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白细胞介素-10可对免疫球蛋白E与免疫球蛋白G4的产生进行差异调节。

IgE versus IgG4 production can be differentially regulated by IL-10.

作者信息

Jeannin P, Lecoanet S, Delneste Y, Gauchat J F, Bonnefoy J Y

机构信息

Geneva Biomedical Research Institute, Immunology Department, Glaxo Wellcome Research and Development SA, Switzerland.

出版信息

J Immunol. 1998 Apr 1;160(7):3555-61.

PMID:9531318
Abstract

Allergen-specific IgE plays a key role in the physiopathology of allergic disorders. This IgE response is usually accompanied by a production of IgG4. Indirect evidence suggests that IgG4 may not be a sensitizing Ab but, in contrast, could be protective. As such, it may be of potential therapeutic interest to selectively modulate IgE vs IgG4 production. To date, IgE and IgG4 switching seems to be controlled by common mechanisms. We report here that IL-10 has a differential effect on IgE vs IgG4 production by PBMC. IL-10 decreases epsilon transcript expression and IgE production induced by IL-4 when added during the first 3 days of in vitro culture, suggesting that IL-10 decreases IL-4-induced IgE switching. In contrast, if added later on B cells that are already IgE switched, IL-10 potentiates IgE production. Interestingly, whatever the time of addition, IL-10 augments IL-4-induced gamma4 transcript expression and IgG4 production, with a maximal effect when added during the first 3 days. As IL-10 is not a switch factor for IgG4, it is likely that IL-10 enhances IgG4 production by potentiating IL-4-induced IgG4 switching. However, IL-10 may also act by enhancing the growth and/or differentiation of cells that are already IgG4 committed. Finally, CD40 ligation reverses the early down-regulating effect of IL-10 on IgE production. These results are the first evidence of a molecule that differentially regulates IgE vs IgG4 production, thereby suggesting the existence of a pathway(s) selectively controlling their production.

摘要

变应原特异性IgE在过敏性疾病的病理生理学中起关键作用。这种IgE反应通常伴随着IgG4的产生。间接证据表明,IgG4可能不是致敏抗体,相反,它可能具有保护作用。因此,选择性调节IgE与IgG4的产生可能具有潜在的治疗意义。迄今为止,IgE和IgG4的类别转换似乎受共同机制控制。我们在此报告,IL-10对PBMC产生IgE与IgG4具有不同的作用。在体外培养的前3天添加IL-10时,它会降低ε转录本表达以及IL-4诱导的IgE产生,这表明IL-10可减少IL-4诱导的IgE类别转换。相反,如果在已经发生IgE类别转换的B细胞上较晚添加IL-10,则会增强IgE的产生。有趣的是,无论添加时间如何,IL-10都会增加IL-4诱导的γ4转录本表达和IgG4产生,在第1天添加时效果最佳。由于IL-10不是IgG4的类别转换因子,IL-10可能通过增强IL-4诱导的IgG4类别转换来增加IgG4的产生。然而,IL-10也可能通过增强已定向产生IgG4的细胞的生长和/或分化来发挥作用。最后,CD40连接可逆转IL-10对IgE产生的早期下调作用。这些结果首次证明了一种分子对IgE与IgG4的产生具有不同的调节作用,从而提示存在选择性控制它们产生的途径。

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IgE versus IgG4 production can be differentially regulated by IL-10.白细胞介素-10可对免疫球蛋白E与免疫球蛋白G4的产生进行差异调节。
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