γ干扰素对静息T细胞中Ly-6复合体表面分子的选择性上调：Ly-6A/E和TAP抗原优先增强。

Selective up-regulation by interferon-gamma of surface molecules of the Ly-6 complex in resting T cells: the Ly-6A/E and TAP antigens are preferentially enhanced.

作者信息

Dumont F J, Dijkmans R, Palfree R G, Boltz R D, Coker L

出版信息

Eur J Immunol. 1987 Aug;17(8):1183-91. doi: 10.1002/eji.1830170816.

Abstract

Surface molecules encoded by the murine Ly-6 locus can transduce triggering signals in T cells and thus may play important roles in T cell function. Previously, we found that Ly-6 molecules are up-regulated by interferon (IFN)-alpha/beta in resting T cells. Here, we examined the possible influence of IFN-gamma on these molecules. Purified T cells from C57BL/6 (Ly-6.2) and BALB/c (Ly-6.1) mice were incubated in vitro with recombinant murine IFN-gamma and the expression of Ly-6 antigens was measured by flow cytofluorometry. It was found that both Ly-6A/E and T cell-activating protein (TAP) molecules are markedly enhanced while Ly-6C is less affected. Under the same conditions, other T cell surface molecules showed no or marginal changes. The effect of IFN-gamma on Ly-6A/E and TAP expression reached a maximum with as little as 10 U/ml and required only 18-24 h of incubation. Moreover, the enhancement of Ly-6A expression induced by IFN-gamma was stable for at least 5 days. Analysis of T cell subsets further revealed that IFN-gamma-induced augmentation of Ly-6A (C57BL/6 mice) involves both Lyt-2+ and L3T4+ cells while the increase of Ly-6E (BALB/c mice) is more pronounced in Lyt-2+ cells. The functional consequence of these phenotypic alterations was evaluated by studying the mitogenic responses of T cells to antibody-mediated Ly-6 cross-linking in the presence of phorbol myristate acetate. Pretreatment of resting T cells with IFN-gamma dramatically increased the responses to anti-Ly-6A and anti-Ly-6E monoclonal antibodies. IFN-gamma treatment also boosted the stimulation induced by anti-TAP monoclonal antibody when this stimulation was performed under suboptimal conditions. Therefore, IFN-gamma selectively up-regulates the Ly-6A/E and TAP activation pathways in resting T cells. We speculate that this effect may contribute to the immunoregulatory activities of IFN-gamma.

摘要

由小鼠Ly-6基因座编码的表面分子可在T细胞中传导触发信号，因此可能在T细胞功能中发挥重要作用。此前，我们发现Ly-6分子在静息T细胞中被干扰素（IFN）-α/β上调。在此，我们研究了IFN-γ对这些分子的可能影响。将来自C57BL/6（Ly-6.2）和BALB/c（Ly-6.1）小鼠的纯化T细胞与重组小鼠IFN-γ在体外孵育，并用流式细胞荧光术检测Ly-6抗原的表达。结果发现，Ly-6A/E和T细胞激活蛋白（TAP）分子均显著增强，而Ly-6C受影响较小。在相同条件下，其他T细胞表面分子无变化或仅有微小变化。IFN-γ对Ly-6A/E和TAP表达的影响在低至10 U/ml时即达到最大值，且仅需孵育18 - 24小时。此外，IFN-γ诱导的Ly-6A表达增强至少可持续5天。对T细胞亚群的分析进一步表明，IFN-γ诱导的Ly-6A（C57BL/6小鼠）增加涉及Lyt-2 +和L3T4 +细胞，而Ly-6E（BALB/c小鼠）的增加在Lyt-2 +细胞中更为明显。通过研究在佛波醇肉豆蔻酸酯乙酸存在下T细胞对抗体介导的Ly-6交联的促有丝分裂反应，评估了这些表型改变的功能后果。用IFN-γ预处理静息T细胞显著增加了对抗Ly-6A和抗Ly-6E单克隆抗体的反应。当在次优条件下进行刺激时，IFN-γ处理也增强了抗TAP单克隆抗体诱导的刺激。因此，IFN-γ选择性地上调静息T细胞中的Ly-6A/E和TAP激活途径。我们推测这种效应可能有助于IFN-γ的免疫调节活性。