Genotype diversity of Trypanosoma cruzi in small rodents and Triatoma sanguisuga from a rural area in New Orleans, Louisiana

Herrera, Claudia; Licon, Meredith H.; Nation, Catherine S.; Jameson, Samuel; Wesson, Dawn M.

doi:10.1186/s13071-015-0730-8

Cited by 61 publications

(60 citation statements)

References 45 publications

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“…14 The high frequency of non-TcI DTUs in Honduras and Mexico is in agreement with the recent findings of a greater diversity than previously reported in the T. cruzi DTUs circulating in Mexico and the US. 16,[40][41][42] It confirms the high frequency of non-TcI infections in Mexican patients determined by lineage-specific serology. 43 Our genotyping by PCR was limited to discriminating between TcI and non-TcI because of the very short sequence length of the marker used, and differences among non-TcI DTUs should be studied further.…”

Section: Discussionsupporting

confidence: 68%

Congenital Transmission of Trypanosoma cruzi in Argentina, Honduras, and Mexico: An Observational Prospective Study

Buekens

Cafferata²,

Alger³

et al. 2018

The American Journal of Tropical Medicine and Hygiene

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Compared with South America, there is a lack of epidemiologic studies about the risk of congenital transmission of in Central America and Mexico. It has been suggested that genotypes might differ by region and that congenital transmission might vary according to the parasite's genotype. Our objective was to compare congenital transmission rates in three countries. We performed an observational prospective study in 2011-2014 enrolling women at delivery in one hospital in Argentina, two hospitals in Honduras, and two hospitals in Mexico. Congenital infection was defined as the presence of one or more of the following criteria: presence of parasites in cord blood (direct parasitological microscopic examination) with positive polymerase chain reaction (PCR) in cord blood, presence of parasites in infant's blood at 4-8 weeks (direct parasitological microscopic examination), and persistence of -specific antibodies at 10 months, as measured by at least two tests. Among 28,145 enrolled women, 347 had at least one antibody rapid test positive in cord blood and a positive enzyme-linked immunosorbent assay in maternal blood. PCR in maternal blood was positive in 73.2% of the cases, and genotyping identified a majority of non-TcI in the three countries. We found no (0.0%; 95% confidence interval [CI]: 0.0, 2.0) confirmed congenital case in Honduras. Congenital transmission was 6.6% (95% CI: 3.1, 12.2) in Argentina and 6.3% (95% CI: 0.8, 20.8) in Mexico. non-TcI predominated and risks of congenital transmission were similar in Argentina and Mexico.

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Section: Discussionsupporting

confidence: 68%

Congenital Transmission of Trypanosoma cruzi in Argentina, Honduras, and Mexico: An Observational Prospective Study

Buekens

Cafferata²,

Alger³

et al. 2018

The American Journal of Tropical Medicine and Hygiene

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“…For example, it was believed that TcI DTU was largely predominant in Mexico and to some extent in Central America (over 95% of the strains), but recent studies have documented the presence of non‐TcI parasite strains in triatomines from different regions in Mexico and Central America at high frequencies (Ibanez‐Cervantes et al., ; Pennington, Paiz, Grajeda, & Cordon‐Rosales, ; Torres‐Montero, López‐Monteon, Dumonteil, & Ramos‐Ligonio, ), and a high proportion of patients appear to be infected with non‐TcI parasite strains (Risso et al., ). Similarly in the southern United States, initial work reported only TcI and TcIV DTUs (Roelling et al., ), but recent studies also indicate the presence of TcII DTUs in rodents (Herrera, Licon, Nation, Jameson, & Wesson, ), as well as the predominant presence of TcII‐TcV‐TcVI in autochthonous human cases (Garcia et al., ). Together, these observations indicate clearly that T. cruzi genotype distribution in Central and North America is still poorly understood (Brenière, Waleckx, & Barnabe, ).…”

Section: Trypanosoma Cruzi Diversity and Virulence Evolutionmentioning

confidence: 99%

Evolutionary ecology of Chagas disease; what do we know and what do we need?

