AUTHOR=Medina Tiago Silva , Oliveira Gabriela Gonçalves , Silva Maria Cláudia , David Bruna Araújo , Silva Grace Kelly , Fonseca Denise Morais , Sesti-Costa Renata , Frade Amanda Farage , Baron Monique Andrade , Ianni Barbara , Pereira Alexandre Costa , Chevillard Christophe , Cunha-Neto Edécio , Marin-Neto José Antonio , Silva João Santana 

TITLE=Ebi3 Prevents Trypanosoma cruzi-Induced Myocarditis by Dampening IFN-γ-Driven Inflammation

JOURNAL=Frontiers in Immunology

VOLUME=8

YEAR=2017

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2017.01213

DOI=10.3389/fimmu.2017.01213

ISSN=1664-3224

ABSTRACT=<p>The identification of anti-inflammatory mediators can reveal important targetable molecules capable of counterbalancing <italic>Trypanosoma cruzi</italic>-induced myocarditis. Composed of Ebi3 and IL-27p28 subunits, IL-27 is produced by myeloid cells and is able to suppress inflammation by inducing IL-10-producing Tr1 cells, thus emerging as a potential candidate to ameliorate cardiac inflammation induced by <italic>T. cruzi</italic>. Although IL-27 has been extensively characterized as a suppressive cytokine that prevents liver immunopathogenesis after <italic>T. cruzi</italic> infection, the mechanisms underlying its effects on <italic>T. cruzi</italic>-induced myocarditis remain largely unknown. Here, wild-type (WT) and Ebi3-deficient animals were intraperitoneally infected with trypomastigotes of <italic>T. cruzi</italic> Y strain and used to evaluate the potential anti-inflammatory properties of Ebi3 during <italic>T. cruzi</italic> infection. The survival rates of mice were daily recorded, the frequency of inflammatory cells was analyzed by flow cytometry and inflammatory mediators were measured by ELISA, real-time PCR and PCR array. We reported that <italic>T. cruzi</italic>-induced myocarditis was prevented by Ebi3. Stressors mainly recognized by TLR2 and TLR4 receptors on myeloid cells were essential to trigger IL-27p28 production. In addition, Ebi3 regulated IFN-γ-mediated myocarditis by promoting an anti-inflammatory environment through IL-10, which was most likely produced by Tr1 cells rather than classical regulatory T cells (Tregs), in the heart tissue of <italic>T. cruzi</italic>-infected animals. Furthermore, <italic>in vivo</italic> IFN-γ blockade ameliorated the host survival without compromising the parasite control in the bloodstream. In humans, IL-27p28 was correlated with cardiac protection during Chagas disease. Patients with mild clinical forms of the disease produced high levels of IL-27p28, whereas lower levels were found in those with severe forms. In addition, polymorphic sites at Ebi3 gene were associated with severe cardiomyopathy in patients with Chagas disease. Collectively, we describe a novel regulatory mechanism where Ebi3 dampens cardiac inflammation by modulating the overproduction of IFN-γ, the <italic>bona fide</italic> culprit of Chagas disease cardiomyopathy.</p>