Department of Medicine, University of Wisconsin Madison School of Medicine and Public Health, Madison, WI 53792-9988, USA.
J Allergy Clin Immunol. 2012 Aug;130(2):489-95. doi: 10.1016/j.jaci.2012.05.023. Epub 2012 Jul 4.
Children with allergic asthma have more frequent and severe human rhinovirus (HRV)-induced wheezing and asthma exacerbations through unclear mechanisms.
We sought to determine whether increased high-affinity IgE receptor (FcεRI) expression and cross-linking impairs innate immune responses to HRV, particularly in allergic asthmatic children.
PBMCs were obtained from 44 children, and surface expression of FcεRI on plasmacytoid dendritic cells (pDCs), myeloid dendritic cells, monocytes, and basophils was assessed by using flow cytometry. Cells were also incubated with rabbit anti-human IgE to cross-link FcεRI, followed by stimulation with HRV-16, and IFN-α and IFN-λ1 production was measured by Luminex. The relationships among FcεRI expression and cross-linking, HRV-induced IFN-α and IFN-λ1 production, and childhood allergy and asthma were subsequently analyzed.
FcεRIα expression on pDCs was inversely associated with HRV-induced IFN-α and IFN-λ1 production. Cross-linking FcεRI before HRV stimulation further reduced PBMC IFN-α (47% relative reduction; 95% CI, 32% to 62%; P< .0001) and IFN-λ1 (81% relative reduction; 95% CI, 69% to 93%; P< .0001) secretion. Allergic asthmatic children had higher surface expression of FcεRIα on pDCs and myeloid dendritic cells when compared with that seen in nonallergic nonasthmatic children. Furthermore, after FcεRI cross-linking, allergic asthmatic children had significantly lower HRV-induced IFN responses than allergic nonasthmatic children (IFN-α, P= .004; IFN-λ1, P= .02) and nonallergic nonasthmatic children (IFN-α, P= .002; IFN-λ1, P= .01).
Allergic asthmatic children have impaired innate immune responses to HRV that correlate with increased FcεRI expression on pDCs and are reduced by FcεRI cross-linking. These effects likely increase susceptibility to HRV-induced wheezing and asthma exacerbations.
儿童过敏性哮喘患者因不明机制导致人鼻病毒(HRV)诱发的喘息和哮喘恶化更为频繁和严重。
我们旨在确定高亲和力 IgE 受体(FcεRI)表达和交联增加是否会损害对 HRV 的固有免疫反应,尤其是在过敏性哮喘患儿中。
从 44 名儿童中获得 PBMC,并通过流式细胞术评估浆细胞样树突状细胞(pDC)、髓样树突状细胞、单核细胞和嗜碱性粒细胞上的 FcεRI 表面表达。还将细胞与兔抗人 IgE 孵育以交联 FcεRI,然后用 HRV-16 刺激,并通过 Luminex 测量 IFN-α 和 IFN-λ1 的产生。随后分析 FcεRI 表达和交联、HRV 诱导的 IFN-α 和 IFN-λ1 产生与儿童过敏和哮喘之间的关系。
pDC 上的 FcεRIα 表达与 HRV 诱导的 IFN-α 和 IFN-λ1 产生呈负相关。HRV 刺激前交联 FcεRI 进一步降低 PBMC IFN-α(47%相对减少;95%CI,32%至 62%;P<.0001)和 IFN-λ1(81%相对减少;95%CI,69%至 93%;P<.0001)分泌。与非过敏性非哮喘儿童相比,过敏性哮喘儿童的 pDC 和髓样树突状细胞上的 FcεRIα 表面表达更高。此外,交联 FcεRI 后,过敏性哮喘儿童的 HRV 诱导 IFN 反应明显低于过敏性非哮喘儿童(IFN-α,P=.004;IFN-λ1,P=.02)和非过敏性非哮喘儿童(IFN-α,P=.002;IFN-λ1,P=.01)。
过敏性哮喘儿童对 HRV 的固有免疫反应受损,与 pDC 上 FcεRI 表达增加有关,并通过 FcεRI 交联而减弱。这些影响可能会增加 HRV 诱发喘息和哮喘恶化的易感性。
