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奥马珠单抗可确保系统性肥大细胞增多症患者在蜂毒免疫疗法(VIT)诱导的过敏反应后对VIT的耐受性。

Omalizumab ensures compatibility to bee venom immunotherapy (VIT) after VIT-induced anaphylaxis in a patient with systemic mastocytosis.

作者信息

Gülsen Askin, Ruëff Franziska, Jappe Uta

机构信息

Interdisciplinary Allergy Outpatient Clinic, Department of Pneumology, University of Luebeck.

Department of Dermatology and Allergology, Klinikum der Ludwig-Maximilians-Universität, Munich, and.

出版信息

Allergol Select. 2021 Mar 11;5:128-132. doi: 10.5414/ALX02196E. eCollection 2021.

Abstract

BACKGROUND

Systemic reactions and anaphylaxis due to Hymenoptera venoms occur in up to 7.5% of the European population. Fatal sting reactions are very rare. Serum tryptase levels should be measured in all patients with a history of severe reactions in order to detect mastocytosis and to determine the risk of severe reactions to venom immunotherapy (VIT). The risk to experience severe or even fatal anaphylaxis due to insect stings is quite high in patients with mastocytosis. Therefore, lifelong VIT is recommended in these highly threatened patients. Multicenter studies involving a large population report that up to 20% of patients undergoing VIT have intolerance and systemic reactions to immunotherapy. Some of these side effects occur repeatedly and cannot be managed by standard treatment. A pre-treatment with the anti-IgE antibody omalizumab was useful in many cases. However, omalizumab is not approved for the indication anaphylaxis. Therefore, there is still no defined protocol for omalizumab pre-treatment, and the optimal duration, dosage as well as long-time benefits are still unclear.

CASE REPORT

We present a 60-year-old female patient with mastocytosis who developed a severe anaphylactic reaction during initiation of bee VIT. Serum tryptase was elevated, and a KIT mutation D816V was subsequently confirmed. Component-resolved diagnostic tests revealed specific IgE antibodies to recombinant Api m 1 only. The patient was treated with 150 mg omalizumab, administered subcutaneously 5 weeks, 3 weeks, and 1 week prior to re-start of immunotherapy and for 2 months in parallel to VIT. Updosing was done by a 7-day rush schedule. During this period, no anaphylactic reaction developed, and the bee VIT was well tolerated with up to 200 µg bee venom. The patient is currently in the 3 year of treatment and tolerates the treatment very well.

CONCLUSION

Omalizumab may be used as a premedication in patients with mastocytosis who do not tolerate VIT. Although there is no consensus on the treatment protocol, treatment for 2 - 6 months is considered adequate. The long-term benefits of such treatment require further research.

摘要

背景

膜翅目昆虫毒液引起的全身反应和过敏反应在欧洲人群中的发生率高达7.5%。致命的蜇伤反应非常罕见。对于所有有严重反应病史的患者,均应检测血清类胰蛋白酶水平,以检测肥大细胞增多症并确定毒液免疫疗法(VIT)严重反应的风险。肥大细胞增多症患者因昆虫蜇伤而发生严重甚至致命过敏反应的风险相当高。因此,建议对这些高危患者进行终身VIT治疗。涉及大量人群的多中心研究报告称,接受VIT治疗的患者中,高达20%对免疫疗法不耐受并出现全身反应。其中一些副作用会反复出现,且无法通过标准治疗进行处理。抗IgE抗体奥马珠单抗预处理在许多情况下是有效的。然而,奥马珠单抗未被批准用于过敏反应适应症。因此,目前仍没有明确的奥马珠单抗预处理方案,其最佳持续时间、剂量以及长期益处仍不明确。

病例报告

我们报告一名60岁患有肥大细胞增多症的女性患者,在开始蜜蜂VIT治疗期间发生了严重的过敏反应。血清类胰蛋白酶升高,随后证实存在KIT突变D816V。组分分辨诊断测试仅显示对重组Api m 1有特异性IgE抗体。在重新开始免疫治疗前5周、3周和1周,以及与VIT并行治疗2个月期间,患者接受了150mg奥马珠单抗皮下注射治疗。采用7天快速递增方案进行剂量调整。在此期间,未发生过敏反应,蜜蜂VIT治疗耐受性良好,最高可耐受200μg蜂毒。患者目前处于治疗的第3年,对治疗耐受性良好。

结论

奥马珠单抗可用于不耐受VIT的肥大细胞增多症患者的预处理。尽管治疗方案尚无共识,但2 - 6个月的治疗被认为是足够的。这种治疗的长期益处需要进一步研究。

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