Nonredundant roles for B cell-derived IL-10 in immune counter-regulation

Rajat Madan, Filiz Demircik, Sangeetha Surianarayanan, Jessica L. Allen, Senad Divanovic, Aurelien Trompette, Nir Yogev, Yuanyuan Gu, Marat Khodoun, David Hildeman, Nicholas Boespflug, Mariela B. Fogolin, Lothar Gröbe, Marina Greweling, Fred D. Finkelman, Rhonda Cardin, Markus Mohrs, Werner Müller, Ari Waisman, Axel RoersChristopher L. Karp

    Research output: Contribution to journalArticlepeer-review

    Abstract

    IL-10 plays a central role in restraining the vigor of inflammatory responses, but the critical cellular sources of this counter-regulatory cytokine remain speculative in many disease models. Using a novel IL-10 transcriptional reporter mouse, we found an unexpected predominance of B cells (including plasma cells) among IL-10-expressing cells in peripheral lymphoid tissues at baseline and during diverse models of in vivo immunological challenge. Use of a novel B cell-specific IL-10 knockout mouse revealed that B cell-derived IL-10 nonredundantly decreases virus-specific CD8+ T cell responses and plasma cell expansion during murine cytomegalovirus infection and modestly restrains immune activation after challenge with foreign Abs to IgD. In contrast, no role for B cell-derived IL-10 was evident during endotoxemia; however, although B cells dominated lymphoid tissue IL-10 production in this model, myeloid cells were dominant in blood and liver. These data suggest that B cells are an underappreciated source of counter-regulatory IL-10 production in lymphoid tissues, provide a clear rationale for testing the biological role of B cell-derived IL-10 in infectious and inflammatory disease, and underscore the utility of cell type-specific knockouts for mechanistic limning of immune counter-regulation.
    Original languageEnglish
    Pages (from-to)2312-2320
    Number of pages8
    JournalJournal of Immunology
    Volume183
    Issue number4
    DOIs
    Publication statusPublished - 15 Aug 2009

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