AUTHOR=dos Santos Nailma Silva Aprigio , de Almeida-Júnior Carlos Roberto , Ricci Mayra Fernanda , Sanches Rodrigo C. O. , Fernandes Renata Salgado , Burle-Caldas Gabriela de A. , de Castro Júlia Teixeira , Reis-Cunha João Luís , Bartholomeu Daniella C. , Meira Ana Clara Martins , Nascimento Thaiane Gomes , Oliveira Natalia Fernanda de Melo , Gazzinelli Ricardo T. , Machado Fabiana S. , Teixeira Santuza M. R. 

TITLE=RNA and protein immunization with Trypanosoma cruzi trans-sialidase containing SAPA repeats protects mice against infection and promotes a balanced inflammatory response

JOURNAL=Frontiers in Cellular and Infection Microbiology

VOLUME=Volume 15 - 2025

YEAR=2025

URL=https://www.frontiersin.org/journals/cellular-and-infection-microbiology/articles/10.3389/fcimb.2025.1681807

DOI=10.3389/fcimb.2025.1681807

ISSN=2235-2988

ABSTRACT=Proteins with repeat domains are commonly found in protozoan parasites. Trypanosoma cruzi, which causes Chagas disease (CD), possesses a group of surface proteins called trans-sialidases (TS). These proteins are responsible for transferring sialic acid from the host’s glycoconjugates to the parasite’s mucins. The TS proteins feature a C-terminal immunogenic domain that includes amino acid repeats known as SAPA (Shed Acute Phase Antigen). Shed in the blood of the infected host, TS mediates several biological effects and because of its essential role during infection, it has been tested recurrently as a vaccine candidate against CD. Here, we investigate the effect of immunizing mice with recombinant TS proteins with and without (w/o) SAPA repeats, as well as with a protein containing only the repeat domain. We also immunize mice with RNA formulations encoding TS sequences with and without SAPA. Besides confirming the immunodominance of the SAPA domain, after challenging immunized animals with T. cruzi, we showed that the presence of the repeats did not significantly impact protection and parasite numbers after infection. However, immunization with TS protein or RNA containing the repeat domain resulted in increased production of IL-10 compared to mice immunized with TS without SAPA, and this increased IL-10 production correlates with a significant reduction in the inflammatory infiltrate in heart tissues of infected animals. These results indicate that the immunodominant SAPA domain plays a role in promoting an anti-inflammatory response, which, as a vaccine component, may contribute to induce a desirable, more balanced immune response.