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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Inhibition of cytokine gene transcription by the human recombinant histamine-releasing factor in human T lymphocytes.
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Inhibition of cytokine gene transcription by the human recombinant histamine-releasing factor in human T lymphocytes.

机译:人重组组胺释放因子在人T淋巴细胞中抑制细胞因子基因转录。

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Human recombinant histamine-releasing factor (HrHRF) preincubation enhances the secretion of histamine, IL-4, and IL-13 from FcepsilonRI-stimulated human basophils. In GM-CSF-primed human eosinophils, HrHRF increases IL-8 production. Our recent experiments were designed to evaluate the effects of HrHRF on human T cell cytokine production. Purified T cells were preincubated with GST-tagged HrHRF, followed by stimulation with PMA and A23187 overnight. A partial inhibition of IL-2 and IL-13 production (30 and 75%, respectively) was detected compared with that in cells treated with PMA/A23187 alone. However, the production of IFN-gamma was similar in PMA/A23187 stimulated cells with or without HrHRF. The inhibition of cytokine protein production was dose dependent and specific to the HrHRF portion of GST-HrHRF. The inhibition was not due to endotoxin, since preincubation with polymyxin B and HrHRF gave similar results to that with HrHRF alone. The same pattern and specificity of cytokine regulation were replicated in the Jurkat T cell line as for primary T cells. The PMA/A23187-stimulated activity of a proximal promoter IL-13, IL-4, or IL-2 luciferase construct transfected into Jurkat cells was partially inhibited (60, 32, or 70%, respectively) upon GST-HrHRF preincubation, suggesting that HrHRF functions to inhibit cytokine production in Jurkat cells by preventing gene transcription. The inhibition of IL-2 promoter activation was specific to the HrHRF portion of GST-HrHRF. We conclude that HrHRF, in addition to functioning as a histamine-releasing factor, can differentially modulate the secretion of cytokines from human basophils, eosinophils, T cells, and murine B cells, suggesting that it may induce a complex array of responses at sites of allergic inflammation.
机译:人重组组胺释放因子(HrHRF)预温育可增强FcepsilonRI刺激的人嗜碱性粒细胞分泌组胺,IL-4和IL-13的能力。在GM-CSF引发的人嗜酸性粒细胞中,HrHRF增加IL-8的产生。我们最近的实验旨在评估HrHRF对人类T细胞细胞因子产生的影响。将纯化的T细胞与GST标签的HrHRF预孵育,然后用PMA和A23187刺激过夜。与单独用PMA / A23187处理的细胞相比,检测到IL-2和IL-13产生的部分抑制(分别为30和75%)。但是,在有或没有HrHRF的PMA / A23187刺激的细胞中,IFN-γ的产生是相似的。细胞因子蛋白产生的抑制是剂量依赖性的,并且对GST-HrHRF的HrHRF部分具有特异性。抑制不是由于内毒素引起的,因为与多粘菌素B和HrHRF的预温育与单独使用HrHRF的预育相类似。在Jurkat T细胞系中复制了与原代T细胞相同的细胞因子调节模式和特异性。 GST-HrHRF预温育后,转染到Jurkat细胞中的近端启动子IL-13,IL-4或IL-2荧光素酶构建体的PMA / A23187刺激的活性被部分抑制(分别为60%,32%或70%),这表明HrHRF通过阻止基因转录来抑制Jurkat细胞中细胞因子的产生。 IL-2启动子激活的抑制作用对GST-HrHRF的HrHRF部分具有特异性。我们得出的结论是,HrHRF除了起组胺释放因子的作用外,还可以差异地调节人嗜碱性粒细胞,嗜酸性粒细胞,T细胞和鼠B细胞的细胞因子分泌,这提示它可能在以下部位诱导一系列复杂的反应:过敏性炎症。

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