Publication | Open Access
Schistosoma japonicum extracellular vesicle miRNA cargo regulates host macrophage functions facilitating parasitism
153
Citations
37
References
2019
Year
Microbial PathogensInnate Immune SystemImmunologyImmune RegulationImmunologic MechanismExtracellular MicrovesiclesS. JaponicumImmune SystemInflammationHost ResponseSchistosomiasisParasitologyHost-pathogen InteractionsMirna CargoParasitic ProtozoaSchistosome Infection PersistsHost-microbe InteractionCell BiologyImmune Cell DevelopmentPathogenesisMicrobiologyHost ResistanceMedicineHost Macrophage Functions
Schistosome infection persists for decades. Parasites are in close contact with host peripheral blood immune cells, yet little is known about the regulatory interactions between parasites and these immune cells. Here, we report that extracellular vesicles (EVs) released from Schistosoma japonicum are taken up primarily by macrophages and other host peripheral blood immune cells and their miRNA cargo transferred into recipient cells. Uptake of S. japonicum EV miR-125b and bantam miRNAs into host cells increased macrophage proliferation and TNF-α production by regulating the corresponding targets including Pros1, Fam212b, and Clmp. Mice infected with S. japonicum exhibit an increased population of monocytes and elevated levels of TNF-α. Reduction of host monocytes and TNF-α level in S. japonicum infected mice led to a significant reduction in worm and egg burden and pathology. Overall, we demonstrate that S. japonicum EV miRNAs can regulate host macrophages illustrating parasite modulation of the host immune response to facilitate parasite survival. Our findings provide valuable insights into the schistosome-host interaction which may help to develop novel intervention strategies against schistosomiasis.
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