Use of Trypanosoma Cruzi Purified Glycoprotein (GP57/51) or Trypomastigote-Shed Antigens to Assess Cure for Human Chagas' Disease

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Am. J. Trop. Med. Hyg., 49(5), 1993, pp. 625-635
Copyright © 1993 by The American Society of Tropical Medicine and Hygiene

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Use of Trypanosoma Cruzi Purified Glycoprotein (GP57/51) or Trypomastigote-Shed Antigens to Assess Cure for Human Chagas' Disease

Ricardo T. Gazzinelli, Lucia M. C. Galvao, Greice Krautz, Ana Paula C. A. Lima, Joaquin-Romeu Cancado, Julio Scharfstein AND Antoniana U. Krettli
Centro de Pesquisas Rene Rachou Fiocruz, Belo Horizonte, Brazil; Escola de Medicina and Departamento de Parasitologia, ICB, Universidade Federal de Minas Gerais, Belo Horizonte, Brazil; Instituto de Biofisica Carlos Chagas Filho da Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brazil

With the exception of assays for the detection of antibodiespromoting complement-mediated lysis of Trypanosoma cruzi, serologictests have generally failed to assess the effectiveness of chemotherapyfor Chagas' disease. Conventional serology, although usefulfor the diagnosis of infection, is not capable of determiningwhich patients have been cured. Here we demonstrate that a highproportion of antibodies detected by conventional serology (usingfixed epimastigotes or trypomastigotes or crude extracts obtainedtherefrom) are directed against the carbohydrate residue galactosyl ${alpha}$ 1->3galactose (Gal ${alpha}$ 1->3 Gal), a determinant also recognized byantibodies from noninfected healthy volunteers. In a study of14 cured patients with long-term followup, we found that thepersistently positive reactions detected using conventionalserology were largely eliminated following immunoadsorptionwith melibiose. Because of their wide distribution among microorganismsof intestinal and pulmonary microflora, these carbohydrate determinantsmay keep stimulating lymphocytes previously primed by T. cruziGal ${alpha}$ 1->3 Gal epitopes, thereby accounting for false-positiveresults in cured patients. Consistent with this proposition,enzyme-linked immunosorbent assays performed with two distinctT. cruzi antigen preparations that lack the Gal ${alpha}$ 1->3 Gal epitope,namely purified GP57/51 and trypomastigoteshed antigens, wereindeed capable of determining a cure after chemotherapy, albeitto a different degree. Collectively, the data indicate thatconventional immunoassays prepared with highly specific T. cruziantigens can be useful in the assessment of a cure after chemotherapy.