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CD8 + 抑制性T淋巴细胞连续系的产生与特性分析

Generation and characterization of continuous lines of CD8+ suppressor T lymphocytes.

作者信息

Aune T M, Pogue S L

机构信息

Department of Molecular Immunology, Genentech, Inc., South San Francisco, CA 94080.

出版信息

J Immunol. 1989 Jun 1;142(11):3731-9.

PMID:2469724
Abstract

The ability to grow normal T lymphocytes in long term culture has advanced our understanding of T cell biology. The growth of CD4+ cell lines allowed a further evaluation and appreciation of functional subtypes within this group. Cytotoxic CD8+ T cells have been characterized as well. The routine and continuous culture of Ag-nonspecific CD8+ Ts cells has been difficult to achieve. We have found that CD8+ T cells that suppress T cell proliferation and lack cytotoxic activity against T cells can be routinely obtained from PWM or PHA-stimulated PBMC. Continuous culture of T cell blasts from PWM or PHA-stimulated PBMC resulted in the growth of CD4+ and CD8+ T cells. These lines developed suppressor cell activity within 7 days after stimulation with PWM and 3 to 4 wk after stimulation with PHA. Concomitant with the development of suppressor activity was the loss of CD4+ T cells resulting in homogeneous lines of CD8+ suppressor cells. These cell lines have been maintained in continuous culture for greater than 6 mo by addition of rIL-2 twice weekly and restimulation with feeder cells and PHA every 2 wk. Activity of these cell lines was relatively resistant to irradiation or treatment with mitomycin C. Both cell lines suppressed proliferation of autologous or heterologous CD4+ T cells stimulated with PWM, OKT3, or tetanus toxoid but failed to suppress proliferation of CD4+ T cells in a mixed lymphocyte reaction. CD4+ T cells stimulated with PWM produced equivalent amounts of IL-2 in the presence or absence of Ts cells but failed to express the IL-2R (TAC) on their surface in the presence of Ts cells. By contrast, CD4+ T cell lines or cytotoxic CD8+ T cell lines failed to suppress proliferation of CD4+ T cells. With these results we describe methods for the generation and continuous culture of Ag-nonspecific CD8+ Ts cells and define some of their properties. These cells lines should be helpful in further elucidating the functional and phenotypic repertoire of CD8+ Ts cells.

摘要

在长期培养中生长正常T淋巴细胞的能力推动了我们对T细胞生物学的理解。CD4+细胞系的生长使得对该组内功能亚型的进一步评估和认识成为可能。细胞毒性CD8+ T细胞也已得到表征。常规且持续地培养抗原非特异性CD8+ Ts细胞一直难以实现。我们发现,抑制T细胞增殖且对T细胞缺乏细胞毒性活性的CD8+ T细胞可常规地从经PWM或PHA刺激的PBMC中获得。对经PWM或PHA刺激的PBMC中的T细胞母细胞进行持续培养导致了CD4+和CD8+ T细胞的生长。这些细胞系在经PWM刺激7天后以及经PHA刺激3至4周后产生了抑制细胞活性。伴随抑制活性的发展,CD4+ T细胞减少,从而产生了均一的CD8+抑制细胞系。通过每周两次添加rIL-2以及每2周用饲养细胞和PHA进行再刺激,这些细胞系已在持续培养中维持了超过6个月。这些细胞系的活性对辐照或丝裂霉素C处理相对抗性。两种细胞系均抑制经PWM、OKT3或破伤风类毒素刺激的自体或异源CD4+ T细胞的增殖,但在混合淋巴细胞反应中未能抑制CD4+ T细胞的增殖。在有或没有Ts细胞存在的情况下,经PWM刺激的CD4+ T细胞产生等量的IL-2,但在有Ts细胞存在的情况下未能在其表面表达IL-2R(TAC)。相比之下,CD4+ T细胞系或细胞毒性CD8+ T细胞系未能抑制CD4+ T细胞的增殖。基于这些结果,我们描述了抗原非特异性CD8+ Ts细胞的产生和持续培养方法,并定义了它们的一些特性。这些细胞系应有助于进一步阐明CD8+ Ts细胞的功能和表型特征。

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