par Flores, Amilcar;Alonso-Vega, Cristina;Hermann, Emmanuel 
;Torrico, Mary Cruz;Montaño Villarroel, Nair Alaide;Torrico, Faustino;Carlier, Yves ;Truyens, Carine
Référence Pathogens, 12, 9, 1103
Publication Publié, 2023-09
;Torrico, Mary Cruz;Montaño Villarroel, Nair Alaide;Torrico, Faustino;Carlier, Yves ;Truyens, Carine Référence Pathogens, 12, 9, 1103
Publication Publié, 2023-09
Article révisé par les pairs
| Résumé : | Activated monocytes/macrophages that produce inflammatory cytokines and nitric oxide are crucial for controlling Trypanosoma cruzi infection. We previously showed that uninfected newborns from T. cruzi infected mothers (M+B- newborns) were sensitized to produce higher levels of inflammatory cytokines than newborns from uninfected mothers (M-B- newborns), suggesting that their monocytes were more activated. Thus, we wondered whether these cells might help limit congenital infection. We investigated this possibility by studying the activation status of M+B- cord blood monocytes and their ability to control T. cruzi in vitro infection. We showed that M+B- monocytes have an upregulated capacity to produce the inflammatory cytokine TNF-α and a better ability to control T. cruzi infection than M-B- monocytes. Our study also showed that T. cruzi-specific Abs transferred from the mother play a dual role by favoring trypomastigote entry into M+B- monocytes and inhibiting intracellular amastigote multiplication. These results support the possibility that some M+B- fetuses may eliminate the parasite transmitted in utero from their mothers, thus being uninfected at birth. |
