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树突状细胞作为小鼠中微小淋巴细胞刺激位点特异性T细胞反应刺激物的作用。I. 树突状细胞刺激微小淋巴细胞刺激位点反应性T细胞杂交瘤及原发性抗微小淋巴细胞刺激位点混合淋巴细胞反应的不同能力。

The role of dendritic cells as stimulators of minor lymphocyte-stimulating locus-specific T cell responses in the mouse. I. Differential capacity of dendritic cells to stimulate minor lymphocyte-stimulating locus-reactive T cell hybridomas and the primary anti-minor lymphocyte-stimulating locus mixed lymphocyte reaction.

作者信息

Hamilos D L, Mascali J J, Chesnut R W, Young R M, Ishioka G, Grey H M

机构信息

Anna Perahia Addato Clinical Research Facilities, National Jewish Center for Immunology and Respiratory Medicine, Denver, CO 80206.

出版信息

J Immunol. 1989 Feb 15;142(4):1069-78.

PMID:2464636
Abstract

The response of T cells to minor lymphocyte-stimulating locus (Mls) determinants remains poorly understood with respect to the antigenic determinants responsible for T cell stimulation and the types of APC capable of stimulating the response. In this report, we demonstrate that highly purified dendritic cells (DC) as well as B cells have the capacity to stimulate Mls-specific responses. Unseparated spleen cells, purified DC, resting B cells, and activated B cells were compared for their capacity to stimulate several Mls-reactive T cell hybridomas. Whereas the entire panel of Mls-reactive T cell hybridomas was stimulated strongly by unseparated spleen cells and activated B cells, the hybridomas responded only weakly to purified DC or resting B cells. Activation of resting B cells with either B cell stimulatory factor-1 (1 day pre-treatment) or LPS/dextran (2 or 3 day pre-treatment) greatly augmented their Mls-stimulatory capacity. In contrast, the Mls-stimulatory capacity of DC was not augmented by a 1-day pre-treatment with either B cell stimulatory factor-1 or supernatant from the DC-induced primary anti-Mls-MLR. In the primary anti-Mls-MLR, both purified DC and LPS/dextran-stimulated B blasts were found to elicit vigorous T cell proliferative responses. Much weaker responses were elicited by unseparated spleen cells. The stimulation of the primary anti-Mls-MLR by purified DC was further confirmed by producing Mls-specific T cell clones which were preferentially stimulated by DC. Autologous (Mlsb) DC were found to markedly enhance the primary anti-Mls-MLR response to small numbers of Mlsa B blasts. Thus, DC possess other "accessory cell" properties that augment the primary anti-Mls-MLR despite the predicted low level of Mls determinant expression on DC based on the results obtained with Mls-reactive hybridomas. Possible accessory cell properties of DC relevant to this phenomenon are discussed.

摘要

关于负责T细胞刺激的抗原决定簇以及能够刺激该反应的抗原呈递细胞(APC)类型,T细胞对次要淋巴细胞刺激位点(Mls)决定簇的反应仍知之甚少。在本报告中,我们证明高度纯化的树突状细胞(DC)以及B细胞具有刺激Mls特异性反应的能力。比较了未分离的脾细胞、纯化的DC、静息B细胞和活化B细胞刺激几种Mls反应性T细胞杂交瘤的能力。虽然整个Mls反应性T细胞杂交瘤组受到未分离的脾细胞和活化B细胞的强烈刺激,但杂交瘤对纯化的DC或静息B细胞的反应较弱。用B细胞刺激因子-1(预处理1天)或脂多糖/葡聚糖(预处理2或3天)激活静息B细胞,极大地增强了它们的Mls刺激能力。相比之下,用B细胞刺激因子-1或DC诱导的原发性抗Mls混合淋巴细胞反应(MLR)的上清液预处理1天,DC的Mls刺激能力并未增强。在原发性抗Mls-MLR中,发现纯化的DC和脂多糖/葡聚糖刺激的B母细胞均能引发强烈的T细胞增殖反应。未分离的脾细胞引发的反应要弱得多。通过产生优先受DC刺激的Mls特异性T细胞克隆,进一步证实了纯化的DC对原发性抗Mls-MLR的刺激作用。发现自体(Mlsb)DC能显著增强对少量Mlsa B母细胞的原发性抗Mls-MLR反应。因此,尽管根据用Mls反应性杂交瘤获得的结果预测DC上Mls决定簇的表达水平较低,但DC具有其他“辅助细胞”特性,可增强原发性抗Mls-MLR。讨论了与该现象相关的DC可能的辅助细胞特性。

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