TY - JOUR
T1 - Nonredundant roles for B cell-derived IL-10 in immune counter-regulation
AU - Madan, Rajat
AU - Demircik, Filiz
AU - Surianarayanan, Sangeetha
AU - Allen, Jessica L.
AU - Divanovic, Senad
AU - Trompette, Aurelien
AU - Yogev, Nir
AU - Gu, Yuanyuan
AU - Khodoun, Marat
AU - Hildeman, David
AU - Boespflug, Nicholas
AU - Fogolin, Mariela B.
AU - Gröbe, Lothar
AU - Greweling, Marina
AU - Finkelman, Fred D.
AU - Cardin, Rhonda
AU - Mohrs, Markus
AU - Müller, Werner
AU - Waisman, Ari
AU - Roers, Axel
AU - Karp, Christopher L.
PY - 2009/8/15
Y1 - 2009/8/15
N2 - 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.
AB - 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.
U2 - 10.4049/jimmunol.0900185
DO - 10.4049/jimmunol.0900185
M3 - Article
C2 - 19620304
SN - 1550-6606
VL - 183
SP - 2312
EP - 2320
JO - Journal of Immunology
JF - Journal of Immunology
IS - 4
ER -