Action of Trypanosoma rangeli in infections with virulent Trypanosoma cruzi populations

Palau, M. T.; Mejía, Ángel María Giraldo; Vergara, U; Zúñiga, CA

doi:10.1590/s0074-02762003000400022

Cited by 22 publications

(23 citation statements)

References 36 publications

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“…These results, which agree with the findings of other studies, show that human infection with T. rangeli does not cause the production of enough cross-reacting antibodies to interfere with the serodiagnosis of Chagas' disease (13,14). However, this does not exclude the possibility that exposure to T. rangeli may elicit a particular humoral and/or cellular immune response that confers some degree of protection against subsequent infection with T. cruzi (11).…”

supporting

confidence: 89%

Evaluation of Serological Tests To Identify Trypanosoma cruzi Infection in Humans and Determine Cross-Reactivity with Trypanosoma rangeli and Leishmania spp

Caballero

Sousa

Marques

et al. 2007

Clin Vaccine Immunol

153

157

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Five commercially available enzyme-linked immunosorbent assays (ELISAs), one in-house ELISA, and two hemagglutination assays were evaluated to determine their diagnostic accuracy for Chagas' disease in two studies. In study 1, ELISA kits showed 100% sensitivity, but specificities ranged from 82.84% to 100% when leishmaniasis cases were included and from 95.57% to 100% when leishmaniasis cases were excluded. Kits using recombinant antigens or synthetic peptides are more specific than those using crude extracts from Trypanosoma cruzi epimastigote forms. Kits evaluated in Panama, in study 2, showed 75% to 100% sensitivity and 97.12% to 100% specificity. These data were obtained by using a Western blot assay with T. cruzi trypomastigote excreted-secreted antigens as a reference test to confirm T. cruzi infection.

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supporting

confidence: 89%

Evaluation of Serological Tests To Identify Trypanosoma cruzi Infection in Humans and Determine Cross-Reactivity with Trypanosoma rangeli and Leishmania spp

Caballero

Sousa

Marques

et al. 2007

Clin Vaccine Immunol

153

157

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“…A diferencia de T. cruzi, T. rangeli secreta copiosamente las sialidasas en el intestino de los vectores, lo cual podría afectar la microbiota bacteriana del insecto y generar un efecto patógeno para el vector (Stoco, et al, 2014). Algunos investigadores consideran que en las regiones donde T. rangeli coexiste con T. cruzi en los mismos vectores y vertebrados, las infecciones de T. rangeli podrían alterar el curso de la enfermedad de Chagas en los vertebrados (Paláu, et al, 2003), pues se ha observado que la vacunación de ratones, cobayos y perros con T. rangeli induce protección inmunitaria contra cepas virulentas de T. cruzi (Basso, et al, 2007;Basso, et al, 2008Basso, et al, , 2014, lo que abre nuevas perspectivas para el control de la enfermedad de Chagas en los reservorios domésticos y, probablemente, en los humanos.…”

Section: Conclusionesunclassified

Trypanosoma rangeli: un protozoo infectivo y no patógeno para el humano que contribuye al entendimiento de la transmisión vectorial y la infección por Trypanosoma cruzi, agente causal de la enfermedad de Chagas

Vallejo

Suárez

Olaya

et al. 2015

Rev. Acad. Colomb. Cienc. Ex. Fis. Nat.

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T. rangeli: modelo para la transmisión vectorial e infección por T. cruzi111 Rev. Acad. Colomb. Cienc. Ex. Fis. Nat. 39(150):111-122, enero-marzo de 2015 Trypanosoma rangeli: un protozoo infectivo y no patógeno para el humano que contribuye al entendimiento de la transmisión vectorial y la infección por Trypanosoma cruzi, agente causal de la enfermedad de Chagas Gustavo ResumenA diferencia de Trypanosoma cruzi, agente causal de la enfermedad de Chagas, Trypanosoma rangeli es un parásito infectivo y no patógeno para el humano, pero sí para los vectores del género Rhodnius. Con base en polimorfismos del ADN del cinetoplasto (kADN), del gen miniexón o líder de empalme (Spliced Leader), del espaciador interno transcrito (ITS) y de la subunidad pequeña del ribosoma (SSU rARN), se han descrito varios genotipos de T. rangeli (KP1+/A, B, KP1-/C, KP1-/D y E), los cuales son transmitidos selectivamente por dos líneas filogenéticas de Rhodnius, lo que indica la ocurrencia de procesos coevolutivos entre el parásito y los vectores. La línea Robustus (Rhodnius prolixus, Rhodnius robustus y Rhodnius neglectus) transmite exclusivamente el genotipo KP1+/A y la línea Pallescens (Rhodnius pallescens, Rhodnius colombiensis y Rhodnius ecuadoriensis) transmite el genotipo KP1-/C. Aunque el conocimiento de las bases moleculares de la interacción parásito-vector es todavía escaso, este trabajo presenta observaciones inéditas sobre la capacidad de los genotipos KP1+/A y KP1-/C para completar el ciclo de vida en algunas de las 19 especies de Rhodnius y la detección de factores tripanolíticos en R. prolixus, R. robustus y R. neglectus contra el genotipo KP1-/C y varios genotipos de T. cruzi. Los avances recientes en los estudios de transcripción genómica de T. rangeli, y su comparación con T. cruzi constituyen el punto de partida para entender cabalmente la transmisión vectorial selectiva de T. rangeli y T. cruzi, así como de la patogenia de T. rangeli para el vector y de la incapacidad de T. rangeli y la capacidad de T. cruzi para invadir células del mamífero. Palabras clave:Trypanosoma rangeli KP1(+), Trypanosoma rangeli KP1(-), epidemiología molecular, genoma de T. rangeli, Rhodnius spp.Trypanosoma rangeli: an infective but non-pathogenic protozoon for humans which contributes to the understanding of the vector-borne transmission and the pathogenesis of Trypanosoma cruzi, causative agent of Chagas' disease AbstractUnlike Trypanosoma cruzi, the causative agent of Chagas' disease, T. rangeli is an infective, non-pathogenic parasite for humans, but pathogenic for vectors from the Rhodnius genus. Several T. rangeli genotypes (KP1+/A, B, KP1-/C, KP1-/D and E) have been described based on kinetoplast DNA (kDNA) polymorphisms, the spliced leader or miniexon, the intergenic transcribed spacer (ITS) and the small ribosomal subunit (SSUrRNA). These are selectively transmitted by two Rhodnius phylogenetic lines, thereby indicating co-evolutionary processes between parasite and vector genotypes. The Robustus line (Rhodnius prolixus, R. robustus...

