par Beschin, Alain 
;De Baetselier, Patrick;Van Den Abbeele, Jan;Pays, Etienne
Référence Trends in parasitology, 30, 11, page (538-547)
Publication Publié, 2014-11
;De Baetselier, Patrick;Van Den Abbeele, Jan;Pays, Etienne Référence Trends in parasitology, 30, 11, page (538-547)
Publication Publié, 2014-11
Article révisé par les pairs
| Résumé : | The life cycle of African trypanosomes involves adaptations to the defense mechanisms of two completely different hosts, the insect vector Glossina and the mammalian host. This interplay ultimately determines host resistance and/or tolerance to parasite infection. In the tsetse fly, the immune deficiency (IMD)-regulated pathway, the scavenger receptor peptidoglycan-recognition protein LB (PGRP-LB), and the reactive oxygen species (ROS)-mediated response modulate the insect's capacity to transmit the parasite. In experimental mice, control of parasite burden and tissue pathogenicity relies on timely regulated interactions between myeloid cells exhibiting distinct activation states (M1 versus M2 type). Tsetse fly saliva and various trypanosome components including adenylate cyclases, DNA, a kinesin heavy chain, and variant surface glycoprotein (VSG) interfere with resistance and tolerance to infection. |
