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Infect. Immun., 05 1997, 1876-1882, Vol 65, No. 5
E Leroy, S Baize, G Wahl, TG Egwang and AJ Georges
Human infection with the parasite Loa loa is characterized by a good
adaptation between the parasite and its host. One portion of the human
population harbors only adult worms in subcutaneous tissues, whereas
another portion also harbors the L1 microfilarial stage in peripheral
circulation. This study was undertaken to understand the mechanisms by
which the parasite evades or modulates host immunological attack. The
cellular responses, based on T-cell proliferation, to the production of
various cytokines (interleukin-2 [IL-2], gamma interferon [IFN-gamma],
IL-4, and IL-5) and to expression of cytokine (IL-2, IFN-gamma, IL-4, IL-5,
IL-10, and IL-12) mRNAs were investigated during the experimental infection
with human parasite L. loa of a nonhuman primate which has been shown to
display a spectrum of disease similar to that found in humans. Our results
indicate that a T-cell unresponsiveness occurs when female worm products
are released into the peripheral circulation, preceded by a transient
period of strong T-cell proliferation, cytokine production, and cytokine
mRNA expression. In the unresponsive state, only IL-10 mRNA is expressed,
suggesting a role for IL-10 in down- regulation and maintenance of
unresponsiveness. Taken together, these results indicate that both IL-10
production, which is known to inhibit B7 expression on monocytes, and the
massive release of female products in the blood where T cells encounter
antigens presented by nonactivated B lymphocytes, which lack costimulatory
signals, should contribute to the inactivation of T cells.
Copyright © 1997, American Society for Microbiology
Experimental infection of a nonhuman primate with Loa loa induces transient strong immune activation followed by peripheral unresponsiveness of helper T cells
Centre International de Recherches Medicales de Franceville, Gabon. eleroy@cauchy.cirmfrv.fr
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