Flores-Ferrer

Marcou

Waleckx

et al. 2017

Evolutionary Applications

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The aetiological agent of Chagas disease, Trypanosoma cruzi, is a key human pathogen afflicting most populations of Latin America. This vectorborne parasite is transmitted by haematophageous triatomines, whose control by large‐scale insecticide spraying has been the main strategy to limit the impact of the disease for over 25 years. While those international initiatives have been successful in highly endemic areas, this systematic approach is now challenged by the emergence of insecticide resistance and by its low efficacy in controlling species that are only partially adapted to human habitat. In this contribution, we review evidences that Chagas disease control shall now be entering a second stage that will rely on a better understanding of triatomines adaptive potential, which requires promoting microevolutionary studies and –omic approaches. Concomitantly, we show that our knowledge of the determinants of the evolution of T. cruzi high diversity and low virulence remains too limiting to design evolution‐proof strategies, while such attributes may be part of the future of Chagas disease control after the 2020 WHO's target of regional elimination of intradomiciliary transmission has been reached. We should then aim at developing a theory of T. cruzi virulence evolution that we anticipate to provide an interesting enrichment of the general theory according to the specificities of transmission of this very generalist stercorarian trypanosome. We stress that many ecological data required to better understand selective pressures acting on vector and parasite populations are already available as they have been meticulously accumulated in the last century of field research. Although more specific information will surely be needed, an effective research strategy would be to integrate data into the conceptual and theoretical framework of evolutionary ecology and life‐history evolution that provide the quantitative backgrounds necessary to understand and possibly anticipate adaptive responses to public health interventions.

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“…DTU TcII is also a widely distributed genotype and it has been found to infect several mammalian taxa in distinct habitats and biomes [35][36][37]. Although DTUs TcIII and TcIV are widely distributed and may infect a wide variety of mammals, they appear to occur at significantly lower rates, most likely because they are maintained in very low parasitemia in nature, which hampers their detection [23,32].…”

Section: Discussionmentioning

confidence: 99%

Trypanosomatids in Small Mammals of an Agroecosystem in Central Brazil: Another Piece in the Puzzle of Parasite Transmission in an Anthropogenic Landscape

et al. 2019

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We surveyed infection by Trypanosoma spp. and Leishmania spp. in small wild mammals from Cumari, Goiás State aiming to investigate the diversity of trypanosomatid in a modified landscape of the Brazilian Cerrado (and possible infection overlapping with canids from the same area). Blood, skin, spleen, and liver samples were collected for parasitological, serological, and molecular assays. Gracilinanus agilis was the most abundant species (N = 70; 48.6%) and it was the only one with patent parasitemia. Characterization by mini-exon and 18SrDNA targets were achieved in 7/10 hemocultures with positive fresh blood examination, which confirmed the T. cruzi infection by Discrete Typing Units (DTU) TcI in single (N = 2) and mixed infections with other DTUs (N = 5). T. rangeli and T. dionisii were detected in skin fragments from Didelphis albiventris and Oecomys cleberi, respectively. G. agilis were found to be infected by L. braziliensis and L. guyanensis, while Leishmania sp. DNA was detected in the liver of Oligoryzomys nigripes and Calomys expulsus. Subpatent infection by T. cruzi and Leishmania sp. was serologically detected in 15% and 9% of the small mammal fauna, respectively. Small mammals from Cumari are included in T. cruzi and Leshmania spp. transmission cycles, showing a higher diversity of trypanosomatid species and/or genotypes than that observed in canids of the same agroecosystem.

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Genotype diversity of Trypanosoma cruzi in small rodents and Triatoma sanguisuga from a rural area in New Orleans, Louisiana

Cited by 61 publications

References 45 publications

Congenital Transmission of Trypanosoma cruzi in Argentina, Honduras, and Mexico: An Observational Prospective Study

Congenital Transmission of Trypanosoma cruzi in Argentina, Honduras, and Mexico: An Observational Prospective Study

Evolutionary ecology of Chagas disease; what do we know and what do we need?

Trypanosomatids in Small Mammals of an Agroecosystem in Central Brazil: Another Piece in the Puzzle of Parasite Transmission in an Anthropogenic Landscape

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