Please use this identifier to cite or link to this item:
https://www.arca.fiocruz.br/handle/icict/5878
UNC93B1 MEDIATES HOST RESISTANCE TO INFECTION WITH TOXOPLASMA GONDII
Author
Affilliation
University of Massachusetts Medical School. Worcester, MA, United States of America
University of Massachusetts Medical School. Worcester, MA, United States of America
University of Massachusetts Medical School. Worcester, MA, United States of America
Institute for Genetics, University of Cologne. Cologne, Germany
University of Massachusetts Medical School. Worcester, MA, United States of America
University of Massachusetts Medical School. Worcester, MA, United States of America
Scripps Research Institute. La Jolla, CA, United States of America
Institute for Genetics, University of Cologne. Cologne, Germany
University of Massachusetts Medical School. Worcester, MA, United States of America/ Fundacão Oswaldo Cruz. Centro de Pesquisas Rene Rachou. Belo Horizonte, MG, Brazil
University of Massachusetts Medical School. Worcester, MA, United States of America , Fundacão Oswaldo Cruz. Centro de Pesquisas Rene Rachou. Belo Horizonte, MG, Brazil/ Universidade Federal de Minas Gerais. Belo Horizonte, MG, Brazil
University of Massachusetts Medical School. Worcester, MA, United States of America
University of Massachusetts Medical School. Worcester, MA, United States of America
Institute for Genetics, University of Cologne. Cologne, Germany
University of Massachusetts Medical School. Worcester, MA, United States of America
University of Massachusetts Medical School. Worcester, MA, United States of America
Scripps Research Institute. La Jolla, CA, United States of America
Institute for Genetics, University of Cologne. Cologne, Germany
University of Massachusetts Medical School. Worcester, MA, United States of America/ Fundacão Oswaldo Cruz. Centro de Pesquisas Rene Rachou. Belo Horizonte, MG, Brazil
University of Massachusetts Medical School. Worcester, MA, United States of America , Fundacão Oswaldo Cruz. Centro de Pesquisas Rene Rachou. Belo Horizonte, MG, Brazil/ Universidade Federal de Minas Gerais. Belo Horizonte, MG, Brazil
Abstract
UNC93B1 associates with Toll-Like Receptor (TLR) 3, TLR7 and TLR9, mediating their translocation from the endoplasmic reticulum to the endolysosome, hence allowing proper activation by nucleic acid ligands. We found that the triple deficient ‘3d’ mice, which lack functional UNC93B1, are hyper-susceptible to infection with Toxoplasma gondii. We established that while mounting a normal systemic pro-inflammatory response, i.e. producing abundant MCP-1, IL-6, TNFa and IFNc, the 3d mice were unable to control parasite replication. Nevertheless, infection of reciprocal bone marrow chimeras between wildtype and 3d mice with T. gondii demonstrated a primary role of hemopoietic cell lineages in the enhanced susceptibility of UNC93B1 mutant mice. The protective role mediated by UNC93B1 to T. gondii infection was associated with impaired IL-12 responses and delayed IFNc by spleen cells. Notably, in macrophages infected with T. gondii, UNC93B1 accumulates on the parasitophorous vacuole. Furthermore, upon in vitro infection the rate of tachyzoite replication was enhanced in nonactivated macrophages carrying mutant UNC93B1 as compared to wild type gene. Strikingly, the role of UNC93B1 on intracellular parasite growth appears to be independent of TLR function. Altogether, our results reveal a critical role for UNC93B1 on induction of IL-12/IFNc production as well as autonomous control of Toxoplasma replication by macrophages.
Share