Chemotherapy with Benznidazole and Itraconazole for mice infected with different Trypanosoma cruzi clonal genotypes.
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2003
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The benznidazole (BZ) and itraconazole (ITC) susceptibilities of a standard set of Trypanosoma cruzi natural
stocks were evaluated during the acute phase and the chronic phase of experimental chagasic infection in
BALB/c mice. Twenty laboratory-cloned stocks representative of the total phylogenetic diversity of T. cruzi,
including genotypes 20 and 19 (T. cruzi I) and genotypes 39 and 32 (T. cruzi II), were analyzed. Our results
demonstrate important differences among stocks that could be pointed out as markers of biological behavior.
Members of the T. cruzi I group were highly resistant to both BZ and ITC, whereas members of the T. cruzi II
group were partially resistant to both drugs, despite their susceptibilities to ITC during the chronic phase of
infection. The resistance to BZ observed for T. cruzi I was mainly triggered by genotype 20 isolates, whereas
resistance to ITC was due to both genotype 20 and 19 isolates. Two polar patterns of response to BZ observed
for genotype 39 isolates had a major impact on the partial resistance pattern observed for members of the T.
cruzi II group. Genotype 32 isolates showed a typical profile of susceptibility. The correlation between the
response to treatment and phylogenetic classification of T. cruzi stocks was clearer for ITC than for BZ. In
conclusion, the data presented show a correlation between phylogenetic divergence among T. cruzi stocks and
their susceptibilities to chemotherapeutic agents in vivo. Our results warn of the necessity to take into account
the lesser genetic subdivisions of T. cruzi stocks since the upper subdivisions (T. cruzi I and II) show a great
deal of heterogeneity for in vivo drug susceptibility.
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TOLEDO, M. J. de O. et al. Chemotherapy with Benznidazole and Itraconazole for mice infected with different Trypanosoma cruzi clonal genotypes. Antimicrobial Agents And Chemotherapy, v. 47, n. 01, p.223-230, 2003. Disponível em: <http://aac.asm.org/content/47/1/223.long>. Acesso em: 10 jan. 2017.