Analysis of Safety, Risk Factors and Pretreatment Methods during Rush Hymenoptera Venom Immunotherapy

Górska, Lucyna; Chełmińska, Marta; Krzemieniecki, Krzysztof; Skrzypski, Marcin; Niedoszytko, Marek; Damps-Konstańska, Iwona; Szymanowska, Amelia; Siemińska, Alicja; Wajda, Beata; Drozdowska, Adrianna; Jutel, Marek; Jassem, Ewa

doi:10.1159/000142048

Cited by 28 publications

(13 citation statements)

References 47 publications

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“…VIT SRs occurred during the dose-increase phase at a median dose of 46 µg (range 2-100 µg), which is comparable to the EAACI study where the median dose in the dose-increase phase was 30 µg (range 0.01-150 µg), and the Polish study where the majority of SRs in the dose-increase phase developed at a dose of 40 µg or 60 µg of the venom extract [14,16].…”

Section: Discussionsupporting

confidence: 70%

“…A Polish study observed SRs in 15.2% of patients during the 5-day rush induction phase of VIT, whereas severe adverse events were present in 5.9% patients. The risk factors were bee venom immunotherapy and female sex [16]. In a study in Spain it was concluded that immunotherapy is a safe treatment when EAACI guidelines are strictly followed [17].…”

Section: Discussionmentioning

confidence: 99%

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The local and systemic side-effects of venom and inhaled-allergen subcutaneous immunotherapy

Adamič

Zidarn

Bajrović

et al. 2009

Wien Klin Wochenschr

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Section: Discussionsupporting

confidence: 70%

Section: Discussionmentioning

confidence: 99%

The local and systemic side-effects of venom and inhaled-allergen subcutaneous immunotherapy

Adamič

Zidarn

Bajrović

et al. 2009

Wien Klin Wochenschr

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show abstract

“…Pre-treatment with antihistamines reduces the number and severity of large local reactions and mild systemic reactions such as urticaria and angio-edema. It is advised that antihistamines be administered 1 h before injection until the maintenance dose has been shown to be well tolerated [49]. Antihistamine pretreatment might also increase the efficacy of VIT [50].…”

Section: Safety Of Vitmentioning

confidence: 99%

Venom immunotherapy: clinical efficacy, safety and contraindications

Košnik

Korošec

2015

Expert Review of Clinical Immunology

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Venom-specific immunotherapy (VIT) is considered for the treatment of patients with IgE-mediated systemic allergic reactions (SARs) after developing a Hymenoptera venom allergy. Tolerance is achieved in a majority of patients after only a few days or even hours of rush immunotherapy. After VIT discontinuation, the allergy returns in up to 15% of patients. During VIT, the majority of patients have local reactions at the site of venom injections. SARs to VIT are much more frequent in honeybee-treated patients than in wasp-treated patients. Increased baseline serum tryptase and increased allergen-specific sensitivity of basophils are other factors that might be associated with systemic reactions (SRs) during VIT. Severe SRs occur mainly during the build-up phase but can also occur in the maintenance phase of the VIT, even in patients with a well-tolerated dose-increase phase. Pre-treatment with humanized anti-IgE antibodies (omalizumab) is effective in patients with repeated SARs; however, this use of omalizumab is off-label. In highly exposed patients with a history of very severe reactions, there are virtually no absolute contraindications for VIT.

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“…Forty-two systemic reactions (0.6% of all injections) were documented in 39 patients (3.4%) [57]. On the other side, some studies involving fast venom immunotherapy regimens have found a lower incidence of systemic reaction than with conventional treatments [45], whereas the systemic reaction incidence was higher with other protocols [58].…”

Section: Risk Factors For Severe Adverse Eventsmentioning

confidence: 99%

Incidence and risk factors for subcutaneous immunotherapy anaphylaxis: the optimization of safety

Caminati

Dama

Djuric

et al. 2014

Expert Review of Clinical Immunology

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Fatal reactions related to subcutaneous allergen immunotherapy are rare: one event in 2.5 million injections has been reported in the USA and none in Europe. The prevalence of very severe systemic reactions (systemic adverse events [SAEs]) is one in 1 million injections. Though the serious events rate is decreasing and the majority of SAEs (∼0.2% per injection) are moderate and reversible, they still represent a major concern. Uncontrolled asthma, long-term therapy with β-blockers and high degree of allergen sensitivity are generally considered risk factors. The relevance of other conditions, like previous local reactions, the use of extracts conjugated with adjuvants and accelerated build-up schedules is controversial, as well as the role of preventative strategies. A careful risk assessment of patients and optimal administration procedures may significantly decrease the risk of SAEs. However, more uniform safety data are required and an accurate safety profile should be provided for every allergen product.

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Analysis of Safety, Risk Factors and Pretreatment Methods during Rush Hymenoptera Venom Immunotherapy

Cited by 28 publications

References 47 publications

The local and systemic side-effects of venom and inhaled-allergen subcutaneous immunotherapy

The local and systemic side-effects of venom and inhaled-allergen subcutaneous immunotherapy

Venom immunotherapy: clinical efficacy, safety and contraindications

Incidence and risk factors for subcutaneous immunotherapy anaphylaxis: the optimization of safety

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