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The Journal of Immunology, 2004, 172: 7031-7042.
Copyright © 2004 by The American Association of Immunologists

Distinct Transcriptional Programs Activated by Interleukin-10 with or without Lipopolysaccharide in Dendritic Cells: Induction of the B Cell-Activating Chemokine, CXC Chemokine Ligand 131

Patrick Perrier*, Fernando O. Martinez{dagger}, Massimo Locati{dagger}, Giancarlo Bianchi*, Manuela Nebuloni{ddagger}, Gianluca Vago{ddagger}, Flavia Bazzoni§, Silvano Sozzani*, Paola Allavena* and Alberto Mantovani2,*,{dagger}

* Istituto di Ricerche Farmacologiche Mario Negri, Milan, Italy; {dagger} Centro di Eccellenza per l’Innovazione Diagnostica e Terapeutica, Institute of General Pathology, University of Milan, Milan, Italy; {ddagger} Institute of Pathology, University of Milan, Ospedale Luigi Sacco, Milan, Italy; § Department of Pathology, University of Verona, Verona, Italy; and Department of Biotechnology and Biomedical Sciences, Section of General Pathology and Immunology, University of Brescia, Brescia, Italy

To understand the modulation of dendritic cell (DC) function by IL-10, gene expression profiling was performed by using Affymetrix technology (Santa Clara, CA) in human monocyte-derived DC treated with IL-10, alone or in combination with LPS. The modulation of selected genes was validated by real-time PCR, Northern blot, and protein production. IL-10 regulated in DC the expression of a limited number of genes, including IL-7, the receptors for transferrin and vitamin D3, structural matrix proteins, and signal transduction elements. The combined treatment with LPS plus IL-10 modulated a number of genes comparable to LPS alone, but the expression profiles were distinct. As expected, IL-10 suppressed the expression of several LPS-inducible proinflammatory molecules. Among genes uniquely modulated by the concomitant treatment with LPS plus IL-10, phosphatidylinositol 3-kinase {gamma} was down-regulated while the suppressor of cytokine signaling 3, signaling lymphocytic activation molecule, regulator of G protein signaling 16, and the chemokine, CXC chemokine ligand (CXCL) 13, were up-regulated. Overall, four distinct transcriptional programs were identified, related to: 1) control of immunity and inflammation; 2) tuning of cytokine receptor and G protein-coupled receptor signaling; 3) remodeling of extracellular matrix; and 4) B cell function and lymphoid tissue neogenesis. Among the latter genes, we further demonstrate that IL-10 synergizes with TLR ligands for the production of functionally active B cell-attracting chemokine, CXCL13, in both myeloid and plasmacytoid DC. This novel finding reveals that IL-10 sustains humoral immunity by inducing the production in APCs of the chemokine, CXCL13, which amplifies B cell recruitment and promotes lymphoid tissue neogenesis.


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