Mucosal and systemic anti-HIV immunity controlled by A20 in mouse dendritic cells
Bangxing Hong, … , Xue F. Huang, Si-Yi Chen
Bangxing Hong, … , Xue F. Huang, Si-Yi Chen
Published January 4, 2011
Citation Information: J Clin Invest. 2011;121(2):739-751. https://doi.org/10.1172/JCI42656.
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Research Article Virology

Mucosal and systemic anti-HIV immunity controlled by A20 in mouse dendritic cells

Abstract

Both mucosal and systemic immune responses are required for preventing or containing HIV transmission and chronic infection. However, currently described vaccination approaches are largely ineffective in inducing both mucosal and systemic responses. In this study, we found that the ubiquitin-editing enzyme A20 — an inducible feedback inhibitor of the TNFR, RIG-I, and TLR signaling pathways that broadly controls the maturation, cytokine production, and immunostimulatory potency of DCs — restricted systemically immunized DCs to induce both robust mucosal and systemic HIV-specific cellular and humoral responses. Mechanistic studies revealed that A20 regulated DC production of retinoic acid and proinflammatory cytokines, inhibiting the expression of gut-homing receptors on T and B cells. Furthermore, A20-silenced, hyperactivated DCs exhibited an enhanced homing capacity to draining and gut-associated lymphoid tissues (GALTs) after systemic administration. Thus, this study provides insights into the role of A20 in innate immunity. This work may allow the development of an efficient HIV vaccination strategy that is capable of inducing both robust systemic and mucosal anti-HIV cellular and humoral responses.

Authors

Bangxing Hong, Xiao-Tong Song, Lisa Rollins, Lindsey Berry, Xue F. Huang, Si-Yi Chen

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Figure 8

CD4+ T cell–independent CTL and antibody responses induced by Ad-siA20-BM-DCs.

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CD4+ T cell–independent CTL and antibody responses induced by Ad-siA20-B...
Groups of C57BL/6 mice (n = 6) were treated with anti-CD4 antibodies (GK1.5, 200 μg/mouse, i.p. injection) 3 days before each immunization (44) and then immunized twice with gp120-pulsed (100 μg/ml), Ad-transfected DCs matured with LPS at a weekly interval, followed by in vivo stimulation with poly(I:C) (i.p., 50 μg/mouse) daily for 3 consecutive days. Splenocytes pooled from immunized mice were subjected to ICS (A), IFN-γ ELISPOT (B), and cytolytic assays against gp120-pulsed syngeneic TC1 cells (36) (C). HIV gp120–specific IgG antibody titers from pooled sera were analyzed by ELISA (D). Data from 1 of 2 repeated experiments are presented. *P < 0.05, Ad-siGFP-BM-DCs versus Ad-siA20-BM-DCs.