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白细胞介素1在小鼠II类限制性T淋巴细胞克隆抗原特异性激活中的作用。

The role of IL 1 in the antigen-specific activation of murine class II-restricted T lymphocyte clones.

作者信息

McKean D J, Nilson A, Beck B N, Giri J, Mizel S B, Handwerger B S

出版信息

J Immunol. 1985 Nov;135(5):3205-16.

PMID:2413115
Abstract

The role of IL 1 in the antigen-specific activation of class II-restricted T lymphocytes was examined by using a model system consisting of cloned WEHI 5 B lymphoma accessory cells and class II-restricted, soluble antigen- or alloantigen-reactive T cell clones. The addition of exogenous recombinant IL 1 to the T cell cultures resulted in a significant enhancement of the antigen-specific T cell proliferation response, but at best, only small increases in IL 2 release. Goat IgG anti-IL 1 antibodies were added to the T cell cultures to assess their effect on T cell activation. The IL 1 enhancement of the T cell proliferation response was inhibited by the anti-IL 1 antibodies in a dose-dependent manner. In contrast, only modest levels (10 to 25%) of proliferation inhibition were observed in T cell cultures containing either WEHI 5 or splenocyte accessory cells but no exogenous IL 1. When the anti-IL 1 antibodies were added to primary mixed lymphocyte cultures stimulated by WEHI 5 cells in the absence of exogenous IL 1, no significant inhibition of proliferation was observed. A small but statistically significant proliferation inhibition was observed when anti-IL 1 antibodies were added to mixed lymphocyte reaction cultures stimulated by splenocytes. Two-color cytofluorometric analysis of the effects of IL 1 on antigen-activated T cell clones demonstrated that under suboptimal stimulation conditions, IL 1 stimulated a small but significant increase in the number of T cells bearing IL 2 receptors. In the presence of optimal numbers of WEHI 5 accessory cells, IL 1 enhanced T cell proliferation in the absence of a detectable increase in the number of T cells bearing IL 2 receptors, the number of IL 2 receptors per T cell, or the levels of IL 2 released. Finally, exogenous IL 1 can be added as late as 18 to 24 hr after culture initiation without significantly reducing its ability to enhance the T cell proliferation response. These data indicate that IL 1 has pleiotropic effects on murine T lymphocytes and can function to enhance T cell activation at multiple points during the activation sequence.

摘要

利用一个由克隆的WEHI 5 B淋巴瘤辅助细胞以及II类限制性、可溶性抗原或同种异体抗原反应性T细胞克隆组成的模型系统,研究了白细胞介素1(IL 1)在II类限制性T淋巴细胞抗原特异性激活中的作用。向T细胞培养物中添加外源性重组IL 1导致抗原特异性T细胞增殖反应显著增强,但IL 2释放最多仅略有增加。将山羊IgG抗IL 1抗体添加到T细胞培养物中,以评估其对T细胞激活的影响。抗IL 1抗体以剂量依赖的方式抑制了IL 1对T细胞增殖反应的增强作用。相比之下,在含有WEHI 5或脾细胞辅助细胞但无外源性IL 1的T细胞培养物中,仅观察到适度水平(10%至25%)的增殖抑制。当在无外源性IL 1的情况下,将抗IL 1抗体添加到由WEHI 5细胞刺激的原发性混合淋巴细胞培养物中时,未观察到显著的增殖抑制。当将抗IL 1抗体添加到由脾细胞刺激的混合淋巴细胞反应培养物中时,观察到了轻微但具有统计学意义的增殖抑制。对IL 1对抗原激活的T细胞克隆的影响进行的双色细胞荧光分析表明,在次优刺激条件下,IL 1刺激了携带IL 2受体的T细胞数量的少量但显著增加。在存在最佳数量的WEHI 5辅助细胞的情况下,IL 1增强了T细胞增殖,而未检测到携带IL 2受体的T细胞数量、每个T细胞的IL 2受体数量或释放的IL 2水平的增加。最后,在培养开始后18至24小时添加外源性IL 1,其增强T细胞增殖反应的能力不会显著降低。这些数据表明,IL 1对小鼠T淋巴细胞具有多效性作用,并且可以在激活序列的多个点发挥作用以增强T细胞激活。

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