The entrance route: Oral, mucous, cutaneous, or systemic has a marked influence on the outcome of Trypanosoma cruzi experimental infection

•The origin of the trypomastigote is a key factor in the severity of acute Trypanosoma cruzi infection in mice.•The entrance route (mucous, cutaneous, or systemic) influences the outcome of T. cruzi infection.•The origin of the trypomastigote form (blood or metacyclic) has a marked influence on tiss...

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Veröffentlicht in:Acta tropica 2022-10, Vol.234, p.106581-106581, Article 106581
Hauptverfasser: Gonçalves, Karolina Ribeiro, Mazzeti, Ana Lia, Nascimento, Alvaro Fernando da Silva, Castro - Lacerda (in memory), Jéssica Mara, Nogueira-Paiva, Nívia Carolina, Mathias, Fernando Augusto Siqueira, Reis, Alexandre Barbosa, Caldas, Sérgio, Bahia, Maria Terezinha
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container_title Acta tropica
container_volume 234
creator Gonçalves, Karolina Ribeiro
Mazzeti, Ana Lia
Nascimento, Alvaro Fernando da Silva
Castro - Lacerda (in memory), Jéssica Mara
Nogueira-Paiva, Nívia Carolina
Mathias, Fernando Augusto Siqueira
Reis, Alexandre Barbosa
Caldas, Sérgio
Bahia, Maria Terezinha
description •The origin of the trypomastigote is a key factor in the severity of acute Trypanosoma cruzi infection in mice.•The entrance route (mucous, cutaneous, or systemic) influences the outcome of T. cruzi infection.•The origin of the trypomastigote form (blood or metacyclic) has a marked influence on tissue tropism.•The intensity of the cardiac inflammation is clearly associated with TNF-α level. In recent decades, the oral infection of Trypanosoma cruzi has gathered increased attention due to frequent outbreaks that can lead to more severe clinical signs than those usually found in the areas of vector transmission. This study addresses the main routes of infection using metacyclic trypomastigotes (MT) and blood trypomastigotes (BT). Herein, BALB/c mice were infected with the Colombian (TcI) strain via intraperitoneal (IP), oral, intragastric (IG), ocular (OC) and cutaneous (CT) routes with 106 culture-derived MT or BT. Parasitemia was intermittent and low in animals inoculated with MT, in contrast, high parasitemia levels were found in BT-mice. A tropism for the muscles was observed in oral or IG infection with BT. Differently, the parasite was widely distributed in the tissues of mice infected with MT. However, the intensity of the inflammation infiltrating the tissues was higher in oral or IG infection with BT. Animals inoculated with BT via the IG route had similar serum levels of IFN-γ and smaller IL-10 compared to those infected with MT via the IG route. TNF-α levels were higher in the serum from BT-animals, which could explain the higher intensity of heart inflammation in these animals. Our results suggest that the infective form and the route of infection differentially modulated the outcome of Trypanosoma cruzi mice infection.
doi_str_mv 10.1016/j.actatropica.2022.106581
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In recent decades, the oral infection of Trypanosoma cruzi has gathered increased attention due to frequent outbreaks that can lead to more severe clinical signs than those usually found in the areas of vector transmission. This study addresses the main routes of infection using metacyclic trypomastigotes (MT) and blood trypomastigotes (BT). Herein, BALB/c mice were infected with the Colombian (TcI) strain via intraperitoneal (IP), oral, intragastric (IG), ocular (OC) and cutaneous (CT) routes with 106 culture-derived MT or BT. Parasitemia was intermittent and low in animals inoculated with MT, in contrast, high parasitemia levels were found in BT-mice. A tropism for the muscles was observed in oral or IG infection with BT. Differently, the parasite was widely distributed in the tissues of mice infected with MT. However, the intensity of the inflammation infiltrating the tissues was higher in oral or IG infection with BT. Animals inoculated with BT via the IG route had similar serum levels of IFN-γ and smaller IL-10 compared to those infected with MT via the IG route. TNF-α levels were higher in the serum from BT-animals, which could explain the higher intensity of heart inflammation in these animals. 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In recent decades, the oral infection of Trypanosoma cruzi has gathered increased attention due to frequent outbreaks that can lead to more severe clinical signs than those usually found in the areas of vector transmission. This study addresses the main routes of infection using metacyclic trypomastigotes (MT) and blood trypomastigotes (BT). Herein, BALB/c mice were infected with the Colombian (TcI) strain via intraperitoneal (IP), oral, intragastric (IG), ocular (OC) and cutaneous (CT) routes with 106 culture-derived MT or BT. Parasitemia was intermittent and low in animals inoculated with MT, in contrast, high parasitemia levels were found in BT-mice. A tropism for the muscles was observed in oral or IG infection with BT. Differently, the parasite was widely distributed in the tissues of mice infected with MT. However, the intensity of the inflammation infiltrating the tissues was higher in oral or IG infection with BT. Animals inoculated with BT via the IG route had similar serum levels of IFN-γ and smaller IL-10 compared to those infected with MT via the IG route. TNF-α levels were higher in the serum from BT-animals, which could explain the higher intensity of heart inflammation in these animals. 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subjects Acute Chagas disease
Blood trypomastigote
Metacyclic Trypomastigote
Oral Chagas disease
Trypanosoma cruzi
title The entrance route: Oral, mucous, cutaneous, or systemic has a marked influence on the outcome of Trypanosoma cruzi experimental infection
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