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细胞毒性T细胞既能产生白细胞介素2,又能对其做出反应。

Cytotoxic T cells both produce and respond to interleukin 2.

作者信息

Andrus L, Granelli-Piperno A, Reich E

出版信息

J Exp Med. 1984 Feb 1;159(2):647-52. doi: 10.1084/jem.159.2.647.

Abstract

Interleukin 2 (IL-2) is a T cell-derived lymphokine that serves as a cofactor for the in vitro response of T lymphocytes to antigen and plays an important role in regulating the growth and/or differentiation of these cells (1, 2). It has been postulated (2, 3) that IL-2 is produced by a discrete regulatory T cell subset, with its effects being exerted on a second, functionally distinct subpopulation of T cells. Cytotoxic T cells have been included in the IL-2-responsive subset (3). Several models of immune regulation have further assumed that the T lymphocyte pool is divided into a complex array of genetically preprogrammed T cell subtypes, each performing a specific regulatory or effector function (4, 5). However, recent results from several laboratories (6-8) have failed to support such a strict functional subdivision of the T cell pool. The availability of highly purified mouse IL-2 (1) prompted us to reevaluate the distinction, if any, between IL-2-producing and IL-2- responsive T cells. For this purpose, we resorted to a cell-cloning procedure using activated T lymphocytes that were maintained only for short periods in culture. T cell clones were tested for cytotoxic activity, responsiveness to IL-2, and for the capacity to produce IL-2 after appropriate stimulation. We found no evidence for the existence of a major functional subdivision involving these parameters among alloantigen-activated T cells: the majority of clones analyzed could perform all three functions.

摘要

白细胞介素2(IL-2)是一种由T细胞产生的淋巴因子,它作为T淋巴细胞在体外对抗原反应的辅助因子,并在调节这些细胞的生长和/或分化中发挥重要作用(1,2)。据推测(2,3),IL-2由一个离散的调节性T细胞亚群产生,其作用施加于第二个功能上不同的T细胞亚群。细胞毒性T细胞已被纳入对IL-2有反应的亚群(3)。几种免疫调节模型进一步假定,T淋巴细胞库被分为一系列复杂的基因预编程T细胞亚型,每个亚型执行特定的调节或效应功能(4,5)。然而,几个实验室最近的结果(6-8)未能支持T细胞库如此严格的功能细分。高度纯化的小鼠IL-2的可得性(1)促使我们重新评估产生IL-2的T细胞和对IL-2有反应的T细胞之间是否存在区别。为此,我们采用了一种细胞克隆程序,使用仅在培养中短期维持的活化T淋巴细胞。对T细胞克隆进行细胞毒性活性、对IL-2的反应性以及在适当刺激后产生IL-2的能力的测试。我们没有发现证据表明在同种异体抗原激活的T细胞中存在涉及这些参数的主要功能细分:分析的大多数克隆都能执行所有三种功能。

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本文引用的文献

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