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Comparative pathogenicity in Swiss mice of Trypanosoma cruzi IV from northern Brazil and Trypanosoma cruzi II from southern Brazil. | LitMetric

AI Article Synopsis

  • Chagas disease (ChD) shows geographical variations largely due to the genetic differences of the parasite Trypanosoma cruzi, especially between its lineages known as Discrete Typing Units (DTUs).
  • The study tested the pathogenicity of two T. cruzi lineages in mice: DTU IV (TcIV) from Amazonas and DTU II (TcII) from Paraná, revealing that TcIV was less virulent with significantly lower parasitemia than TcII.
  • Results indicated that mice infected with TcIV experienced fewer inflammatory responses, supporting the hypothesis that the TcIV strain is less pathogenic and correlating to milder human Chagas disease cases in the Amazon

Article Abstract

The geographical heterogeneity of Chagas disease (ChD) is mainly caused by genetic variability of the etiological agent Trypanosoma cruzi. Our hypothesis was that the pathogenicity for mice may vary with the genetic lineage (or Discrete Typing Unit - DTU) of the parasite. To test this hypothesis, parasitological and histopathological evaluations were performed in mice inoculated with strains belonging to the DTU T. cruzi IV (TcIV) from the State of Amazonas (northern Brazil), or the DTU T. cruzi II (TcII) from the State of Paraná (southern Brazil). Groups of 10 Swiss mice were inoculated with eight strains of TcIV obtained from acute cases (7) from two outbreaks of orally acquired ChD, and from the triatomine Rhodnius robustus (1) from Amazonas; and three strains of TcII obtained from chronic patients in Paraná. We evaluated the pre-patent period, patent period, maximum peak of parasitemia, day of maximum peak of parasitemia, area under the parasitemia curve, inflammatory process, and tissue parasitism in the acute phase. TcIV was less virulent than TcII, and showed significantly (p < 0.005) lower parasitemia levels. Although the levels of tissue parasitism did not differ statistically, mice infected with TcIV displayed significantly (p < 0.001) fewer inflammatory processes than mice infected with TcII. This supported the working hypothesis, since TcIV from Amazonas was less pathogenic than TcII from Paraná; and agreed with the lower severity of human cases of ChD in the Amazon region.

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http://dx.doi.org/10.1016/j.exppara.2014.08.014DOI Listing

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