ABSTRACT
OBJECTIVES: To prospectively evaluate demographic, anthropometric and health-related quality of life (HRQoL) in pediatric patients with laboratory-confirmed coronavirus disease 2019 (COVID-19) METHODS: This was a longitudinal observational study of surviving pediatric post-COVID-19 patients (n=53) and pediatric subjects without laboratory-confirmed COVID-19 included as controls (n=52) was performed. RESULTS: The median duration between COVID-19 diagnosis (n=53) and follow-up was 4.4 months (0.8-10.7). Twenty-three of 53 (43%) patients reported at least one persistent symptom at the longitudinal follow-up visit and 12/53 (23%) had long COVID-19, with at least one symptom lasting for >12 weeks. The most frequently reported symptoms at the longitudinal follow-up visit were headache (19%), severe recurrent headache (9%), tiredness (9%), dyspnea (8%), and concentration difficulty (4%). At the longitudinal follow-up visit, the frequencies of anemia (11% versus 0%, p=0.030), lymphopenia (42% versus 18%, p=0.020), C-reactive protein level of >30 mg/L (35% versus 0%, p=0.0001), and D-dimer level of >1000 ng/mL (43% versus 6%, p=0.0004) significantly reduced compared with baseline values. Chest X-ray abnormalities (11% versus 2%, p=0.178) and cardiac alterations on echocardiogram (33% versus 22%, p=0.462) were similar at both visits. Comparison of characteristic data between patients with COVID-19 at the longitudinal follow-up visit and controls showed similar age (p=0.962), proportion of male sex (p=0.907), ethnicity (p=0.566), family minimum monthly wage (p=0.664), body mass index (p=0.601), and pediatric pre-existing chronic conditions (p=1.000). The Pediatric Quality of Live Inventory 4.0 scores, median physical score (69 [0-100] versus 81 [34-100], p=0.012), and school score (60 [15-100] versus 70 [15-95], p=0.028) were significantly lower in pediatric patients with COVID-19 at the longitudinal follow-up visit than in controls. CONCLUSIONS: Pediatric patients with COVID-19 showed a longitudinal impact on HRQoL parameters, particularly in physical/school domains, reinforcing the need for a prospective multidisciplinary approach for these patients. These data highlight the importance of closer monitoring of children and adolescents by the clinical team after COVID-19.
Subject(s)
Humans , Male , Child , Adolescent , COVID-19/complications , Quality of Life , Prospective Studies , Tertiary Care Centers , COVID-19 Testing , SARS-CoV-2 , Latin AmericaABSTRACT
OBJETIVOS: Avaliar a composição de ácidos graxos do leite humano maduro de mulheres residentes em área distante da costa litorânea brasileira. MÉTODOS: Amostras de leite materno maduro foram obtidas de 47 mulheres lactantes com idade entre 18 e 35 anos, que tiveram partos a termo e em aleitamento exclusivo ou predominante. A coleta de leite se deu a partir da 5ª semana pós-parto, por meio de ordenha manual. A composição de ácidos graxos do leite foi determinada por cromatografia gasosa. RESULTADOS: Verificou-se que a concentração de eicosapentaenoico (0,08%) foi superior ao observado em estudos brasileiros prévios. Entretanto, o teor de docosahexaenoico (0,09%) encontrado no leite humano foi um dos menores já verificados no mundo. O teor de ácidos graxos trans (2,05%) foi similar ao relatado em estudos nacionais prévios à obrigatoriedade de declaração do teor deste em rótulos de alimentos, sugerindo que esta medida não surtiu efeito na redução de seu teor na dieta habitual das mulheres. CONCLUSÕES: Baixo teor de docosahexaenoico e elevada concentração de ácidos graxos trans foram verificados no leite materno maduro de mulheres residentes em área distante da costa litorânea brasileira.
