对奥马珠单抗有反应和无反应的严重慢性自发性荨麻疹:已知和新型体外变量的预后价值分析。

R Asero, P Calzari, S Ferrucci, M Lorini, V Carbonelli, S Stella, D Consonni, M Cugno
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引用次数: 0

摘要

摘要:背景。慢性自发性荨麻疹(CSU)对抗 IgE 治疗的反应可能很快,也可能很晚或没有反应。最近,有人描述了替代 FceRI 的肥大细胞活化潜在机制,包括 Mas 相关 G 蛋白偶联受体 X2(MRGPRX2)、凝血级联激活和嗜酸性粒细胞激活。我们测量了对奥马珠单抗有反应和无反应的 CSU 患者血清中的几种潜在体外标记物,包括众所周知的 MRGPRX2 激活剂。方法在基线和开始使用奥马珠单抗治疗一周后,对 32 名严重 CSU 患者和 20 名健康对照者的 D-二聚体、P 物质 (SP)、嗜酸性粒细胞阳离子蛋白 (ECP)、可溶性 MRGPRX2、抗 FceRI 的 IgE、抗 FceRII 的 IgE、抗 FceRI 的 IgG 和抗 FceRII 的 IgG 进行了测定。结果显示基线时,CSU 患者的 D-二聚体、IgE 抗 FceRI、IgG 抗 FceRI 和 ECP 水平明显高于对照组(所有病例的 p 均小于 0.001),可溶性 MRGPRX2 水平明显低于对照组(p = 0.009)。两组患者对 FceRII 和 SP 的 IgG 和 IgE 水平相似。首次使用奥马珠单抗一周后,早期应答者的抗 FceRI IgE(p < 0.001)和 D-二聚体(p = 0.028)水平明显下降。无论对奥马珠单抗的最终反应如何,所有 CSU 患者的 SP 均有所增加(p < 0.001)。一周时的 IgE 抗 FceRI 反应与奥马珠单抗的最终反应相关(OR:0.12 [95%CI 0.01-1.06])。结论严重的CSU与高水平的血浆生物标志物(包括D-二聚体、IgE抗FceRI、IgG抗FceRI和ECP)和低水平的可溶性MRGPRX2有关。一周后的 IgE 抗 FceRI 反应可预测对奥马珠单抗的最终反应。
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Severe chronic spontaneous urticaria responding and not responding to omalizumab: analysis of the prognostic value of known and novel in-vitro variables.

Summary: Background. Chronic spontaneous urticaria (CSU) response to anti-IgE treatment can be rapid, late or absent. Recently, potential mechanisms of activation of mast cells alternative to FceRI, including mas-related G protein-coupled receptor X2 (MRGPRX2), activation of coagulation cascade, and activation of eosinophils have been described. We measured several potential in-vitro markers, including well-known MRGPRX2 activators, in sera of patients CSU both responding and not responding to omalizumab. Methods. D-dimer, substance P (SP), eosinophil cationic protein (ECP), soluble MRGPRX2, IgE anti-FceRI, IgE anti-FceRII, IgG anti-FceRI and IgG anti-FceRII were measured in 32 patients with severe CSU at baseline and one week after the start of omalizumab therapy, and in 20 healthy controls. Results. At baseline CSU patients showed significantly higher levels of D-dimer, IgE anti-FceRI, IgG anti-FceRI, and ECP (p < 0.001 in all cases), and significantly lower levels of soluble MRGPRX2 (p = 0.009) than controls. The two groups showed similar levels of IgG and IgE to FceRII and SP. One week after the first omalizumab administration there was a significant drop of IgE anti-FceRI (p < 0.001) and D-dimer (p = 0.028), in early responders. SP increased in all CSU patients (p < 0.001) irrespective of the final response to omalizumab. IgE anti-FceRI response at one week was associated with the final response to omalizumab (OR:0.12 [95%CI 0.01-1.06]). Conclusions. Severe CSU is associated with high plasma levels of several biomarkers including D-dimer, IgE anti-FceRI, IgG anti-FceRI and ECP and low levels of soluble MRGPRX2. IgE anti-FceRI response at one week may predict the final response to omalizumab.

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