8 results on '"Ana Cláudia Reis Schneider"'
Search Results
2. Chronic exposure to ethanol causes steatosis and inflammation in zebrafish liver
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Larisse Longo, Maria Cristina Faccioni-Heuser, Tais Malysz, Ranieli Guizzo, Themis Reverbel da Silveira, Cleandra Gregório, Ana Cláudia Reis Schneider, and Carolina Uribe-Cruz
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0301 basic medicine ,medicine.medical_specialty ,Hepatic steatosis ,Etanol ,Inflammation ,Hepatopatias alcoólicas ,03 medical and health sciences ,chemistry.chemical_compound ,Internal medicine ,medicine ,Alcoholic fatty liver ,Zebrafish ,Adiponectin receptor 2 ,Hepatology ,biology ,Adiponectin ,Glycogen ,Ethanol ,business.industry ,Basic Study ,biology.organism_classification ,medicine.disease ,Inflamação ,030104 developmental biology ,Endocrinology ,chemistry ,Tumor necrosis factor alpha ,medicine.symptom ,Steatosis ,business ,Peixe-zebra - Abstract
Aim To evaluate the effects of chronic exposure to ethanol in the liver and the expression of inflammatory genes in zebrafish. Methods Zebrafish (n = 104), wild type, adult, male and female, were divided into two groups: Control and ethanol (0.05 v/v). The ethanol was directly added into water; tanks water were changed every two days and the ethanol replaced. The animals were fed twice a day with fish food until satiety. After two and four weeks of trial, livers were dissected, histological analysis (hematoxilin-eosin and Oil Red staining) and gene expression assessment of adiponectin, adiponectin receptor 2 (adipor2), sirtuin-1 (sirt-1), tumor necrosis factor-alpha (tnf-a), interleukin-1b (il-1b) and interleukin-10 (il-10) were performed. Ultrastructural evaluations were conducted at fourth week. Results Exposing zebrafish to 0.5% ethanol developed intense liver steatosis after four weeks, as demonstrated by oil red staining. In ethanol-treated animals, the main ultrastructural changes were related to cytoplasmic lipid particles and droplets, increased number of rough endoplasmic reticulum cisterns and glycogen particles. Between two and four weeks, hepatic mRNA expression of il-1b, sirt-1 and adipor2 were upregulated, indicating that ethanol triggered signaling molecules which are key elements in both hepatic inflammatory and protective responses. Adiponectin was not detected in the liver of animals exposed and not exposed to ethanol, and il-10 did not show significant difference. Conclusion Data suggest that inflammatory signaling and ultrastructural alterations play a significant role during hepatic steatosis in zebrafish chronically exposed to ethanol.
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- 2016
3. Low plasma zinc concentrations in pediatric patients with cirrhosis
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Themis Reverbel da Silveira, Pedro Eduardo Fröehlich, Raquel B. Pinto, Ana Cláudia Reis Schneider, and Thais Ortiz Hammes
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Liver Cirrhosis ,Male ,medicine.medical_specialty ,Food intake ,Cirrhosis ,Adolescent ,chemistry.chemical_element ,Zinc ,Gastroenterology ,Liver disease ,Internal medicine ,Blood plasma ,medicine ,Humans ,Child ,Plasma zinc ,Anthropometry ,business.industry ,Control subjects ,medicine.disease ,Endocrinology ,chemistry ,Pediatrics, Perinatology and Child Health ,Female ,Epidemiologic Methods ,business - Abstract
OBJECTIVE To determine plasma zinc concentrations in children and adolescents with cirrhosis and to investigate the association between these results and dietary zinc intake, anthropometric data, and severity of liver disease. METHODS Plasma zinc concentration was assessed by atomic absorption spectrophotometry in 30 children and adolescents with cirrhosis (105.0+/-60.0 months; 22 girls) and 27 without liver disease (122.3+/-47.3 months, 14 girls). Dietary zinc data were evaluated by 3-day food intake records. Anthropometry measures included height, weight, skinfold thickness, brachial circumference, and upper arm muscle size. Severity of liver disease was classified according to the Child-Pugh, MELD, and PELD criteria. RESULTS The mean (+/- standard deviation) plasma zinc concentrations in control subjects and patients were 105.69+/-19.46 and 75.44+/-24.45 microg/dL, respectively (p < 0.001). No associations were found between anthropometric measures, dietary zinc intake, and plasma zinc concentration. There was statistical difference related to plasma zinc concentrations between Child-Pugh B + C patients and control subjects (p < 0.001), and concerning PELD, between patients below the cutoff score of 15 and those above (p = 0.002). CONCLUSIONS The prevalence of hypozincemia was 43% for patients with cirrhosis. Although low plasma zinc concentration was associated with more severe liver disease, it was present even in some Child-Pugh A patients. Therefore, zinc supplementation should be considered for cirrhotic children.
