Protection against malaria in mice is induced by blood stage-arresting histamine-releasing factor (HRF)-deficient parasites

Affiliation auteurs!!!! Error affiliation !!!!
TitreProtection against malaria in mice is induced by blood stage-arresting histamine-releasing factor (HRF)-deficient parasites
Type de publicationJournal Article
Year of Publication2016
AuteursDemarta-Gatsi C, Smith L, Thiberge S, Peronet R, Commere P-H, Matondo M, Apetoh L, Bruhns P, Menard R, Mecheri S
JournalJOURNAL OF EXPERIMENTAL MEDICINE
Volume213
Pagination1419-1428
Date PublishedJUL 25
Type of ArticleArticle
ISSN0022-1007
Résumé

Although most vaccines against blood stage malaria in development today use subunit preparations, live attenuated parasites confer significantly broader and more lasting protection. In recent years, Plasmodium genetically attenuated parasites (GAPs) have been generated in rodent models that cause self-resolving blood stage infections and induce strong protection. All such GAPs generated so far bear mutations in housekeeping genes important for parasite development in red blood cells. In this study, using a Plasmodium berghei model compatible with tracking anti-blood stage immune responses over time, we report a novel blood stage GAP that lacks a secreted factor related to histamine-releasing factor (HRF). Lack of HRF causes an IL-6 increase, which boosts T and B cell responses to resolve infection and leave a cross-stage, cross-species, and lasting immunity. Mutant-induced protection involves a combination of antiparasite IgG2c antibodies and Fc gamma R+ CD11b(+) cell phagocytes, especially neutrophils, which are sufficient to confer protection. This immune-boosting GAP highlights an important role of opsonized parasite-mediated phagocytosis, which may be central to protection induced by all self-resolving blood stage GAP infections.

DOI10.1084/jem.20151976