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“…Of special interest is the unclear role of T. rangeli on human infections. This trypanosome is considered totally benign (Cuba Cuba 1998, Guhl & Vallejo 2003 but with significant immunological consequences on T. cruzi infection (Zuñiga et al 1997, Palau et al 2003, Basso et al 2004. It is therefore necessary to update the information concerning human trypanosome infections in endemic regions from Panama.…”

mentioning

confidence: 99%

“…Some authors have suggested that a previous T. rangeli infection in vertebrate hosts may have favourable effects in the clinical outcome of T. cruzi infection (Zuñiga et al 1997, Palau et al 2003, Basso et al 2004. To what extent the high prevalence of T. rangeli infection could explain the milder clinical form and/or the low prevalence of Chagas disease observed in this region (Sousa & Johnson 1973) further needs to be investigated.…”

mentioning

confidence: 99%

Predominance of Trypanosoma rangeli infection in children from a Chagas disease endemic area in the west-shore of the Panama canal

Saldaña

Samudio

Miranda

et al. 2005

Mem. Inst. Oswaldo Cruz

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A total of 206 serum samples from children (3-14 years old) Human Trypanosoma cruzi and T. rangeli infections have, for a long time, been recognized as endemic in Panama (Sousa & Johnson 1971, 1973, Sousa & Saldaña 1994. However, currently available, seroepidemiological information is insufficient to convey an acceptable picture of the prevalence of Chagas disease in the country. Of special interest is the unclear role of T. rangeli on human infections. This trypanosome is considered totally benign (Cuba Cuba 1998, Guhl & Vallejo 2003 but with significant immunological consequences on T. cruzi infection (Zuñiga et al. 1997, Palau et al 2003, Basso et al. 2004. It is therefore necessary to update the information concerning human trypanosome infections in endemic regions from Panama.During 2004, a descriptive, parasitological, and seroprevalence study on human trypanosome infections was conducted in the Amador County, La Chorrera District, in the Province of Panama. Four neighboring rural communities, previously recognized as endemic for T. cruzi infection, were selected: Lagartera Grande, Los Hules, Lagarterita, and Las Pavas. The estimated population of these four areas is 1000 inhabitants. In these localities the ecoepidemiological characteristics are favorable for trypanosomes transmission and, at present, no organized vector control measures have been established by the health authorities. The climate in this region is tropical and comprises pasture lands where the presence of the royal palm tree, Attalea butyracea, is abundant. A. butyracea is the primary biotope of Rhodnius pallescens, the main vector of T. cruzi and T. rangeli in Panama. Also, this palm tree is considered a good ecological indicator of Chagas disease risk areas (Romaña et al. 2003).To determine the prevalence of anti-T. cruzi antibodies and blood trypanosomes in these localities, 206 apparently healthy children aged between 3 and 14 years old were investigated. This sample size represents 80% of the total number of children in this age range inhabiting the studied sites. Blood samples were obtained by venipuncture from each child, informed written consent was obtained from all parents or legal guardians. Hemoculture of samples was performed as described by Vasquez et al. (1997). To corroborate and identify the species of trypanosomes isolated, a duplex PCR assay (Chiurillo et al. 2003) followed by dot blot hybridization with radiolabeled oligonucleotide probes specific for T. cruzi and T. rangeli was performed on initially microscopically positive hemocultures.Sera samples were at first screened for the presence of anti-T. cruzi antibodies using an indirect immunofluorescence antibody test (IFAT) with a local T. cruzi isolate (Burunga strain) as antigen, according to the technique described by Guhl and Nicholls (2001). The sensitivity and specificity of this assay is of 95.2 and 96.3%, respectively. Samples with circulating anti-T. cruzi antibodies in the screening test were further submitted to a commercial recombinant ELISA (ELISA, Cha...

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Action of Trypanosoma rangeli in infections with virulent Trypanosoma cruzi populations

Abstract: In experimental murine infections with

Cited by 22 publications

References 36 publications

Evaluation of Serological Tests To Identify Trypanosoma cruzi Infection in Humans and Determine Cross-Reactivity with Trypanosoma rangeli and Leishmania spp

Evaluation of Serological Tests To Identify Trypanosoma cruzi Infection in Humans and Determine Cross-Reactivity with Trypanosoma rangeli and Leishmania spp

Trypanosoma rangeli: un protozoo infectivo y no patógeno para el humano que contribuye al entendimiento de la transmisión vectorial y la infección por Trypanosoma cruzi, agente causal de la enfermedad de Chagas

Predominance of Trypanosoma rangeli infection in children from a Chagas disease endemic area in the west-shore of the Panama canal

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