AI Article Synopsis
- The study investigates the treatment failure of oral Chagas disease (oCD) in Venezuela, despite close supervision of patients receiving nitroheterocyclic drugs since its emergence in 2007.
- Researchers analyzed blood samples and hemoculture isolates from nine patients, identifying significant genetic variability in parasite populations before and after treatment.
- Findings suggest a connection between poor drug response and the presence of resistant parasite clones, emphasizing the importance of understanding drug susceptibility for effective treatment guidelines in the region.
Article Abstract
The oral transmission of Chagas disease (oCD) in Venezuela announced its appearance in 2007. Different from other populations affected by oCD and despite close supervision during treatment with nitroheterocyclic drugs, the result was treatment failure. We studied genetic features of natural bloodstream parasite populations and populations after treatment of nine patients of this outbreak. In total, we studied six hemoculture isolates, eight Pre-Tx blood samples, and 17 samples collected at two or three Post-Tx time-points between 2007 and 2015. Parasitic loads were determined by quantitative polymerase chain reaction (qPCR), and discrete typing units (DTU), minicircle signatures, and gene sequences were searched from blood samples and hemocultures. Half-maximal inhibitory concentration (IC) values were measured from the hemocultures. All patients were infected by TcI. Significant decrease in parasitic loads was observed between Pre-Tx and Post-Tx samples, suggesting the evolution from acute to chronic phase of Chagas disease. 60% of intra-DTU-I variability was observed between Pre-Tx and Post-Tx minicircle signatures in the general population, and 43 single-nucleotide polymorphisms (SNPs) were detected in a total of 12 gene sequences, indicative of a polyclonal source of infection. SNPs in three post-Tx samples produced stop codons giving rise to putative truncated proteins or displaced open reading frames, which would render resistance genes. IC values varied from 5.301 ± 1.973 to 104.731 ± 4.556 μM, demonstrating a wide range of susceptibility. The poor drug response in the Pre-Tx parasite populations may be associated with the presence of naturally resistant parasite clones. Therefore, any information that can be obtained on drug susceptibility from in vitro assays, in vivo assays, or molecular characterization of natural populations of becomes essential when therapeutic guidelines are designed in a given geographical area.
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