慢性自发性荨麻疹患者的发病率,这些患者在六年后仍无法停用奥马珠单抗。

IF 3.3 Q2 ALLERGY
Frontiers in allergy Pub Date : 2024-10-02 eCollection Date: 2024-01-01 DOI:10.3389/falgy.2024.1464466
V Schichter-Konfino, R Mubariki, E Toubi, Z Vadasz
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引用次数: 0

摘要

背景:奥马珠单抗(Omalizumab,OMA)是美国食品及药物管理局(FDA)批准的第一种治疗严重慢性自发性荨麻疹(CSU)的生物药物,也是迄今为止唯一有效且真正安全的药物。我们的目标是评估长期无法停用 OMA 的 CSU 患者的患病率。我们还询问生物标志物(如抗TPO 抗体和总 IgE)是否有助于预测这一问题:我们对 93 名患者进行了前瞻性登记,其中包括 CSU 病程、开始接受 OMA 治疗的时间、随访期间的荨麻疹活动评分 (UAS7)、合并疾病、血清 IgE 水平以及是否存在抗TPO 抗体。最后,我们还评估了六年来对 OMA 的反应:在接受治疗的 93 名 CSU 患者中,有 10 名患者在 6 个月后停用了 OMA,被定义为治疗失败。另有 10 名患者在治疗 2-4 年后,病情得到缓解,停止了 OMA 的治疗。73名患者仍在接受2至6年的治疗,他们的反应程度各不相同。其中,有 38 名患者(52%)由于 CSU 复发,即使在 6 年后我们也无法停止 OMA 的治疗。在无法停用 OMA 的 CSU 患者中,血清 IgE 水平降低和抗TPO 抗体阳性的发生率明显更高:这是首次对接受过 OMA 治疗的 CSU 患者进行长达六年的随访研究。结论:这是第一项对接受过 OMA 治疗的 CSU 患者进行长达六年随访的研究,其中半数患者仍需接受六年的长期治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The prevalence of patients suffering from chronic spontaneous urticaria, in whom omalizumab cannot be stopped even after six years.

Background: Omalizumab (OMA) was the first FDA-approved biological drug for severe chronic spontaneous urticaria (CSU), and until today is the only beneficial and truly safe one. The objectives were: To assess the prevalence of CSU patients in whom OMA cannot be stopped over time. We also asked if biomarkers (e.g., anti-TPO antibodies and total IgE) could assist in anticipating this issue.

Methods: We used our prospective registry of 93 patients, which included CSU disease duration, the onset of OMA treatment, Urticaria Activity Score (UAS7) during follow-up, co-morbidities, serum IgE levels and the presence of anti-TPO antibodies. Finally, we assessed the response to OMA during a period of six years.

Results: Out of the 93 treated CSU patients, OMA was stopped in ten patients after six months being defined as failures. In another ten patients, OMA was discontinued after 2-4 years of therapy, achieving a remission. Seventy-three patients are still treated between 2 and 6 years, having different degrees of response. Of these, in thirty-eight (52%) patients, we could not stop OMA even after six years due to CSU relapses. The prevalence of lower serum IgE levels and anti-TPO antibody positivity was significantly higher in CSU patients in whom OMA could not be stopped.

Conclusion: This is the first study where OMA-treated CSU patients were followed up to six years. In half of them, long-term therapy of six years is still required.

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CiteScore
2.80
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