The Journal of Experimental Medicine
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© The Rockefeller University Press, 0022-1007/1998/12/2075/ $5.00
The Journal of Experimental Medicine, Volume 188, Number 11, December 7, 1998 2075-2082

Articles

Prevention of Peripheral Tolerance by a Dendritic Cell Growth Factor: Flt3 Ligand as an Adjuvant

Bali Pulendran*, J.L. Smith*, M. Jenkins{ddagger}, M. Schoenborn*, E. Maraskovsky*, and C.R. Maliszewski*

From * Immunex Corporation, Seattle, Washington 98101; and the {ddagger} Department of Microbiology, Center for Immunology, Minneapolis, Minnesota 55455

Injections of soluble proteins are poorly immunogenic, and often elicit antigen-specific tolerance. The mechanism of this phenomenon has been an enduring puzzle, but it has been speculated that tolerance induction may be due to antigen presentation by poorly stimulatory, resting B cells, which lack specific immunoglobulin receptors for the protein. In contrast, adjuvants, or infectious agents, which cause the release of proinflammatory cytokines such as tumor necrosis factor {alpha} and interleukin 1β in vivo are believed to recruit and activate professional antigen-presenting cells to the site(s) of infection, thereby eliciting immunity. Here we show that administration of Flt3 ligand (FL), a cytokine capable of inducing large numbers of dendritic cells (DCs) in vivo, (a) dramatically enhances the sensitivity of antigen-specific B and T cell responses to systemic injection of a soluble protein, through a CD40–CD40 ligand–dependent mechanism; (b) influences the class of antibody produced; and (c) enables productive immune responses to otherwise tolerogenic protocols. These data support the hypothesis that the delicate balance between immunity and tolerance in vivo is pivotally controlled by DCs, and underscore the potential of FL as a vaccine adjuvant for immunotherapy in infectious disease and other clinical settings.

Key Words: Flt3 ligand • dendritic cells • adjuvant • tolerance • immunity

Address correspondence to Bali Pulendran at his present address, Baylor Institute for Immunology Research, 3434 Live Oak, Dallas, TX 75204. Phone: 214-820-7450; Fax: 214-820-4813.

Abbreviations used: CD40L, CD40 ligand; DC, dendritic cell; FL, Flt3 ligand; MSA, mouse serum albumin.


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