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Recombinant interferon-alpha selectively inhibits the production of interleukin-5 by human CD4+ T cells.

机译:重组干扰素-α选择性抑制人CD4 + T细胞产生白介素5。

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摘要

The effects of recombinant IFN-alpha on the production of IL-5 by human CD4+ T cells were first analyzed on resting CD4+ T cells purified from normal PBMC and stimulated either with a combination of PMA and anti-CD28 mAb or anti-CD3 mAb cross-linked on B7-1/CD32-transfected mouse fibroblasts. We found that IFN-alpha profoundly inhibited in a dose-dependent manner IL-5 production by resting CD4+ T cells whereas IL-10 was upregulated in both systems. The addition of a neutralizing anti-IL-10 mAb to PMA and anti-CD28 mAb upregulated IL-5 production by resting CD4+ T cells but did not prevent IFN-alpha-induced IL-5 inhibition. We then analyzed the effect of IFN-alpha on the production of cytokines by differentiated type 2 helper (Th2) CD4+CD3- cells isolated from peripheral blood of two patients with the hypereosinophilic syndrome. In both cases, IFN-alpha markedly inhibited IL-5 production while it induced mild upregulation of IL-4 and IL-10. Finally, the inhibitory effect of IFN-alpha on IL-5 production was confirmed on a panel of Th2 and Th0 clones generated in vitro. In 2 out of 6 clones, IL-5 inhibition was associated with upregulation of IL-4 and IL-10. We conclude that IFN-alpha selectively downregulates IL-5 synthesis by human CD4+ T cells.
机译:首先在正常PBMC纯化的静息CD4 + T细胞上分析重组IFN-α对人CD4 + T细胞产生IL-5的影响,并用PMA和抗CD28 mAb或抗CD3 mAb交叉刺激-在B7-1 / CD32转染的小鼠成纤维细胞上连接。我们发现,IFN-α通过静息CD4 + T细胞以剂量依赖的方式深刻抑制了IL-5的产生,而IL-10在两个系统中均被上调。向PMA中添加中和性抗IL-10 mAb和抗CD28 mAb可通过静息CD4 + T细胞上调IL-5的产生,但不能阻止IFN-α诱导的IL-5抑制。然后,我们分析了从两名患有嗜酸性粒细胞增多症患者的外周血中分离出来的分化型2型辅助(Th2)CD4 + CD3-细胞对IFN-α产生的细胞因子的影响。在这两种情况下,IFN-α均显着抑制IL-5的产生,同时诱导IL-4和IL-10的轻度上调。最后,在体外产生的一组Th2和Th0克隆中证实了IFN-α对IL-5产生的抑制作用。在6个克隆中的2个中,IL-5抑制与IL-4和IL-10的上调相关。我们得出结论,IFN-α选择性下调人CD4 + T细胞的IL-5合成。

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