在对 Timothy 草花粉提取物进行皮下免疫治疗的剂量递增过程中,预处理 IgE 致敏模式决定 IgG4 反应的分子特征。
Pretreatment IgE sensitization patterns determine the molecular profile of the IgG4 response during updosing of subcutaneous immunotherapy with timothy grass pollen extract.
机构信息
Departments of Respiratory Medicine and Allergy, Aarhus University Hospital, Aarhus, Denmark.
Global Research, ALK-Abelló, Hørsholm, Denmark.
出版信息
J Allergy Clin Immunol. 2016 Feb;137(2):562-70. doi: 10.1016/j.jaci.2015.05.023. Epub 2015 Jun 30.
BACKGROUND
Allergen immunotherapy is an effective treatment of allergic rhinoconjunctivitis. Clinical efficacy is associated with improvement of basophil sensitivity and an increase in allergen-specific immunoglobulin concentration.
OBJECTIVE
We sought to determine whether changes in allergen component-specific serum IgE and IgG4 levels during the updosing phase of subcutaneous immunotherapy (SCIT) are biomarkers of the immunologic changes that can lead to treatment efficacy.
METHODS
Twenty-four subjects with grass pollen-induced allergic rhinoconjunctivitis were randomized 3:1 to receive SCIT (Alutard SQ) or to an open control group. IgE and IgG4 concentrations were determined for the major allergens Phl p 1 or Phl p 5 by using ImmunoCAP and for 8 grass pollen molecules by using Immuno Solid-phase Allergy Chip (ISAC) before treatment and after updosing.
RESULTS
Levels of specific IgE against the dominant major allergens Phl p 1 and Phl p 5 increased from a mean of 23.0 to 48.8 kU/L (P = .01, n = 18) during the updosing phase in ImmunoCAP measurements but decreased from a median of 4.6 ISAC specific units (ISU) to 2.14 ISU (P < .0001, n = 102) when measured by using ISAC against 8 grass allergen components. The updosing phase induced a specific IgG4 level increase from a median of 0 ISU before treatment to 0.83 ISU after 12 weeks (P < .0001, n = 102) but only for allergen molecules to which pretreatment-specific IgE antibodies were detected (Spearman σ = 0.72, P < .0001, n = 102).
CONCLUSION
Pretreatment allergen component-specific IgE appears to determine the induction of IgG4 in the updosing phase. Induced IgG4 seems to suppress IgE levels on ISAC, resulting in a marked decrease in ISAC-measured specific IgE levels after updosing of SCIT. Thus this decrease in ISAC IgE levels can be used to monitor the blocking effect of allergen-specific immunotherapy-induced non-IgE antibodies.
背景
变应原免疫疗法是治疗过敏性鼻结膜炎的有效方法。临床疗效与嗜碱性粒细胞敏感性的提高和过敏原特异性免疫球蛋白浓度的增加有关。
目的
我们旨在确定在皮下免疫治疗(SCIT)的加量阶段,变应原成分特异性血清 IgE 和 IgG4 水平的变化是否是导致治疗效果的免疫变化的生物标志物。
方法
24 例花粉致敏的变应性鼻炎结膜炎患者被随机分为 3:1 组接受 SCIT(Alutard SQ)或开放对照组。在治疗前和加量后,使用 ImmunoCAP 测定主要过敏原 Phl p 1 或 Phl p 5 的 IgE 和 IgG4 浓度,并使用 Immuno Solid-phase Allergy Chip(ISAC)测定 8 种花粉分子的浓度。
结果
在 ImmunoCAP 测量中,主要过敏原 Phl p 1 和 Phl p 5 的特异性 IgE 水平从加量阶段的平均 23.0 增加到 48.8 kU/L(P=0.01,n=18),但在使用 ISAC 测量时,从中位数 4.6 ISAC 特异性单位(ISU)降至 2.14 ISU(P<0.0001,n=102)。在 8 种花粉过敏原成分中,加量阶段诱导特异性 IgG4 水平从治疗前的中位数 0 ISU 增加到 12 周后的 0.83 ISU(P<0.0001,n=102),但仅在治疗前检测到特异性 IgE 抗体的过敏原分子中(Spearman σ=0.72,P<0.0001,n=102)。
结论
治疗前的变应原成分特异性 IgE 似乎决定了加量阶段 IgG4 的诱导。诱导的 IgG4 似乎抑制了 ISAC 上的 IgE 水平,导致 SCIT 加量后 ISAC 测定的特异性 IgE 水平显著下降。因此,ISAC IgE 水平的下降可用于监测过敏原特异性免疫治疗诱导的非 IgE 抗体的阻断效应。
Zotero 插件