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1.
Mansoura Medical Journal. 2008; 39 (3, 4): 165-178
em Inglês | IMEMR | ID: emr-100888

RESUMO

Similarities in clinical picture between manganese toxicity and chronic hepatic encephalopathy suggest that this metal may have a role in the pathogenesis of chronic hepatic encephalopathy. As, dietary manganese is normally cleared by liver, we hypothesized that hepatic dysfunction could lead to manganese overload with its abnormal deposition in brain tissues that account for magnetic resonance imaging [MRI] signal hyperintenisity seen in these patients. To examine the phenomenon of manganese overload in an experimental model of cirrhotic rats and to determine the importance of a normal liver function as a natural barrier agairst the development of manganese overload with its hazardous neuropsychatric sequels in chronic hepatic disease We induced liver cirrhosis in a group of rats to examine the phenomenon of manganese overload in experimental models of cirrhotic rats. We made use also of a healthy group of rats that was fed a manganese enriched food for 4 weeks. The !eve of manganese in blood and brain tissues was assayed by atomic absorption spectrometry. There was a significant increase in both blood and brain manganese level in cirrhotic rats when compared to normal control group. The blood and brain level of manganese did not change significantly in healthy rats that fed high manganese enriched food when compared to control rats. These findings support the hypothesis that normal liver function is of utmost importance as a barrier against the development of manganese overload. Chronic hepatobiliary dysfunction might lead to manganese overload. Further studies in cirrhotic rats could be useful because the use of chelating agent and! or treatment of dopaminergic deficit could prove to be a new therapeutic option to prevent or reverse this neuropsychatric syndrome in chronic liver disease


Assuntos
Animais de Laboratório , Fígado , Cirrose Hepática Experimental , Manganês/sangue , Encéfalo , Espectrofotometria Atômica , Testes de Função Hepática , Ratos , Manifestações Neurológicas
2.
Benha Medical Journal. 2001; 18 (3): 105-116
em Inglês | IMEMR | ID: emr-56439

RESUMO

The essential constituents of a conventional oral rehydration solution [ORS] are sodium, glucose and a bicarbonate precursor. The glucose promotes sodium uptake but because these solutions are isotonic, it is insufficient to sustain calorie requirements. This paper examines the efficacy of a novel ORSs with twice and three times the conventional glucose concentration, by comparing it with the WHO-ORS in an experimental model of chromic diarrhea in rats. Rats were either treated or not for one weak with magnesium citrate- phenolphthalein to produce chronic osmotic- secretory diarrhea. Intestinal absorption of fluids and solutes were measured using in vivo intestinal perfusion method. Plasma changes were evaluated 4 hours after the beginning of intestinal perfusion. Inclusion of additional glucose enhances fluids and solutes absorption, though, absorption of the ORS containing twice the conventional glucose concentration of WHO-ORS was superior to ORS with three times the conventional glucose concentration. Novel hgpertonic solutions showed also greater ability to correct hypoglycemia, hyponatremia metabolic acidosis in diarrheal rats. It, therefore, appears possible to depart from the traditional isotonic formulations in cases of long standing diarrhea and gain significant nutritional support while retaining effective intestinal absorption and correction of acidbase and electrolyte disturbances. This seems especially important in infants where energy deprivation imposes a particular penalty. The use of a novel ORSs should not, however, be extended to other species without further research


Assuntos
Masculino , Animais de Laboratório , Doença Crônica , Soluções para Reidratação , Hidratação , Solução Hipertônica de Glucose , Ratos , Potássio , Bicarbonatos , Concentração de Íons de Hidrogênio
3.
Egyptian Journal of Surgery [The]. 1996; 15 (1): 109-114
em Inglês | IMEMR | ID: emr-40652
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