OBJECTIVES: To evaluate the fatty acid composition of mature human milk of women living far from the coastal area of Brazil. METHODS: Mature breast milk samples were obtained from 47 lactating women aged between 18 and 35 years, who delivered their babies at term and who exclusively or predominantly breastfed. Milk collection took place after the fifth week postpartum by hand expression. The fatty acid composition of the milk was determined by gas chromatography. RESULTS: It was observed that the concentration of eicosapentaenoic acid (0.08%) was higher than that observed in previous studies in Brazil. However, the content of docosahexaenoic acid (0.09%) found in human milk was one of the lowest verified in the world. The content of trans fatty acids (2.05%) was similar to that reported in national studies previous to the mandatory declaration of this fatty acid content in food labels, suggesting that this measure had no effect on reducing the content of this fatty acid in the usual diet of women. CONCLUSIONS: Low levels of docosahexaenoic acid and high concentrations of trans fatty acids were observed in mature breast milk of women living far from the coastal area in Brazil.
Subject(s)
Adolescent , Adult , Female , Humans , Young Adult , Fatty Acids/analysis , Milk, Human/chemistry , Brazil , Dietary Fats/analysis , Docosahexaenoic Acids/analysis , Eicosapentaenoic Acid/analysis , Lactation/physiology , Prospective Studies , Trans Fatty Acids/analysis , Urban Population/statistics & numerical dataABSTRACT
PURPOSE: The increase in fructose consumption is paralleled by a higher incidence of obesity worldwide. This monosaccharide is linked to metabolic syndrome, being associated with hypertriglyceridemia, hypertension, insulin resistance and diabetes mellitus. It is metabolized principally in the liver, where it can be converted into fatty acids, which are stored in the form of triglycerides leading to NAFLD. Several models of NAFLD use diets high in simple carbohydrates. Thus, this study aimed to describe the major metabolic changes caused by excessive consumption of fructose in humans and animals and to present liver abnormalities resulting from high intakes of fructose in different periods of consumption and experimental designs in Wistar rats. METHODS: Two groups of rats were fasted for 48 hours and reefed for 24 or 48 hours with a diet containing 63 percent fructose. Another group of rats was fed an diet with 63 percent fructose for 90 days. RESULTS: Refeeding for 24 hours caused accumulation of large amounts of fat, compromising 100 percent of the hepatocytes. The amount of liver fat in animals refed for 48 hours decreased, remaining mostly in zone 2 (medium-zonal). In liver plates of Wistar rats fed 63 percent fructose for 45, 60 and 90 days it's possible to see that there is an increase in hepatocytes with fat accumulation according to the increased time; hepatic steatosis, however, is mild, compromising about 20 percent of the hepatocytes. CONCLUSIONS: Fructose is highly lipogenic, however the induction of chronic models in NAFLD requires long periods of treatment. The acute supply for 24 or 48 hours, fasted rats can cause big changes, liver steatosis with macrovesicular in all lobular zones.
OBJETIVO: O aumento do consumo de frutose é concomitante a maior incidência mundial de obesidade. Este monossacarídeo está relacionado à Síndrome Metabólica, sendo vinculado à hipertrigliceridemia, hipertensão arterial, resistência à insulina e diabetes mellitus. É metabolizada principalmente no fígado, onde pode ser convertida em ácidos graxos, os quais serão estocados na forma de trigligérides ocasionando a esteatose hepática não alcoólica (NAFLD). Vários modelos de NAFLD utilizam dietas ricas em carboidratos simples. Desta forma, este trabalho teve como objetivos descrever as principais alterações metabólicas causadas pelo consumo excessivo de frutose em humanos e em animais e apresentar as alterações hepáticas decorrentes da alta ingestão de frutose em diferentes períodos de consumo e desenhos experimentais em ratos Wistar. MÉTODOS: Dois grupos de ratos Wistar foram mantidos em jejum durante 48 horas e realimentados por 24 ou 48 horas com dieta contendo 63 por cento de frutose. Outro grupo de ratos Wistar foi alimentado com 63 por cento de frutose durante 90 dias. RESULTADOS: A realimentação por 24 horas provocou acúmulo de grande quantidade de gordura. A quantidade de gordura hepática nos animais realimentados por 48 horas diminuiu, mantendo-se principalmente nas zona 2 (medio-zonal). Em fígados de ratos Wistar alimentados com 63 por cento de frutose até 90 dias foi possível observar que há aumento de hepatócitos com acúmulo de gordura consequente ao aumento do tempo, no entanto a esteatose hepática é leve (20 por cento). CONCLUSÕES: A frutose é altamente lipogênica, no entanto a indução de NAFLD em modelos crônicos necessita de longos períodos de tratamento. A oferta aguda, por 24 ou 48 horas, a ratos mantidos em jejum é capaz de ocasionar grandes mudanças hepáticas, com presença de esteatose macrovesicular em todas as zonas lobulares.