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- 2009
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4. An Assay for Determination of Hepatic Zinc by AAS - Comparison of Fresh and Deparaffinized Tissue
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Themis Reverbel da Silveira, André Castagna Wortmann, Raquel Borges Pinto, Tiago Muller Weber, Ana Cláudia Reis Schneider, and Pedro Eduardo Fröehlich
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medicine.medical_specialty ,business.industry ,Family medicine ,Medicine ,business - Abstract
Raquel Borges Pinto1, Pedro Eduardo Froehlich2, Ana Claudia Reis Schneider3, Andre Castagna Wortmann3, Tiago Muller Weber2 and Themis Reverbel da Silveira1,* 1Post Graduate Program in Medicine: Pediatrics, 2Post Graduate Program in Pharmaceutical Sciences, UFRGS, Porto Alegre, 3Post Graduate Program in Medical Sciences: Gastroenterology and Hepatology, Universidade Federal do Rio Grande do Sul (UFRGS), Hospital de Clinicas de Porto Alegre, Brazil
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- 2012
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5. MR findings of the brain in children and adolescents with portal hypertension and the relationship with blood manganese levels
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T R da Silveira, Ana Cláudia Reis Schneider, J A Bragatti, Raquel Borges Pinto, J Becker, Pedro Eduardo Fröehlich, A F H Cornely, and Eduardo Hennemann Pitrez
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Male ,medicine.medical_specialty ,Pathology ,Cirrhosis ,Adolescent ,Central nervous system ,Chronic liver disease ,Gastroenterology ,Liver disease ,Young Adult ,Ammonia ,Internal medicine ,Hypertension, Portal ,Image Processing, Computer-Assisted ,Medicine ,Humans ,Child ,Retrospective Studies ,Manganese ,business.industry ,Vascular disease ,Liver Diseases ,Case-control study ,Brain ,General Medicine ,medicine.disease ,Magnetic Resonance Imaging ,Hyperintensity ,medicine.anatomical_structure ,Case-Control Studies ,Pediatrics, Perinatology and Child Health ,Portal hypertension ,Female ,Neurology (clinical) ,business - Abstract
Background Few studies have evaluated abnormalities on brain magnetic resonance imaging (MRI) in children and adolescents with chronic liver disease. Aims The aim of this study was to investigate the presence of T1 hyperintensity in the basal ganglia of pediatric patients with portal hypertension and its association with blood manganese levels. Methods A case control study of 22 patients with portal hypertension (14 Child-Pugh A cirrhosis, 8 non-cirrhotic portal hypertension) and 15 controls was conducted from 2006 to 2007. Blood manganese levels were measured using atomic absorption spectrophotometry. Brain MRI scans were performed using a 1.5 Tesla (Philips) scanner. Results Blood manganese levels were 26.01+/-12.82 microg/L for patients with portal hypertension (cirrhotic: 22.73+/-11.67 microg/L, non-cirrhotic: 32+/-13.32 microg/L) and 15.64+/-6.61 microg/L for controls (p=0.003). 14/22 patients with portal hypertension presented T1 hyperintensity in the basal ganglia [6/14 cirrhotic; 8/8 non-cirrhotic (p=0.018); zero controls (p=0.001)]. Mean blood manganese levels of patients with liver disease and normal vs. abnormal brain MRI scans were 18.45+/-8.38 microg/L and 30.47+/-13.07 microg/L, respectively (p=0.04). Conclusions Brain MRI showed a high frequency (64%) of T1 hyperintensity in the basal ganglia of patients with portal hypertension, which correlated positively with blood manganese levels. This abnormality was found in 100% of the patients with portal hypertension and in 43% of those with mild cirrhotic disease.
