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γ干扰素在免疫调节中的抗增殖作用。I. γ干扰素抑制Th2而非Th1小鼠辅助性T淋巴细胞克隆的增殖。

Anti-proliferative effect of IFN-gamma in immune regulation. I. IFN-gamma inhibits the proliferation of Th2 but not Th1 murine helper T lymphocyte clones.

作者信息

Gajewski T F, Fitch F W

机构信息

Department of Pathology, University of Chicago, IL 60637.

出版信息

J Immunol. 1988 Jun 15;140(12):4245-52.

PMID:2967332
Abstract

A biphasic dose-response curve was observed when the IL-1-dependent HTL clone D10 was exposed to IL-1 plus supernatants from some activated T cell clones but not others. The active component that inhibited proliferation at high concentrations of these supernatants appeared to be IFN-gamma based on the following findings: 1) the biphasic pattern of responsiveness correlated with the presence of IFN-gamma in the supernatants; 2) an anti-IFN-gamma mAb augmented the proliferation of D10 cells to these supernatants; 3) rIFN-gamma inhibited profoundly the response of D10 cells stimulated with rIL-1 plus supernatant from activated D10 cells or with rIL-1 plus rIL-4; 4) the response of D10 cells to rIL-1 plus rIL-2 also was inhibited by rIFN-gamma, although to a lesser extent. The proliferation of an additional Th2 clone stimulated with rIL-1 plus rIL-4 or rIL-2 also was inhibited by rIFN-gamma, implicating IFN-gamma as an inhibitory lymphokine for Th2 cells in general. rIFN-gamma did not affect the proliferation of two Th1 clones, nor did it affect the proliferation of an unconventional HTL clone which produces both IL-4 and IFN-gamma and proliferates in response to IL-2 or IL-4 in an IL-1-independent fashion. The proliferation of D10 cells stimulated by Ag or by immobilized anti-CD3 antibody also was blocked by rIFN-gamma, whereas IL-4 production in response to these stimuli was unaffected, indicating that proliferation and not general cell function was specifically inhibited. Collectively, these data implicate IFN-gamma as a suppressive factor for the proliferation of the subset of HTL designated Th2, and suggest that the relative amounts of the various lymphokines present during an immune response may direct which T cell types increase in number.

摘要

当IL-1依赖的HTL克隆D10暴露于IL-1加上某些活化T细胞克隆的上清液(而非其他上清液)时,观察到双相剂量反应曲线。基于以下发现,在这些上清液高浓度时抑制增殖的活性成分似乎是IFN-γ:1)反应的双相模式与上清液中IFN-γ的存在相关;2)抗IFN-γ单克隆抗体增强了D10细胞对这些上清液的增殖;3)重组IFN-γ深刻抑制了用重组IL-1加活化D10细胞的上清液或重组IL-1加重组IL-4刺激的D10细胞的反应;4)D10细胞对重组IL-1加重组IL-2的反应也被重组IFN-γ抑制,尽管程度较小。用重组IL-1加重组IL-4或重组IL-2刺激的另一个Th2克隆的增殖也被重组IFN-γ抑制,这表明IFN-γ总体上是Th2细胞的抑制性淋巴因子。重组IFN-γ不影响两个Th1克隆的增殖,也不影响一个非传统HTL克隆的增殖,该克隆产生IL-4和IFN-γ,并以不依赖IL-1的方式对IL-2或IL-4作出反应而增殖。重组IFN-γ也阻断了由抗原或固定化抗CD3抗体刺激的D10细胞的增殖,而对这些刺激产生的IL-4产生没有影响,表明增殖而非一般细胞功能被特异性抑制。总体而言,这些数据表明IFN-γ是指定为Th2的HTL亚群增殖的抑制因子,并表明免疫反应期间存在的各种淋巴因子的相对量可能指导哪些T细胞类型数量增加。

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