100B e do NT-proBNP em portadores de cardiomiopatia dilatada / Correlação entre os níveis sangüíneos da proteína S100B e do NT-proBNP em portadores de cardiomiopatia dilatadaBordignon, Solange 10 February 2009 (has links)
A proteína S100B é considerada um marcador bioquímico para lesão cerebral. Entretanto, foi demonstrado que há liberação de S100B em coração isolado de rato. Neste estudo, investigou-se os níveis séricos de S100B em pacientes portadores de cardiomiopatia dilatada (CMD). Métodos e Resultados: Foram selecionados 21 pacientes com CMD, excluindo qualquer condição que pudesse influenciar os níveis séricos de S100B. O grupo controle foi composto por 21 indivíduos pareados por sexo e idade. Ambos os grupos foram submetidos à avaliação clínica, ecocardiográfica, mensuração da proteína S100B e de NT-proBNP (expressos como mediana [variação interquartil]). Os níveis de NT-proBNP no grupo de pacientes (1462 pg/ml [426 - 3591]) foram maiores do que no grupo controle (35 pg/ml [29 - 55]); P<0.001. Os níveis de S100B foram maiores no grupo de pacientes (0.051µg/L [0.022 - 0.144]) do que no grupo controle (0.017µg/L [0.003 - 0.036]); P=0.009. Houve correlação positiva entre os níveis séricos de S100B e NT-proBNP somente no grupo de pacientes (Coeficiente de Spearman r=0.534; P=0.013). Conclusão: A proteína S100B está aumentada na CMD. Embora não possamos excluir a influência de dano cerebral, houve uma correlação positiva entre os níveis séricos de S100B e NT-proBNP em pacientes com CMD / The S100B protein is considered a biochemical marker for brain injuries. However, the isolated rat heart releases S100B. In this study, the serum levels of S100B was investigated in dilated cardiomyopathy (DCM) patients in order to evaluate its levels in heart disease. Methods and Results: It was selected DCM patients, excluding any condition that could influence S100B serum levels. Control individuals were sex and age matched. Both groups were submitted to clinical evaluation and echocardiography. The S100B and NT-proBNP serum levels (expressed as median [interquartile range]) were measured. NT-proBNP levels in patients group (1462 pg/ml [426 - 3591]) were higher than in controls (35 pg/ml [29 - 55]); P<0.001. S100B serum levels were higher in patients group (0.051µg/L [0.022 - 0.144]) than in controls (35 pg/ml [29 - 55]); P<0.001. S100B serum levels were higher in patients group (0.051µg/L [0.022 - 0.144]) than in controls (0.017µg/L [0.003 - 0.036]); P=0.009. Additionally, a positive correlation between S100B and NT-proBNP serum levels only in patients group (Spearman\'s coefficient r=0.534; P=0.013) was found . Conclusions: Although the influence of S100B from brain cannot rule out, the positive correlation between S100B and NT-proBNP levels in DCM patients points to the myocardium as the main source for the rise in S100B serum levels
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Avaliação clínica de cães com cardiomiopatia dilatada idiopática, submetidos ao tratamento com carvedilol / Clinical avaliation of dogs with dilated cardiomyopathy (DCM) treated by carvedilolLeomil Neto, Moacir 09 January 2006 (has links)
A cardiomiopatia dilatada (CMD) é uma doença freqüente na clínica veterinária que acomete, principalmente, a espécie canina, habitualmente os machos, jovens ou adultos-jovem, das raças grandes e gigantes, em especial Doberman e Boxer. A doença caracteriza-se por uma redução na contratilidade e, freqüentemente, por arritmias que resultam na diminuição do volume sistólico e do débito cardíaco. O tratamento convencionalmente preconizado para cães acometidos pela CMD consiste na prescrição de vasodilatadores, agentes inotrópicos positivos (digitálico), diuréticos, dieta hipossódica e, quando necessário, antiarrítmicos. A ativação do sistema nervoso simpático (SNAS) ocorre em resposta à redução do débito cardíaco e da pressão arterial observados em casos de insuficiência cardíaca. Porém a partir de um certo grau os efeitos hipertensivos, cronotrópicos e inotrópicos positivos do SNAS geram graves alterações cardíacas como a sobrecarga de pressão e volume nos ventrículos, conseqüente isquemia miocárdica, morte de miócitos com deposição de