Trypanosoma cruzi discrete typing units in Chagas disease patients with HIV co-infection

BISIO M, CURA C, DUFFY T, ALTCHEH J, GIGANTI SALVADOR O, BEGHER S, SCAPELLATO PG, BURGOS JM, LEVIN MJ, SCHRECK R, FREILIJ H, SCHIJMAN AG

Revista Biomédica

Año: 2009 vol. 20

Natural populations of T. cruzi have been classified into six phylogenetic lineages or discrete typing units, T. cruzi I, IIa, IIb, IIc, IId, and IIe, believed to play a role in tissue tropism and disease pathogenesis. The impact of HIV infection in the T. cruzi genetic diversity in coinfected patients is a scarcely explored field of parasitology. To characterize parasitic lineages in clinical samples from patients co-infected with T. cruzi and HIV We analyzed blood and lesions samples from 25 patients residing in Argentina, namely 8 infants born to 7 HIV - T. cruzi co-infected mothers, 3 indeterminate adult chagasic patients with HIV co-infection and 7 presenting cerebral Chagas due to AIDS. Molecular diagnosis and monitoring of etiological treatment was carried out by PCR targeted to kinetoplastid (kDNA) and/or satellite sequences. T. cruzi lineages were identified by means of PCR targeted to the intergenic spacer of miniexon gene and 24s ribosomal ARN genes. To characterize the infra-lineage diversity, restriction fragment length polymorphism (RFLP) of KDNA amplicons was carried out. Out of the 7 co-infected mothers, two transmitted both HIV and T. cruzi to their siblings, four transmitted only T. cruzi. The remaining case was a pregnant woman with cerebral Chagas disease who entered into a coma being treated with benznidazole; she did not transmit congenital Chagas disease nor HIV to her newborn. Most bloodstream populations belonged to T. cruzi IId, with unique minicircle signatures for each patient´s strain, but identical signatures between strains from mothers and their congenitally infected infants. Mixtures of lineages T. cruzi I and T. cruzi IId were also detected. Differential tissue tropism of T. cruzi IIb and T. cruzi I was found in patients with cerebral chagas. Minicircle signatures showed complex patterns suggestive of polyclonal populations. The higher proportion of PCR positive samples suggests higher parasite loads that in chagasic population without HIV. The higher prevalence of T. cruzi IId in bloodstream is in agreement with previous findings in this region. The association of rare lineages at sites of encephalytis suggests differential tropism. The direct characterization of parasite lineages in clinical samples allowed identification of a higher prevalence of mixed infections, than previously assumed, from studies based on culture isolates.