Department of Pathophysiology and Allergy Research, Center for Pathophysiology, Infectiology and Immunology, Medical University of Vienna, Vienna, Austria.
Department of Biosciences, University of Salzburg, Salzburg, Austria.
Allergy. 2021 Aug;76(8):2555-2564. doi: 10.1111/all.14817. Epub 2021 May 6.
Evidence has accumulated that birch pollen immunotherapy reduces rhinoconjunctivitis to pollen of birch homologous trees. Therapeutic efficacy has been associated with IgE-blocking IgG antibodies. We have recently shown that sera collected after 16 weeks of sublingual immunotherapy with recombinant Bet v 1 (rBet v 1-SLIT) display strong IgE-blocking bioactivity for Bet v 1. Here, we assessed whether rBet v 1-SLIT-induced IgG antibodies display cross-blocking activity to related allergens in Fagales pollen.
IgE, IgG1 and IgG4 reactivity to recombinant Bet v 1, Aln g 1, Car b 1, Ost c 1, Cor a 1, Fag s 1, Cas s 1 and Que a 1 were assessed in pre- and post-SLIT samples of 17 individuals by ELISA. A basophil inhibition assay using stripped basophils re-sensitized with a serum pool containing high Bet v 1-specific IgE levels was established and used to assess CD63 expression in response to allergens after incubation with pre-SLIT or post-SLIT samples. IgG1 and IgG4 were depleted from post-SLIT samples to assess its contribution to IgE-cross-blocking.
Sublingual immunotherapy with recombinant Bet v 1 boosted cross-reactive IgE antibodies and induced IgG1 and IgG4 antibodies with inter- and intra-individually differing reactivity to the homologs. Highly variable cross-blocking activities of post-SLIT samples to the different allergens were found. IgG1 and IgG4 antibodies displayed cross-blocking activity with individual variance.
Our mechanistic approach suggested that immunotherapy with the reference allergen Bet v 1 induces individual repertoires of cross-reactive IgG1 and IgG4 antibodies. The cross-blocking bioactivity of these antibodies was also highly variable and neither predictable from protein homology nor IgE-cross-reactivity.
有证据表明桦树花粉免疫疗法可减少花粉致敏同源树木的鼻结膜炎。治疗效果与 IgE 阻断 IgG 抗体有关。我们最近表明,在舌下免疫疗法 16 周后收集的血清中,重组 Bet v 1(rBet v 1-SLIT)显示出对 Bet v 1 具有强烈的 IgE 阻断生物活性。在此,我们评估了 rBet v 1-SLIT 诱导的 IgG 抗体是否对山毛榉花粉中的相关过敏原具有交叉阻断活性。
通过 ELISA 评估 17 名个体的 SLIT 前和 SLIT 后血清样本对重组 Bet v 1、Aln g 1、Car b 1、Ost c 1、Cor a 1、Fag s 1、Cas s 1 和 Que a 1 的 IgE、IgG1 和 IgG4 反应性。建立了使用富含高特异性 IgE 水平的血清池重新敏化的脱颗粒嗜碱性粒细胞的嗜碱性粒细胞抑制测定法,并用于评估与过敏原孵育后响应物的 CD63 表达。从 SLIT 后样本中耗尽 IgG1 和 IgG4,以评估其对 IgE 交叉阻断的贡献。
重组 Bet v 1 的舌下免疫疗法增强了交叉反应性 IgE 抗体,并诱导了 IgG1 和 IgG4 抗体,其对同源物的反应性具有个体间和个体内的差异。发现 SLIT 后样本对不同过敏原的交叉阻断活性具有高度可变性。IgG1 和 IgG4 抗体显示出个体差异的交叉阻断活性。
我们的机制方法表明,参考过敏原 Bet v 1 的免疫疗法诱导了交叉反应性 IgG1 和 IgG4 抗体的个体库。这些抗体的交叉阻断生物活性也具有高度可变性,既不能从蛋白质同源性预测,也不能从 IgE 交叉反应性预测。
