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白细胞介素1介导产生白细胞介素4(IL-4)的T淋巴细胞的激活。通过依赖IL-4和不依赖IL-4的机制进行增殖。

Interleukin 1-mediated activation of interleukin 4 (IL 4)-producing T lymphocytes. Proliferation by IL 4-dependent and IL 4-independent mechanisms.

作者信息

Ho S N, Abraham R T, Nilson A, Handwerger B S, McKean D J

出版信息

J Immunol. 1987 Sep 1;139(5):1532-40.

PMID:3114369
Abstract

The role of IL 1 in the activation of IL 4-producing murine T cell clones was investigated by using a calcium ionophore (ionomycin) or a phorbol ester (12-O-tetradecanoylphorbol 13-acetate; TPA) as T cell receptor-independent costimuli. The use of these pharmacologic agents to investigate IL 1-mediated T cell activation revealed two distinct mechanisms of activation. IL 1 in combination with ionomycin (iono/rIL 1) stimulated a proliferative response that was associated with the production of IL 4 as measured by lymphokine bioassay and mRNA studies. Furthermore, inhibition of this proliferative response with an anti-IL 4 monoclonal antibody or cyclosporine indicated that IL 4 functions as an autocrine growth factor. In contrast, IL 1 synergized with TPA (TPA/rIL 1) to induce proliferation in the absence of either IL 4 or IL 2 gene transcription or lymphokine secretion. The IL 4-independence of this activation mechanism was further supported by the failure of both anti-IL 4 antibodies and cyclosporine to inhibit the response. In addition, activation by TPA/rIL 1 caused no detectable alteration in cytoplasmic calcium levels. Both IL 4-dependent and IL 4-independent activation responses were associated with the expression of functional receptors for IL 2 as well as IL 4. Characterization of these activation responses suggests that the synergistic activity of IL 1 during T cell activation is multipotential. The nature of an IL 1-dependent T cell growth response, therefore, may vary depending on the balance of intracellular signals generated concurrently through the T cell receptor complex and other regulatory surface molecules.

摘要

通过使用钙离子载体(离子霉素)或佛波酯(12-O-十四烷酰佛波醇13-乙酸酯;TPA)作为不依赖T细胞受体的共刺激剂,研究了白细胞介素1(IL 1)在激活产生IL 4的小鼠T细胞克隆中的作用。使用这些药物制剂来研究IL 1介导的T细胞激活揭示了两种不同的激活机制。IL 1与离子霉素联合使用(离子霉素/rIL 1)刺激了增殖反应,通过淋巴因子生物测定和mRNA研究测量,该反应与IL 4的产生相关。此外,用抗IL 4单克隆抗体或环孢素抑制这种增殖反应表明IL 4作为自分泌生长因子发挥作用。相比之下,IL 1与TPA协同作用(TPA/rIL 1)在没有IL 4或IL 2基因转录或淋巴因子分泌的情况下诱导增殖。抗IL 4抗体和环孢素均未能抑制该反应,进一步支持了这种激活机制不依赖IL 4。此外,TPA/rIL 1激活未引起细胞质钙水平的可检测变化。依赖IL 4和不依赖IL 4的激活反应均与IL 2以及IL 4功能性受体的表达相关。对这些激活反应的表征表明,IL 1在T细胞激活过程中的协同活性具有多潜能性。因此,依赖IL 1的T细胞生长反应的性质可能会因通过T细胞受体复合物和其他调节性表面分子同时产生的细胞内信号的平衡而有所不同。

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