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Infection and Immunity, May 2001, p. 3190-3196, Vol. 69, No. 5
Centre for Medical Parasitology at Department
of Infectious Diseases, Copenhagen University Hospital (Rigshospitalet)
and Institute for Medical Microbiology and Immunology, University of
Copenhagen, Copenhagen, Denmark1;
Department of Child Health, Korle-Bu Teaching Hospital,
Accra,2 and Immunology Unit, Noguchi
Memorial Institute for Medical Research,
Legon,3 Ghana; and Unité
d'Immunologie Moléculaires des Parasites, CNRS URA
1960,4 and Unité de Biologie
Moleculaire du Gene,5 Institut
Pastéur, Paris, France
Received 29 December 2000/Returned for modification 10 February
2001/Accepted 20 February 2001
0019-9567/01/$04.00+0 DOI: 10.1128/IAI.69.5.3190-3196.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.
Perturbation and Proinflammatory Type Activation of
V
1+ 
T Cells in African Children with
Plasmodium falciparum Malaria
T cells have variously been implicated in the protection
against, and the pathogenesis of, malaria, but few studies have examined the T-cell response to malaria in African children, who
suffer the large majority of malaria-associated morbidity and
mortality. This is unfortunate, since available data suggest that
simple extrapolation of conclusions drawn from studies of nonimmune
adults ex vivo and in vitro is not always possible. Here we show that
both the frequencies and the absolute numbers of T cells are
transiently increased following treatment of Plasmodium
falciparum malaria in Ghanaian children and they can constitute
30 to 50% of all T cells shortly after initiation of antimalarial
chemotherapy. The bulk of the T cells involved in this
perturbation expressed V1 and had a highly activated phenotype.
Analysis of the T-cell receptors (TCR) of the V1+ cell
population at the peak of their increase showed that all expressed V
chains were used, and CDR3 length polymorphism indicated that the
expanded V1 population was highly polyclonal. A very high proportion
of the V1+ T cells produced gamma interferon, while
fewer V1+ cells than the average proportion of all
CD3+ cells produced tumor necrosis factor alpha. No
interleukin 10 production was detected among TCR-+
cells in general or V1+ cells in particular. Taken
together, our data point to an immunoregulatory role of the expanded
V1+ T-cell population in this group of semi-immune
P. falciparum malaria patients.
*
Corresponding author. Mailing address: Department of
Infectious Diseases M7641, Rigshospitalet, Tagensvej 20, 2200 Copenhagen N, Denmark. Phone: (45) 35 45 79 57. Fax: (45) 35 45 76 44. E-mail: lhcmp{at}rh.dk.
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