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Vaccination with Trypanosoma rangeli modulates the profiles of immunoglobulins and IL-6 at local and systemic levels in the early phase of Trypanosoma cruzi experimental infection
Marini, Vanina; Moretti, Edgardo; Bermejo, Daniela; Basso, Beatriz.
Affiliation
  • Marini, Vanina; Laboratorio de la Coordinación Nacional de Control de Vectores. Córdoba. AR
  • Moretti, Edgardo; Laboratorio de la Coordinación Nacional de Control de Vectores. Córdoba. AR
  • Bermejo, Daniela; Universidad Nacional de Córdoba. Facultad de Ciencias Químicas. Departamento de Bioquímica Clínica. Córdoba. AR
  • Basso, Beatriz; Laboratorio de la Coordinación Nacional de Control de Vectores. Córdoba. AR
Mem. Inst. Oswaldo Cruz ; 106(1): 32-37, Feb. 2011. ilus, graf, tab
Article ي En | LILACS | ID: lil-578813
المكتبة المسؤولة: BR1.1
ABSTRACT
In America, there are two species of Trypanosoma that can infect humans Trypanosoma cruzi, which is responsible for Chagas disease and Trypanosoma rangeli, which is not pathogenic. We have developed a model of vaccination in mice with T. rangeli epimastigotes that protects against T. cruzi infection. The goal of this work was to study the pattern of specific immunoglobulins in the peritoneum (the site of infection) and in the sera of mice immunized with T. rangeli before and after challenge with T. cruzi. Additionally, we studied the effects triggered by antigen-antibodies binding and the levels of key cytokines involved in the humoral response, such as IL-4, IL-5 and IL-6. The immunization triggered the production of antibodies reactive with T. cruzi in peritoneal fluid (PF) and in serum, mainly IgG1 and, to a lesser magnitude, IgG2. Only immunized mice developed specific IgG3 antibodies in their peritoneal cavities. Antibodies were able to bind to the surface of the parasites and agglutinate them. Among the cytokines studied, IL-6 was elevated in PF during early infection, with higher levels in non-immunized-infected mice. The results indicate that T. rangeli vaccination against T. cruzi infection triggers a high production of specific IgG isotypes in PF and sera before infection and modulates the levels of IL-6 in PF in the early periods of infection.
الموضوعات
Key words

النص الكامل: 1 الفهرس: LILACS الموضوع الرئيسي: Immunoglobulins / Antibodies, Protozoan / Protozoan Vaccines / Chagas Disease / Trypanosoma rangeli / Antigens, Protozoan المحددات: Animals اللغة: En مجلة: Mem. Inst. Oswaldo Cruz موضوع المجلة: MEDICINA TROPICAL / PARASITOLOGIA السنة: 2011 نوع: Article

النص الكامل: 1 الفهرس: LILACS الموضوع الرئيسي: Immunoglobulins / Antibodies, Protozoan / Protozoan Vaccines / Chagas Disease / Trypanosoma rangeli / Antigens, Protozoan المحددات: Animals اللغة: En مجلة: Mem. Inst. Oswaldo Cruz موضوع المجلة: MEDICINA TROPICAL / PARASITOLOGIA السنة: 2011 نوع: Article