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Th17: An Effector CD4 T Cell Lineage with Regulatory T Cell Ties

Published byPiroska Bodnárné Modified over 5 years ago

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Presentation on theme: "Th17: An Effector CD4 T Cell Lineage with Regulatory T Cell Ties"— Presentation transcript:

1 Th17: An Effector CD4 T Cell Lineage with Regulatory T Cell Ties
Casey T. Weaver, Laurie E. Harrington, Paul R. Mangan, Maya Gavrieli, Kenneth M. Murphy  Immunity  Volume 24, Issue 6, Pages (June 2006) DOI: /j.immuni Copyright © 2006 Elsevier Inc. Terms and Conditions

2 Figure 1 Diversification of CD4 T Cell Lineages
Although functional CD4 T cell development has been dominated by the Th1-Th2 paradigm for nearly two decades, the number of defined lineages has now increased. The cytokines associated with arrows indicate dominant cytokines involved in specification of each of the indicated lineages. The cytokines listed below each cell type indicate key effector or regulatory cytokines produced by differentiated cells of that lineage or, in the case of nTreg, a contact-dependent mechanism of suppression. Tn: naive, postthymic CD4 T cell precursors; Tp: thymic precursors. Dotted lines represent less well-defined lineage relationships. Immunity  , DOI: ( /j.immuni ) Copyright © 2006 Elsevier Inc. Terms and Conditions

3 Figure 2 Model of Branching Th17 and Adaptive Treg Lineage Development
This model emphasizes distinct pathways leading to mature Th17 effector cells or Foxp3+ adaptive Tregs (aTreg), induced by a common requirement for TGF-β but differential effects of IL-6 and IL-23. Naive CD4 T cells (Tn) activated by antigen presented on immature DCs that do not produce IL-6 production are induced by TGF-β to express Foxp3 and develop into aTregs (top panel). Tns activated by mature, TLR-activated DCs that produce IL-6 are induced by TGF-β to upregulate IL-23R and become competent for IL-17 production and IL-23 signaling. IL-23 signaling induces responsiveness to IL-18 and IL-1, which can act synergistically with IL-23 to induce Th17 cytokine production independently of TCR stimulation. Alternatively, TCR stimulation by antigen can induce Th17 cytokine production directly, without a requirement for IL-23, IL-1, or IL-18. Dotted lines indicate possible positive feedback loops by which cytokine products of Th17 (IL-6) or aTreg cells (TGF-β1) may reinforce lineage development. Immunity  , DOI: ( /j.immuni ) Copyright © 2006 Elsevier Inc. Terms and Conditions

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