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- 2010
6. [Nutritional risk and malnutrition determination by anthropometry in cirrhotic children and adolescents]
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Ana Cláudia Reis, Schneider, Raquel Borges, Pinto, and Themis Reverbel da, Silveira
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Liver Cirrhosis ,Male ,Adolescent ,Malnutrition ,Infant ,Nutritional Status ,Child Nutrition Disorders ,Risk Assessment ,Severity of Illness Index ,Infant Nutrition Disorders ,Cross-Sectional Studies ,Child, Preschool ,Humans ,Body Weights and Measures ,Female ,Child - Abstract
The malnutrition is a frequent finding in adults with cirrhosis, but the prevalence of nutritional risk and malnutrition is little known in pediatric patients.To evaluate through anthropometry the presence of nutritional risk and malnutrition in cirrhotic pediatric patients regularly attended at the Pediatric Gastroenterology Service of "Hospital de Clínicas" of Porto Alegre, RS, Brazil.Cross-sectional study with 42 cirrhotic children and adolescents aged between 3 months and 18 years. The nutritional evaluation was made by the determination of the weight/age, height/age, body mass index and triceps skinfold thickness and arm muscle circumference measurements. Patients considered in nutritional risk wereor = -1,28 Z score which corresponds toor = 10th percentile, and those under -2,0 Z andor = 3th percentile were in malnutrition status. According to Child-Pugh criteria, 22 patients were classified as A (mild severity), 15 (moderate) B and 5 C (intense).The mean weight/age, height/age and body mass index Z scores were, respectively, - 0,38 +/- 1,4 SD, - 0,83 +/- 1,16 SD and 0,17 +/- 1,3 SD. Patients in nutritional risk were 3/42 (weight/age), 8/42 (height/age), 12/37 (triceps skinfold thickness), 9/37 (arm muscle circumference), 2/38 (body mass index); in malnutrition status were 6/42 (weight/age), 7/42 (height/age), 4/37 (triceps skinfold thickness) and 4/37 (arm muscle circumference) and 3/38 (body mass index).The prevalence of nutritional risk was 32.4% and chronic malnutrition was 16.7%. The index which better reflected the nutritional risk in these patients was triceps skinfold thickness. Chronic malnutrition status occurrence was greater in the height/age index.
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- 2008
7. Zebrafish: modelo consagrado para estudos de doenças humanas
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Thais Ortiz Hammes, Ana Cláudia Reis Schneider, and Themis Reverbel da Silveira
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General Earth and Planetary Sciences ,Biology ,General Environmental Science - Published
- 2012
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8. Cirrhosis in children and adolescents: An overview
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Ana Cláudia Reis Schneider, Themis Reverbel da Silveira, and Raquel Borges Pinto
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Pediatrics ,medicine.medical_specialty ,Gastrointestinal bleeding ,Cirrhosis ,Hepatology ,business.industry ,Review ,Autoimmune hepatitis ,medicine.disease ,Primary sclerosing cholangitis ,Liver disease ,Malnutrition ,Spontaneous bacterial peritonitis ,Biliary atresia ,Medicine ,business - Abstract
Several conditions, especially chronic liver diseases, can lead to cirrhosis in children and adolescents. Most cases in clinical practice are caused by similar etiologies. In infants, cirrhosis is most often caused by biliary atresia and genetic-metabolic diseases, while in older children, it tends to result from autoimmune hepatitis, Wilson's disease, alpha-1-antitrypsin deficiency and primary sclerosing cholangitis. The symptoms of cirrhosis in children and adolescents are similar to those of adults. However, in pediatric patients, the first sign of cirrhosis is often poor weight gain. The complications of pediatric cirrhosis are similar to those observed in adult patients, and include gastrointestinal bleeding caused by gastroesophageal varices, ascites and spontaneous bacterial peritonitis. In pediatric patients, special attention should be paid to the nutritional alterations caused by cirrhosis, since children and adolescents have higher nutritional requirements for growth and development. Children and adolescents with chronic cholestasis are at risk for several nutritional deficiencies. Malnutrition can have severe consequences for both pre- and post-liver transplant patients. The treatment of cirrhosis-induced portal hypertension in children and adolescents is mostly based on methods developed for adults. The present article will review the diagnostic and differential diagnostic aspects of end-stage liver disease in children, as well as the major treatment options for this condition.
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- 2015
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