Evaluación de Toxoplasma gondii en llamas hembras de dos comunidades campesinas de la región de Puno / Evaluation of toxoplasma gondii in female llamas from two peasant communities in Puno

El objetivo del estudio fue determinar la presentación de Toxoplasma gondii en llamas hembras en edad reproductiva de dos comunidades campesinas de la provincia de Melgar, Puno. Se colectó muestras de sangre a 30 y 77 llamas de las comunidades de Huaycho y Huataywasi. Las muestras se procesaron con la técnica de inmunofluorescencia indirecta. La seroprevalencia hallada frente a T. gondii fue de 36.7% en Huaycho y 6.5% en Huataywasi. Ambas explotaciones presentaban condiciones y sistemas de manejo disímiles, por lo que el tipo de explotación, sistema de manejo y la presencia de hospedero definitivo influirían en la presentación de T. gondiien el ganado.

The objective the study was to determine the seroprevalence of Toxopasma gondii in adult female llamas from two peasant communities from the province of Melgar, Puno. Blood samples were collected in 30 and 77 llamas from Huaycho and Huataywasi communities. Samples were analyzed by the indirect immunofluorescent test. The seroprevalence to T. gondii was 36.7% in Huaycho and 6.5% in Huataywasi. Both communities showed different conditions and management systems, which can explain the high differences in seroprevalence.

La sobredosis de paracetamol y la colestasis experimental inducen la expresión de los genes que codifican la P-glicoprotína tipo 1 en ratas / Paracetamol overdose and experimental cholestasis induced gene expresion that codified P-glicoprotein tipe 1 in rats

Excretion of lipophilic cationic toxic compounds from the interior of the hepatocyte to the bile is mediated by P-Glycoprotein. It is an integral protein located in the bile canaliculi. The present work study the hepatic expression of P-Glycoprotein in different models of experimental liver disease: Acute paracetamol intoxication, extrahepatic cholestasis and cholestasis followed by acute paracetamol intoxication. mRNA was isolated from liver tissue, and the expression of Pg-p was assessed by Northern blot. It is concluded that the hepatic expression of mdr1b is increased in the experimental liver diseases when compared to controls. On the other hand, mdr2 expression was similar between the different groups (AU)

La sobredosis de paracetamol y la colestasis experimental inducen la expresión de los genes que codifican la P-glicoprotína tipo 1 en ratas / Paracetamol overdose and experimental cholestasis induced gene expresion that codified P-glicoprotein tipe 1 in rats

Excretion of lipophilic cationic toxic compounds from the interior of the hepatocyte to the bile is mediated by P-Glycoprotein. It is an integral protein located in the bile canaliculi. The present work study the hepatic expression of P-Glycoprotein in different models of experimental liver disease: Acute paracetamol intoxication, extrahepatic cholestasis and cholestasis followed by acute paracetamol intoxication. mRNA was isolated from liver tissue, and the expression of Pg-p was assessed by Northern blot. It is concluded that the hepatic expression of mdr1b is increased in the experimental liver diseases when compared to controls. On the other hand, mdr2 expression was similar between the different groups

[Paracetamol overdose and experimental cholestasis induced gene expression regulation that codified P-Glycoprotein type 1 in rats]. / La sobredosis de paracetamol y la colestasis experimental inducen la expresión de los genes que codifican la P-glicoprotína tipo 1 en ratas.

Excretion of lipophilic cationic toxic compounds from the interior of the hepatocyte to the bile is mediated by P-Glycoprotein. It is an integral protein located in the bile canaliculi. The present work study the hepatic expression of P-Glycoprotein in different models of experimental liver disease: Acute paracetamol intoxication, extrahepatic cholestasis and cholestasis followed by acute paracetamol intoxication. mRNA was isolated from liver tissue, and the expression of Pg-p was assessed by Northern blot. It is concluded that the hepatic expression of mdr1b is increased in the experimental liver diseases when compared to controls. On the other hand, mdr2 expression was similar between the different groups.

La sobredosis de paracetamol y la colestasis experimental inducen la expresión de los genes que codifican la P-glicoprotína tipo 1 en ratas. / [Paracetamol overdose and experimental cholestasis induced gene expression regulation that codified P-Glycoprotein type 1 in rats]

Excretion of lipophilic cationic toxic compounds from the interior of the hepatocyte to the bile is mediated by P-Glycoprotein. It is an integral protein located in the bile canaliculi. The present work study the hepatic expression of P-Glycoprotein in different models of experimental liver disease: Acute paracetamol intoxication, extrahepatic cholestasis and cholestasis followed by acute paracetamol intoxication. mRNA was isolated from liver tissue, and the expression of Pg-p was assessed by Northern blot. It is concluded that the hepatic expression of mdr1b is increased in the experimental liver diseases when compared to controls. On the other hand, mdr2 expression was similar between the different groups.

Síndrome HELLP / HELLP syndrome

Objetivo: Describir las características clínicas y las complicaciones maternoperinatales del síndrome HELLP. Diseño: Estudio retrospectivo descriptivo. Material y método: casos de síndrome HELLP atendidos en el Hospital Nacional Guillermo Almenara Irigoyen (HNGAI) en 1999. Resultados: La incidencia de síndrome HELLP fue 16,3 por 1000 nacidos vivos, 16(41 por ciento) con criterios completos y 23 (58,9 por ciento) con HELLP parcial. Se registró epigastralgia y dolor en hipocondrio derecho en 46,2 por ciento de pacientes, asociándose con mayor trombocitopenia (OR igual 5, p menor 0,001). Las complicaciones obstétricas principales fueron coagulación intravascular diseminada 17(43,6 por ciento), insuficiencia respiratoria aguda 14 (35,9 por ciento), desprendimiento prematuro de placenta 9 (23,1) y eclampsia 4 (10,3 por ciento). Las complicaciones en el HELLP parcial fueron menores. Se culminó la gestación en 63 por ciento de pacientes entre las 33 y 37 semanas, 95 por ciento por cesárea. Se usó hemoderivados en 67 por ciento, conforme a la severidad de la trombocitopenia. La morbilidad perinatal consistió en 28 (76 por ciento) prematuros y 19(15 por ciento) recién nacidos de peso bajo al nacer. La mortalidad materna fue 0 por ciento y la perinatal 14 por ciento, esta última se asocia a la prematuridad (OR igual 10, p menor 0,005). En la evolución de la plaquetopenia hubo una reducción máxima durante las primeras 48 horas postparto, hasta una recuperación plaquetaria espontánea a los siete días. Los corticoides ejercerían un efecto beneficioso en el adelanto de esta recuperación. Conclusión: El síndrome HELLP es una entidad de alta morbimortalidad maternoperinatal. Las complicaciones obstétricas se asocian a la mayor trombocitopenia, mientras que las perinatales a la prematuridad. El manejo medicoquirúrgico y el soporte de cuidados intensivos reducen las complicaciones asociadas a esta entidad.