Subject(s)
Animals , Male , Rats , Disease Models, Animal , Fatty Liver/metabolism , Fructose/metabolism , Liver/metabolism , Metabolic Syndrome/metabolism , Sweetening Agents/metabolism , Fatty Liver/etiology , Fructose/adverse effects , Metabolic Syndrome/etiology , Obesity/etiology , Obesity/metabolism , Rats, Wistar , Sweetening Agents/adverse effects , Time FactorsABSTRACT
Modelo de estudo: Estudo experimental. Objetivos: este estudo teve como objetivo avaliar e caracterizar a dieta hipoprotéica como um modelo experimental para estudo de EHNA. Métodos: foram utilizados ratos da linhagem Wistar divididos em dois grupos com dietas isocalóricas: controle (GC) no qual a dieta utilizada seguiu o preconizado pela AIN-93 e hipoprotéico (GH) com quantidade de proteína reduzida de 20% para 10%. As dietas e água foram ofertadas ad libitum por quatro semanas. Após esse período, os animais foram sacrificados e analisados: glicemia; nitrogênio urinário; proteína sérica; gordura hepática; colesterol; variação de peso e quantidade de ração consumida. Resultados: glicemia e nitrogênio urinário não apresentaram diferenças significativas entre GC e GH (p>0,05), a variação de peso no último dia do experimento foi significativa (p<0,02). A porcentagem de gordura hepática foi estatisticamente maior no GH, quando comparado ao GC (p<0,04). Foram menores o nível de colesterol (p<0,01) e proteína sérica (p<0,005) no GH. A quantidade de dieta consumida não foi diferente entre os grupos, considerando-se as médias de ingestão semanal. Conclusões: neste trabalho a dieta hipoprotéica constitui um modelo de indução de EHNA que pode ser caracterizada pela diminuição da proteína sérica e do colesterol plasmático e aumento da gordura hepática, entretanto não ocorreram alterações na glicemia sugerindo que não existiu mudança na sensibilidade à insulina, constituindo assim um modelo falho para estudar um dos principais fatores de risco para o estabelecimento da EHNA, a resistência à insulina.
Model of study: Experimental study. Objectives: this study had as objective evaluate and characterize a low protein diet as an experimental model for non alcoholic fatty liver disease(NAFLD). Methods: male Wistar rats were divided in two groups with isocaloric diets: control (GC) in which the used diet followed praised for the AIN-93 and the low protein (GH), with reduced amount of protein of 20% for 10%. The diets and water had been offered ad libitum over four weeks. After this period the animals were sacrificed and analyzed: glycemia; urinary nitrogen; serum protein; liver total lipids; cholesterol; weight variation and food consumed. Results: the glycemia and the urinary nitrogen had not presented significant differences between GC and GH (p>0,05). The change of weight in the last day of the experiment was significant (p<0,02). The percentage of total liver lipids was higher in the GH, when compared with the GC (p<0,04). There was lower levels of cholesterol (p<0,01) and serum protein (0,005) in GH. The food consumed was not different between the groups. Conclusions: in this paper the low protein diet constitutes a model of NAFLD induction that can be characterized for serum protein and plasmatic cholesterol and increased fat in the liver, however not alterations in the glycemia suggest no changes in insulin sensitivity, thus constituting a defective model to study one of the main factors of risk for the establishment of the NAFLD, the resistance to insulin.