tecido conjuntivo, diminuição da contratilidade cardíaca e nova sobrecarga de pressão e volume. O carvedilol é um β-bloqueador de 3a geração, não seletivo, que bloqueia igualmente e competitivamente os receptores β1, β2 e β1. O carvedilol produz uma evidente vasodilatação periférica, exerce efeitos anti-oxidantes, removendo radicais livres de oxigênio e prevenindo a peroxidação lipídica nas membranas cardíacas, prevenindo a perda de miócitos e a ocorrência de arritmias e reduzindo a taxa de mortalidade em pacientes humanos. O objetivo do presente estudo foi avaliar clínica, eletrocardiográfica, radiográfica e ecocardiograficamente a evolução de cães com cardiomiopatia dilatada (CMD) tratatos com terapia convencional associada ao carvedilol. Para tal foram avaliados 49 cães com CMD divididos em: grupo NT, tratado com terapia convencional, e grupo T, tratado com terapia convencional associada ao carvedilol. Os animais foram submetidos à avaliação clínica e a exames complementares durante o período de um ano. Os resultados demonstraram que a terapia com carvedilol apresentou boa tolerabilidade na dose de 0,3 mg/kg/12-12horas, aumentou a sobrevida dos cães em 30,9%, não alterou as pressões sistólica e diastólica, reduziu a freqüência cardíaca após três semanas de terapia, melhorou significantemente as frações de encurtamento e ejeção após seis meses de tratamento, não promoveu alterações radiográficas e da distância E-septo, diminuiu o índice de letalidade da doença, fato demonstrado pela melhora no escore clínico e na classe funcional dos animais, obtidas após três semanas de terapia com carvedilol. / Dilated cardiomyopathy (DCM) is a frequent disease in veterinary clinics which occurs specially in dogs, mostly males, young or young-adults, of big and giant breeds, mainly Dobermans and Boxers. The disease is characterized by a reduction in contractility and, frequently, by arrhythmias resulting in decrease of systolic volume and cardiac output. Commonly prescribed therapy for dogs presenting DCM consists of vasodilators, positive inotropic drugs (digitalics), diuretics, low-sodium diet and, when necessary, anti-arrhythmics. Activation of sympathetic nervous system (SNS) occurs in response to decrease in cardiac output and arterial pressure observed in cases of heart failure. However, after a certain degree, hypotensive, chronotropic and positive inotropic effects of SNS lead to severe heart alterations like pressure and volume overload on ventricles with consequent myocardial ischemia, death of myocytes with connective tissue deposition, decrease in heart contractility, and again pressure and volume overload. Carvedilol is a third generation non-selective ?- blocker which blocks equally and competitively β1, β2 and β1 receptors. Carvedilol produces an evident peripheral vasodilation, exerts anti-oxidative effects, removing free radicals of oxygen and preventing lipidic peroxydation of cardiac membranes, and the loss of myocytes and arrhythmias, as well as reducing mortality rate in human patients. The aim of the present study was to evaluate by physical examination, electrocardiography, radiography, and echocardiography the evolution of dogs with dilated cardiomyopathy (DCM) treated by conventional therapy associated to carvedilol. Forty-nine dogs with DCM were divided in two groups: group NT: treated with conventional therapy, and group T: treated with conventional therapy associated to carvedilol. The animals were submitted to clinical and complementary examinations during one year. The results demonstrated that carvedilol therapy presented good tolerability on the dose of 0,3 mg/Kg each 12 hours, prolonged lifetime of the dogs in 30,9%, did not alter systolic or diastolic pressure, reduced heart frequency after three weeks of treatment, significantly enhanced shortening and ejection fractions after six months of treatment, did not promote radiographic or E-septum distance alterations, decreased patients letality, as demonstrated by improvement of clinical score and functional class (heart failure according to NYHA) of the animals, obtained three weeks after the beginning of cavedilol therapy.
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