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白细胞介素2诱导抑制性T细胞

Induction of suppressor T cells by interleukin 2.

作者信息

Ting C C, Yang S S, Hargrove M E

出版信息

J Immunol. 1984 Jul;133(1):261-6.

PMID:6233372
Abstract

The optimal concentration of interleukin 2 (IL 2) for maintaining the in vitro growth of T cells was quite different from that required for the induction of cytotoxic T lymphocytes (CTL) in nu/nu spleen cells. Higher concentrations of IL 2-containing preparations (10 to 30% v/v or 5 to 15 U/ml) were needed to promote the T cell growth, whereas lower concentrations (1 to 3% v/v or 0.5 to 1.5 U/ml) were needed to generate alloreactive CTL. It was further shown that the addition of high concentrations of IL 2 (10 to 30%) suppressed the generation of alloreactive CTL in conventional MLC. High concentrations of IL 2 induced the generation of antigen-nonspecific suppressor T cells in normal spleen cell cultures and augmented the generation of antigen-specific suppressor T cells in MLC. These suppressor cells suppressed the generation of CTL in fresh MLC and in polyclonal CTL cultures. These suppressor T cells could be induced by rat (spleen)-produced, murine (EL-4 cells) produced IL 2 preparations, and a purified human recombinant IL 2 (HR-IL2). The ability to induce suppressor cells correlated with the activity of IL 2 present in these preparations and was independent of their ability to induce cytotoxic effectors. These findings indicate that IL 2 may play a dual role in the regulation of CTL responses. We suggest that during antigen sensitization, the initial endogenous production of lower levels of IL 2 provided the second signal for the differentiation and proliferation of CTL. When higher levels of IL 2 were produced later, the suppressor T cell precursors were activated and differentiated into suppressor effectors to regulate the CTL response.

摘要

维持T细胞体外生长的白细胞介素2(IL-2)最佳浓度与诱导无胸腺裸鼠脾脏细胞中的细胞毒性T淋巴细胞(CTL)所需的浓度大不相同。促进T细胞生长需要更高浓度的含IL-2制剂(10%至30% v/v或5至15 U/ml),而产生同种反应性CTL则需要较低浓度(1%至3% v/v或0.5至1.5 U/ml)。进一步研究表明,添加高浓度的IL-2(10%至30%)会抑制传统混合淋巴细胞培养(MLC)中同种反应性CTL的产生。高浓度的IL-2在正常脾细胞培养物中诱导产生抗原非特异性抑制性T细胞,并增强MLC中抗原特异性抑制性T细胞的产生。这些抑制性细胞抑制新鲜MLC和多克隆CTL培养物中CTL的产生。这些抑制性T细胞可由大鼠(脾脏)产生的、小鼠(EL-4细胞)产生的IL-2制剂以及纯化的人重组IL-2(HR-IL2)诱导产生。诱导抑制性细胞的能力与这些制剂中IL-2的活性相关,且与其诱导细胞毒性效应器的能力无关。这些发现表明,IL-2可能在CTL反应的调节中发挥双重作用。我们认为,在抗原致敏过程中,最初内源性产生的较低水平的IL-2为CTL的分化和增殖提供了第二个信号。当随后产生较高水平的IL-2时,抑制性T细胞前体被激活并分化为抑制性效应器,以调节CTL反应。

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