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Requirement for delivery of signals by physical interaction and soluble factors from accessory cells in the induction of receptor-mediated T cell proliferation. Effectiveness of IFN-gamma modulation of accessory cells for physical interaction with T cells.

作者信息

Kawakami K, Yamamoto Y, Kakimoto K, Onoue K

机构信息

Department of Biochemistry, Kumamoto University Medical School, Japan.

出版信息

J Immunol. 1989 Mar 15;142(6):1818-25.

PMID:2493498
Abstract

We analyzed the mechanism by which accessory cells support the induction of the proliferation of human peripheral blood T cells by a monoclonal anti-CD3 antibody, OKT3. Cross-linking of T cell receptor/CD3 complex by anti-CD3 coupled to latex beads and the addition of IL-1 are not enough to induce the IL-2 production and proliferation of T cells extensively depleted of accessory cells, while the addition of both the culture supernatant of macrophages or a monoblastic cell line, U937 cells, and the paraformaldehyde-fixed macrophages or U937 cells which had been precultured with interferon-gamma before fixation into the culture of the T cells with anti-CD3-latex did induce the T cell proliferation. Lack of the addition of either one of these did not induce the response. These results indicate that the signal(s) delivered by soluble factors released from the accessory cells and that delivered by the physical interaction between accessory cells and T cells are both required for the induction of IL 2 production and proliferation of T cells by anti-CD3-latex. Importantly, the macrophages or U937 cells had to be cultured with Con A-stimulated lymphocyte culture supernatant or IFN-gamma prior to fixation with paraformaldehyde, suggesting that a molecule(s) inducible on accessory cells surface by IFN-gamma or other lymphokine is necessary for the effective accessory cell-T cell interaction to induce the T cell response. It was further revealed that the activity of the culture supernatant of accessory cells may be mediated synergistically by IL 1 and a certain other factor(s) and was actually shown to be replaced by the combined addition of rIL-1 and rIL-6 but not by rIL-1 alone. The experimental system described here will be very useful for dissecting the accessory functions for T cell activation.

摘要

相似文献

1
Requirement for delivery of signals by physical interaction and soluble factors from accessory cells in the induction of receptor-mediated T cell proliferation. Effectiveness of IFN-gamma modulation of accessory cells for physical interaction with T cells.
J Immunol. 1989 Mar 15;142(6):1818-25.
2
Signal delivery by physical interaction and soluble factors from accessory cells in the induction of receptor-mediated T-cell proliferation. Synergistic effect of BSF-2/IL-6 and IL-1.在受体介导的T细胞增殖诱导过程中,辅助细胞通过物理相互作用和可溶性因子进行信号传递。BSF-2/IL-6与IL-1的协同效应。
Immunology. 1989 Jul;67(3):314-20.
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Immobilized anti-CD3 monoclonal antibodies induce accessory cell-independent lymphokine production, proliferation and helper activity in human T lymphocytes.固定化抗CD3单克隆抗体可诱导人T淋巴细胞产生不依赖辅助细胞的淋巴因子、增殖并具有辅助活性。
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Induction of human monocyte IL-1 mRNA and secretion during anti-CD3 mitogenesis requires two distinct T cell-derived signals.在抗CD3促有丝分裂过程中,人单核细胞IL-1 mRNA的诱导及分泌需要两种不同的T细胞衍生信号。
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Differences in the stimulating capacity of immobilized anti-CD3 monoclonal antibodies: variable dependence on interleukin-1 as a helper signal for T-cell activation.固定化抗CD3单克隆抗体刺激能力的差异:对白细胞介素-1作为T细胞激活辅助信号的可变依赖性。
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Accessory cell independent proliferation of human T4 cells stimulated by immobilized monoclonal antibodies to CD3.通过固定化抗CD3单克隆抗体刺激的人T4细胞的辅助细胞非依赖性增殖。
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7
Cross-linking Fc receptors on monocytes triggers IL-6 production. Role in anti-CD3-induced T cell activation.单核细胞上的Fc受体交联可触发白细胞介素-6的产生。在抗CD3诱导的T细胞活化中的作用。
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J Immunol. 1986 Nov 15;137(10):3065-73.

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