Impact of dual infections on chemotherapeutic efficacy in balb/c mice infected with major genotypes of trypanosoma cruzi.
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2007
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The aim of this work was to investigate the impact of dual infections with stocks of Trypanosoma cruzi major
genotypes on benznidazole (BZ) treatment efficacy. For this purpose, T. cruzi stocks representative of the
genetic T. cruzi lineages, displaying different susceptibilities to BZ, belonging to the major T. cruzi genotypes
broadly dispersed in North and South America and important in Chagas’ disease epidemiology were used.
Therapeutic efficacy was observed in 27.8% of the animals treated. Following BZ susceptibility classification,
significant differences were observed in dual infections on the major genotype level, demonstrating that
combinations of genotypes 19 39 and genotypes 19 32 led to a shift in the expected BZ susceptibility profile
toward the resistance pattern. Analysis on the T. cruzi stock level demonstrated that 9 out of 24 dual infections
shifted the expected BZ susceptibility profile compared with the respective single infections, including shifts
toward lower and higher BZ susceptibilities. Microsatellite identification was able to identify a mixture of T.
cruzi stocks in 7.7% of the T. cruzi isolates from infected and untreated mice (6.9%) and infected and treated
but not cured mice (9.0%), revealing in some mixtures of BZ-susceptible and -resistant stocks that the T. cruzi
stock identified after BZ treatment was previously susceptible in single infections. Considering the clonal
structure and evolution of T. cruzi, an unexpected result was the identification of parasite subpopulations with
distinct microsatellite alleles in relation to the original stocks observed in 12.2% of the isolates. Taken together,
the data suggest that mixed infections, already verified in nature, may have an important impact on the efficacy
of chemotherapy.
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MARTINS, H. R. et al. Impact of dual infections on chemotherapeutic efficacy in balb/c mice infected with major genotypes of trypanosoma cruzi. Antimicrobial Agents And Chemotherapy, v. 51, p.3282-3289, 2007. Disponível em: <http://aac.asm.org/content/51/9/3282.full>. Acesso em: 10 jan. 2017.