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Infection and Immunity, March 2000, p. 1252-1258, Vol. 68, No. 3
0019-9567/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
High Immunoglobulin G2 (IgG2) and Low IgG4 Levels
Are Associated with Human Resistance to Plasmodium
falciparum Malaria
Christophe
Aucan,1
Yves
Traoré,2
François
Tall,3
Boubacar
Nacro,3
Thérèse
Traoré-Leroux,2
Francis
Fumoux,1,2 and
Pascal
Rihet1,*
Faculté des Sciences de Luminy,
Université de la Méditerranée, Marseille,
France,1 and Centre Muraz,
O.C.C.G.E.,2 and Hôpital Souro
Sanou,3 Bobo-Dioulasso, Burkina Faso
Received 6 August 1999/Returned for modification 7 October
1999/Accepted 8 December 1999
There is accumulating evidence for a role of immunoglobulin G (IgG)
in protection against malarial infection and disease. Only IgG1 and
IgG3 are considered cytophilic and protective against P. falciparum, whereas IgG2 and IgG4 were thought to be neither and
even to block protective mechanisms. However, no clear pattern of
association between isotypes and protection has so far emerged. We
analyzed the isotypic distribution of the IgG response to conserved epitopes and P. falciparum blood-stage extract in 283 malaria-exposed individuals whose occurrence of infection and malaria
attack had been monitored for about 1 year. Logistic regression
analyses showed that, at the end of the season of transmission, high
levels of IgG2 to RESA and to MSP2 epitopes were associated with low risk of infection. Indeed, IgG2 is able to bind Fc
RIIA in
individuals possessing the H131 allele, and we showed that 70% of the
study subjects had this allele. Also, high specific IgG4 levels were associated with an enhanced risk of infection and with a high risk of
malaria attack. Moreover, specific IgG2 and IgG3 levels, as well as the
IgG2/IgG4 and IgG3/IgG4 ratios, increased with the age of subjects, in
parallel with the protection against infection and disease. IgG4 likely
competes with cytophilic antibodies for antigen recognition and may
therefore block cytotoxicity mediated by antibody-activated effector
cells. In conclusion, these results favor a protective role of IgG3 and
IgG2, which may activate effector cells through Fc
RIIA, and provide
evidence for a blocking role of IgG4 in malarial infection and disease.
*
Corresponding author. Mailing address: Université
de la Méditerranée, Faculté des Sciences de Luminy,
EA 864, 163 Ave. de Luminy, I3E Case 901, 13288 Marseille Cedex 9, France. Phone: (33) 4-91-82-90-21. Fax: (33) 4-91-41-66-69. E-mail:
rihet{at}luminy.univ-mrs.fr.
Infection and Immunity, March 2000, p. 1252-1258, Vol. 68, No. 3
0019-9567/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
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