Thompson Angus G, O'Sullivan Brendan J, Beamish Heather, Thomas Ranjeny
Centre for Immunology and Cancer Research, Princess Alexandra Hospital, University of Queensland, Brisbane, Australia.
J Immunol. 2004 Aug 1;173(3):1671-80. doi: 10.4049/jimmunol.173.3.1671.
Paradoxically, while peripheral self-tolerance exists for constitutively presented somatic self Ag, self-peptide recognized in the context of MHC class II has been shown to sensitize T cells for subsequent activation. We have shown that MHC class II(+)CD86(+)CD40(-) DC, which can be generated from bone marrow in the presence of an NF-kappa B inhibitor, and which constitutively populate peripheral tissues and lymphoid organs in naive animals, can induce Ag-specific tolerance. In this study, we show that CD40(-) human monocyte-derived dendritic cells (DC), generated in the presence of an NF-kappa B inhibitor, signal phosphorylation of TCR zeta, but little proliferation or IFN-gamma in vitro. Proliferation is arrested in the G(1)/G(0) phase of the cell cycle. Surprisingly, responding T cells are neither anergic nor regulatory, but are sensitized for subsequent IFN-gamma production. The data indicate that signaling through NF-kappa B determines the capacity of DC to stimulate T cell proliferation. Functionally, NF-kappa B(-)CD40(-)class II(+) DC may either tolerize or sensitize T cells. Thus, while CD40(-) DC appear to "prime" or prepare T cells, the data imply that signals derived from other cells drive the generation either of Ag-specific regulatory or effector cells in vivo.
矛盾的是,尽管外周自身耐受性针对组成性呈现的体细胞自身抗原存在,但在MHC II类背景下识别的自身肽已被证明可使T细胞对随后的激活敏感。我们已经表明,MHC II(+)CD86(+)CD40(-)树突状细胞(DC)可在存在NF-κB抑制剂的情况下从骨髓生成,并且在幼稚动物中组成性地分布于外周组织和淋巴器官,能够诱导抗原特异性耐受性。在本研究中,我们表明在存在NF-κB抑制剂的情况下生成的CD40(-)人单核细胞衍生树突状细胞(DC)可使TCR ζ发生信号磷酸化,但在体外几乎没有增殖或产生IFN-γ。增殖在细胞周期的G(1)/G(0)期被阻断。令人惊讶的是,反应性T细胞既无反应性也不是调节性的,而是对随后的IFN-γ产生敏感。数据表明通过NF-κB的信号传导决定了DC刺激T细胞增殖的能力。在功能上,NF-κB(-)CD40(-)II类(+)DC可能使T细胞耐受或致敏。因此,虽然CD40(-)DC似乎“启动”或准备T细胞,但数据表明来自其他细胞的信号在体内驱动抗原特异性调节性或效应性细胞的产生。
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