Lordan James L, Bucchieri Fabio, Richter Audrey, Konstantinidis Athanassias, Holloway John W, Thornber Matthew, Puddicombe Sarah M, Buchanan Diana, Wilson Susan J, Djukanović Ratko, Holgate Stephen T, Davies Donna E
School of Medicine, Respiratory Cell and Molecular Biology Division, Southampton General Hospital, Southampton, United Kingdom.
J Immunol. 2002 Jul 1;169(1):407-14. doi: 10.4049/jimmunol.169.1.407.
In sensitized individuals, exposure to allergens such as Dermatophagoides pteronyssinus (Der p) causes Th2 polarization and release of cytokines, including IL-4 and IL-13. Because Der p extracts also have direct effects on epithelial cells, we hypothesized that allergen augments the effects of Th2 cytokines by promoting mediator release from the bronchial epithelium in allergic asthma. To test our hypothesis, primary bronchial epithelial cultures were grown from bronchial brushings of normal and atopic asthmatic subjects. RT-PCR showed that each culture expressed IL-4R(alpha), common gamma-chain, and IL-13R(alpha)(1), as well as IL-13R(alpha)(2), which negatively regulates IL-13 signaling; FACS analysis confirmed IL-13R(alpha)(2) protein expression. Exposure of epithelial cultures to either Der p extracts, TNF-alpha, IL-4, or IL-13 enhanced GM-CSF and IL-8 release, and this was partially suppressible by corticosteroids. Simultaneous exposure of the epithelial cultures to IL-4 or IL-13 together with Der p resulted in a further increase in cytokine release, which was at least additive. Release of TGF-alpha was also increased by TNF-alpha and combinations of IL-4, IL-13, and Der p; however, this stimulation was only significant in the asthma-derived cultures. These data suggest that, in an allergic environment, Th2 cytokines and allergen have the potential to sustain airway inflammation through a cooperative effect on cytokine release by the bronchial epithelium. Our novel finding that IL-4, IL-13, and allergen enhance release of TGF-alpha, a ligand for the epidermal growth factor receptor that stimulates fibroblast proliferation and goblet cell differentiation, provides a potential link between allergen exposure, Th2 cytokines, and airway remodelling in asthma.
在致敏个体中,接触如屋尘螨(Der p)等过敏原会导致Th2极化并释放包括IL-4和IL-13在内的细胞因子。由于Der p提取物对上皮细胞也有直接作用,我们推测过敏原通过促进过敏性哮喘患者支气管上皮释放介质来增强Th2细胞因子的作用。为了验证我们的假设,我们从正常和特应性哮喘患者的支气管刷检物中培养出原代支气管上皮细胞。逆转录聚合酶链反应(RT-PCR)显示,每种培养物都表达IL-4R(α)、共同γ链、IL-13R(α)(1)以及负调节IL-13信号传导的IL-13R(α)(2);荧光激活细胞分选(FACS)分析证实了IL-13R(α)(2)蛋白的表达。将上皮细胞培养物暴露于Der p提取物、肿瘤坏死因子-α(TNF-α)、IL-4或IL-13中会增强粒细胞-巨噬细胞集落刺激因子(GM-CSF)和IL-8的释放,而皮质类固醇可部分抑制这种释放。将上皮细胞培养物同时暴露于IL-4或IL-13与Der p中会导致细胞因子释放进一步增加,且至少具有相加作用。TNF-α以及IL-4、IL-13和Der p的组合也会增加转化生长因子-α(TGF-α)的释放;然而,这种刺激仅在哮喘来源的培养物中显著。这些数据表明,在过敏环境中,Th2细胞因子和过敏原有可能通过对支气管上皮细胞因子释放的协同作用来维持气道炎症。我们的新发现,即IL-4、IL-13和过敏原会增强TGF-α的释放,TGF-α是一种表皮生长因子受体的配体,可刺激成纤维细胞增殖和杯状细胞分化,这为过敏原暴露、Th2细胞因子与哮喘气道重塑之间提供了潜在联系。
