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Muscle damage and autoantibody fixation in an experimental model of autoimmune myopathy
Losada, Mercedes; Wangüemert, Ana Marina; Torres, Sonia H; Hernández, Noelina; Rivas, Miriam; Bravo, Carlos; Pulido, María Magdalena.
  • Losada, Mercedes; Central University of Venezuela. Faculty of Medicine. Institute of Experimental Medicine. Caracas. VE
  • Wangüemert, Ana Marina; Central University of Venezuela. Faculty of Medicine. Institute of Experimental Medicine. Caracas. VE
  • Torres, Sonia H; s.af
  • Hernández, Noelina; Central University of Venezuela. Faculty of Medicine. Institute of Experimental Medicine. Caracas. VE
  • Rivas, Miriam; Central University of Venezuela. Faculty of Medicine. Institute of Experimental Medicine. Caracas. VE
  • Bravo, Carlos; Central University of Venezuela. Faculty of Medicine. Institute of Experimental Medicine. Caracas. VE
  • Pulido, María Magdalena; Central University of Venezuela. Faculty of Medicine. Institute of Experimental Medicine. Caracas. VE
Acta cient. venez ; 53(4): 290-296, 2002. ilus, tab, graf
Article Dans Anglais | LILACS | ID: lil-343949
ABSTRACT
An experimental model of autoimmune myopathy was designed using parental antigens (muscle mitochondrial fraction) inF1 hybrid rats (male Wistar female Sprague-Dawley). The immune response was modulated by spleen fragment transplant from either Wistar (W) or F1. Antibody fixation and inflammatory reaction were studied in Extensor digitorum longus and soleus muscles. Immunizationwithout spleen transplant resulted in antibody fixation mainly in capillaries and incompletely around muscle fibers; whorled fibers were found in 1/3 of F1 rats immunized with antigen from W rats. Spleen transplants from Sprague Dawley (SD) rats were usually accepted by F1;in some animals, antibodies surrounded completely muscle fibers and the percentage of animals showing soleus muscle lesions was increased. Spleen transplants from non immunized F1 were usually rejected by immunized F1; antibody reaction was found inside fibers of most of the rats, muscle damage was present in 40% of the animals immunized with W, but absent in those immunized with SD antigen. In conclusion, this model can be used to study immunological responses to alloantigens (parental to F1). Spleen fragment transplant modulates the immune response. There was discrepancy between antibody fixation and muscle damage. The immunological response was different according to muscle fiber type composition and/or microcirculatory characteristics.
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Indice: LILAS (Amériques) Sujet Principal: Autoanticorps / Maladies auto-immunes / Muscles / Maladies musculaires Type d'étude: Étude pronostique Limites du sujet: Animaux langue: Anglais Texte intégral: Acta cient. venez Thème du journal: Science Année: 2002 Type: Article Pays d'affiliation: Venezuela Institution/Pays d'affiliation: Central University of Venezuela/VE

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Indice: LILAS (Amériques) Sujet Principal: Autoanticorps / Maladies auto-immunes / Muscles / Maladies musculaires Type d'étude: Étude pronostique Limites du sujet: Animaux langue: Anglais Texte intégral: Acta cient. venez Thème du journal: Science Année: 2002 Type: Article Pays d'affiliation: Venezuela Institution/Pays d'affiliation: Central University of Venezuela/VE