| Literature DB >> 27084100 |
Lorena M Coria1, Andrés E Ibañez1, Mercedes Tkach2, Florencia Sabbione3, Laura Bruno1, Marianela V Carabajal1, Paula M Berguer4, Paula Barrionuevo3, Roxana Schillaci2, Analía S Trevani3, Guillermo H Giambartolomei5, Karina A Pasquevich1, Juliana Cassataro6.
Abstract
In this study, we demonstrate that the unlipidated (U) outer membrane protein (Omp) 19 from Brucella spp. is a competitive inhibitor of human cathepsin L. U-Omp19 inhibits lysosome cathepsins and APC-derived microsome activity in vitro and partially inhibits lysosomal cathepsin L activity within live APCs. Codelivery of U-Omp19 with the Ag can reduce intracellular Ag digestion and increases Ag half-life in dendritic cells (DCs). U-Omp19 retains the Ag in Lamp-2(+) compartments after its internalization and promotes a sustained expression of MHC class I/peptide complexes in the cell surface of DCs. Consequently, U-Omp19 enhances Ag cross-presentation by DCs to CD8(+) T cells. U-Omp19 s.c. delivery induces the recruitment of CD11c(+)CD8α(+) DCs and monocytes to lymph nodes whereas it partially limits in vivo Ag proteolysis inside DCs. Accordingly, this protein is able to induce CD8(+) T cell responses in vivo against codelivered Ag. Antitumor responses were elicited after U-Omp19 coadministration, increasing survival of mice in a murine melanoma challenge model. Collectively, these results indicate that a cysteine protease inhibitor from bacterial origin could be a suitable component of vaccine formulations against tumors.Entities:
Mesh:
Substances:
Year: 2016 PMID: 27084100 DOI: 10.4049/jimmunol.1501188
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422