Antioxidant Role of Vitamin E in Atherogenesis Induced by Hyperfibrinogenemia

Candelaria Llorens; Ma. del Carmen Baez; Mariana Taran; Vilma Campana; Ismael Fonseca; Elsa Oyola; Jose Palma; Monica Moya

Ayuda

Antioxidant Role of Vitamin E in Atherogenesis Induced by Hyperfibrinogenemia

Llorens, Candelaria ^[1] ; Baez, Ma. del Carmen ; Taran, Mariana ; Campana, Vilma ; Fonseca, Ismael ; Oyola, Elsa ; Palma, Jose ; Moya, Monica
1. [1] Universidad Nacional de Córdoba
  
  Universidad Nacional de Córdoba
  
  Argentina
Localización: Revista Argentina de Cardiología (RAC), ISSN-e 1850-3748, ISSN 0034-7000, Vol. 78, Nº. 5, 2010, págs. 405-410
Idioma: inglés
Títulos paralelos:
- Papel antioxidante de la vitamina E en la aterogénesis inducida por hiperfibrinogenemia
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Resumen
- español
  Con el propósito de estudiar el efecto de la vitamina E sobre el estrés oxidativo desencade- nado por hiperfibrinogenemia (HF) en un modelo experimental de aterogénesis y la posible normalización de los indicadores de estrés oxidativo, se evaluaron: óxido nítrico (NO), L-citrulina, superóxido dismutasa (SOD) e involución de lesiones histopatológicas en la aorta torácica. El estudio se realizó en 36 ratas, cepa Wistar, que se dividieron en tres grupos (n = 12 cada uno): A, control; B, HF × 90 días; C, HF × 90 días + vitamina E. La HF se indujo mediante inyecciones de adrenalina (0,1 ml/día/rata) por 90 días. La dosis de vitamina E fue de 2 mg/día/rata durante 75 días. Se dosaron en plasma los niveles de fibrinógeno (mg/dl), NO (uM) y L-citrulina (mM) y en lisado de glóbulos rojos, por espectrofotometría, se determinó la actividad de la SOD (U/ml). Se analizaron cortes de la aorta torácica por microscopia óptica (MO). Rev Argent Cardiol 2010;78:405-410.
- English
  We used an experimental model of atherogenesis to evaluate the effect of vitamin E on oxidative stress induced by hyperfibrinogenemia (HF) and the possible normalization of oxidative stress markers. The following variables were studied: nitric oxide (NO), L-citrulline, superoxide dismutase (SOD) activity and regression of histopathological lesions in the thoracic aorta. The study was performed in 36 Wistar rats that were divided into three groups of 12 rats each: A, control group; B, HF for 90 days; C, HF for 90 days + vitamin E. Hyperfibrinogenemia was induced by the injection of epinephrine (0.1 ml/day/rat) during 90 days. The dose of vitamin E was 2 mg/day/rat during 75 days. We measured the plasma levels of fibrinogen (mg/dl), NO (uM) and L-citrulline (mM); SOD activity (U/ml) was assayed in red cell lysates using spectrophotometry. The histopathological sections of the thoracic aorta were examined using light microscopy (LM). Statistical analysis was performed using MANOVA and Fisher’s test; a p value <0.05 was considered statistically significant. Rats in group B had a significant increase in fibrinogen levels B (407±8.9 mg/dl) compared to groups A (203±9 mg/dl) and C (191.58±17.79 mg/dl) (p<0.001). We observed a significant decrease in NO in group B (13.73±1.76 uM) versus groups A (23.58±0.08 uM) and C (26.64±3.65 uM) (p<0.001). L-citrulline increased significantly in groups B (4.99±0.18 mM) and C (6.60±0.16 mM) compared to group A (3.03±0.13 mM) (p<0.001). SOD activity was greater in groups B (251.67±10.34 U/ml) and C (304.75±10.43 U/ml) versus group A (139.44±4.74 U/ml) (p<0.001). Light microscopic examination revealed the presence of endothelial denudation, intimal thickening and vessel wall protrusion in group B (90%), while recovery of endothelial denudation and a 50% reduction in intimal thickening was observed in group C (p<0.001). High SOD activity might be insufficient to prevent abnormalities in the oxidative stress pathway induced by HF. Vitamin E would stop the chain reaction initiated by free radicals and thus decrease the superoxide anion, stimulating the bioavailability of NO with normalization of fibrinogen plasma levels.