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T细胞克隆与辅助细胞和辅助性T细胞相互作用以产生增殖反应。

T cell clones interacting with accessory and T helper cells for a proliferative response.

作者信息

Di Pauli R, Brückner T

出版信息

Eur J Immunol. 1984 Oct;14(10):915-22. doi: 10.1002/eji.1830141011.

DOI:10.1002/eji.1830141011
PMID:6237920
Abstract

The requirement for cell interactions in T cell activation has been studied with two continuously in vitro growing T cell clones. These clones are specific for minor histocompatibility antigens, are H-2K restricted, and one clone is functionally a cytolytic T lymphocyte. Both can proliferate when interleukin 2 is added to the cultures, but for continuous growth they require irradiated spleen cells carrying the specific minor histocompatibility antigen and the restricting H-2. In this study we show that for proliferation the clones require at least two cell populations in the stimulator spleen, one is a splenic-adherent cell (SAC), the other a T cell. The SAC are plastic adherent, Thy-1-, Ia+. The T cells are nylon wool nonadherent, Thy-1+, Lyt-1+2- and Ia-. Cell mixing experiments of stimulator cells (all were done with H-2-syngeneic cells), depleted of either SAC or T cells confirm the requirement for a specific interaction between these two cell types and the T clone. Neither SAC, syngeneic with the T clone when mixed with T cells of the stimulator type, nor T cells syngeneic with the clone added to stimulator SAC, can induce an optimal proliferative response. Such a response is obtained only if both cell types, SAC and T cells, are of the stimulating genotype. This suggests that, in addition to an interaction of clonal T cells with SAC, a specific recognition at the T cell level between T stimulator and T clone is necessary. The interaction of the T clones with stimulator SAC and T cells leads to an activation, mediated by antigen recognition, of all three cell populations. Since we also show that each of the stimulator cell types are impaired by ultraviolet light irradiation, we conclude that factor production by SAC and T helpers is the final prerequisite for clonal expansion.

摘要

利用两个体外持续生长的T细胞克隆研究了T细胞激活中细胞间相互作用的要求。这些克隆对次要组织相容性抗原有特异性,受H-2K限制,其中一个克隆在功能上是细胞毒性T淋巴细胞。当向培养物中添加白细胞介素2时,两者均可增殖,但要持续生长,它们需要携带特异性次要组织相容性抗原和限制性H-2的经照射的脾细胞。在本研究中,我们表明,为了增殖,这些克隆在刺激脾中至少需要两个细胞群体,一个是脾黏附细胞(SAC),另一个是T细胞。SAC可被塑料黏附,Thy-1阴性、Ia阳性。T细胞不能被尼龙毛黏附,Thy-1阳性、Lyt-1阳性2阴性且Ia阴性。刺激细胞(所有实验均使用H-2同基因细胞)的细胞混合实验,去除SAC或T细胞后,证实了这两种细胞类型与T克隆之间特异性相互作用的必要性。与刺激型T细胞混合时与T克隆同基因的SAC,或添加到刺激型SAC中的与克隆同基因的T细胞,均不能诱导最佳增殖反应。只有当两种细胞类型,即SAC和T细胞,均为刺激基因型时,才能获得这种反应。这表明,除了克隆性T细胞与SAC相互作用外,T刺激细胞与T克隆之间在T细胞水平的特异性识别也是必要的。T克隆与刺激型SAC和T细胞的相互作用导致所有三个细胞群体通过抗原识别介导的激活。由于我们还表明,每种刺激细胞类型都受到紫外线照射的损害,因此我们得出结论,SAC和T辅助细胞产生因子是克隆扩增的最终先决条件。

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