The Driving of Immune Response by Th1 Adjuvants in Immunization of Mice with Trypanosoma cruzi marinkellei Elicits a Controversial Infection Control

Gabriel Antonio Nogueira Nascentes; César Gómez Hernández; Rosiley Aparecida de Souza Rabelo; Raquel Fernandes Coelho; Fabiana Rossetto de Morais; Tatiane Marques; Lara Rocha Batista; Wendell Sérgio Ferreira Meira; Carlo José Freire de Oliveira; Eliane Lages Silva; Luis Eduardo Ramírez

doi:10.1089/vbz.2015.1874

The Driving of Immune Response by Th1 Adjuvants in Immunization of Mice with Trypanosoma cruzi marinkellei Elicits a Controversial Infection Control

Vector Borne Zoonotic Dis. 2016 May;16(5):317-25. doi: 10.1089/vbz.2015.1874. Epub 2016 Mar 9.

Affiliations

¹ 1 Microbiology and Immunology Discipline, Federal Institute of Education , Science and Technology at Triângulo Mineiro (IFTM), Uberaba, Brazil .
² 2 Department of Microbiology, Immunology and Parasitology, Institute of Biological and Natural Sciences, Federal University of Triângulo Mineiro (UFTM) , Uberaba, Brazil .
³ 3 School of Pharmaceutical Sciences at Ribeirão Preto, University of São Paulo (USP) , Ribeirão Preto, Brazil .

PMID: 26959861
DOI: 10.1089/vbz.2015.1874

Abstract

In previous studies, we have demonstrated that inoculation with a Trypanosoma cruzi marinkellei (avirulent RM1 strain) was able to reduce parasitemia in mice challenged with T. cruzi, although it was not able to prevent histopathological lesions. Th1 response stimulation by immunization is necessary for T. cruzi infection control, but the resistance is also dependent on immunoregulatory mechanisms, which can be induced by adjuvants. Thus, we evaluated whether inoculation of T. cruzi marinkellei associated with administration of different adjuvants would be capable of inducing different patterns of immune response to maximize the immune response against T. cruzi (virulent Romildo strain) infection. Two hundred eighty nonisogenic mice were divided into 14 groups according to the immunization scheme and the subsequent challenge with virulent Romildo T. cruzi strain. Nonimmunized groups and animals inoculated without adjuvants were also included. Immune protection was not observed with Th2 adjuvants (incomplete Freund's adjuvant [IFA] and Alum) due to high parasitemia. Th1/Th2-polarizing adjuvants also did not induce immune protection because inulin was unable to maintain survival, and immune-stimulating complexes induced intense inflammatory processes. Animals sensitized with RM1 strain without adjuvants were able to reduce parasitemia, increase survival, and protect against severe histological lesions, followed by adequate cytokine stimulation. Finally, our results demonstrate that the early and balanced IFN-γ production becomes critical to promote protection and that Th1 adjuvant elicited a controversial infection control due to increased histopathological damage. Therefore, the host's immunomodulation remains one of the most important challenges in the research for effective protection against T. cruzi infection. Similarly, the identification of protective antigens in the RM1 strain of T. cruzi marinkellei may contribute to further studies on vaccine development against human Chagas disease.

Keywords: Adjuvant; Cytokine; IFN-γ; Immunization; Trypanosoma cruzi marinkellei.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adjuvants, Immunologic*
Animals
Chagas Disease / metabolism
Chagas Disease / prevention & control*
Male
Mice
Protozoan Vaccines / immunology*
Trypanosoma cruzi / classification
Trypanosoma cruzi / immunology*

Substances

Adjuvants, Immunologic
Protozoan Vaccines