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The Journal of Immunology, 2004, 172: 5986-5993.
Copyright © 2004 by The American Association of Immunologists

IL-10-Secreting Regulatory T Cells Do Not Express Foxp3 but Have Comparable Regulatory Function to Naturally Occurring CD4+CD25+ Regulatory T Cells 1

Pedro L. Vieira2,*, Jillian R. Christensen*, Sophie Minaee{ddagger}, Emma J. O’Neill{ddagger}, Franck J. Barrat§, André Boonstra*, Thomas Barthlott{dagger}, Brigitta Stockinger{dagger}, David C. Wraith{ddagger} and Anne O’Garra2,*

* Division of Immunoregulation, {dagger} Division of Molecular Immunology, The National Institute for Medical Research, London, United Kingdom; {ddagger} Department of Pathology and Microbiology, University of Bristol School of Medical Sciences, Bristol, United Kingdom; and § Dynavax Technologies, Berkeley, CA 94710

Regulatory T cells (TReg) control immune responses to self and nonself Ags. The relationship between Ag-driven IL-10-secreting TReg (IL-10-TReg) and naturally occurring CD4+CD25+ TReg is as yet unclear. We show that mouse IL-10-TReg obtained using either in vitro or in vivo regimens of antigenic stimulation did not express the CD4+CD25+ TReg-associated transcription factor Foxp3. However, despite the absence of Foxp3 expression, homogeneous populations of IL-10-TReg inhibited the in vitro proliferation of CD4+CD25 T cells with a similar efficiency to that of CD4+CD25+ TReg. This inhibition of T cell proliferation by IL-10-TReg was achieved through an IL-10-independent mechanism as seen for CD4+CD25+ TReg and was overcome by exogenous IL-2. Both IL-10-TReg and CD4+CD25+ TReg were similar in that they produced little to no IL-2. These data show that Foxp3 expression is not a prerequisite for IL-10-TReg activity in vitro or in vivo, and suggest that IL-10-TReg and naturally occurring CD4+CD25+ TReg may have distinct origins.




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