Human Malaria in Immunocompromised Mice: An In Vivo Model to Study Defense Mechanisms against Plasmodium falciparum

doi:10.1084/jem.192.11.1653

Published online 4 December 2000.

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© The Rockefeller University Press, 0022-1007/2000/12/1653/ $5.00
The Journal of Experimental Medicine, Volume 192, Number 11, December 4, 2000 1653-1660

Brief Definitive Report

Human Malaria in Immunocompromised Mice: An In Vivo Model to Study Defense Mechanisms against Plasmodium falciparum

Edgar Badell^a, Claude Oeuvray^a, Alicia Moreno^a, Soe Soe^a, Nico van Rooijen^b, Ahmed Bouzidi^c, and Pierre Druilhe^a
^a Bio-Medical Parasitology Unit, Institut Pasteur, 75015 Paris, France
^b Department of Cell Biology and Immunology, Faculty of Medicine, Vrije Universiteit, Amsterdam 1081 BT, The Netherlands
^c SEDAC-Therapeutics SA, 59000 Lille, France

Correspondence to: Pierre Druilhe, Bio-Medical Parasitology Unit, Institut Pasteur 28, rue du Dr Roux, 75015 Paris, France. Tel:33-1-45-68-85-78 Fax:33-1-45-68-86-40 E-mail:druilhe{at}pasteur.fr.

We have recently described that sustained Plasmodium falciparumgrowth could be obtained in immunodeficient mice. We now reportthe potential of this new mouse model by assaying the effectof the passive transfer of antibodies (Abs) which in humanshave had a well-established effect.

Our results show that the total African adult hyperimmune immunoglobulinGs (HI-IgGs) strongly reduce P. falciparum parasitemia similarlyto that reported in humans, but only when mice are concomitantlyreconstituted with human monocytes (HuMNs). In contrast, neitherHI-IgGs nor HuMNs alone had any direct effect upon parasitemia.We assessed the in vivo effect of epitope-specific human Absaffinity-purified on peptides derived either from the ring erythrocytesurface antigen (RESA) or the merozoite surface protein 3 (MSP3).The inoculation of low concentrations of anti-synthetic peptidefrom MSP3, but not of anti-RESA Abs, consistently suppressedP. falciparum in the presence of HuMNs. Parasitemia decreasewas stronger and faster than that observed using HI-IgGs andas fast as that induced by chloroquine. Our observations demonstratethat this mouse model is of great value to evaluate the protectiveeffect of different Abs with distinct specificity in the sameanimal, a step hardly accessible and therefore never performedbefore in humans.

Key Words: mouse model, protective immunity, antibody-dependent cellularinhibition, merozoite surface protein 3, ring erythrocyte surfaceantigen

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