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Randomized Controlled Trial
. 2023 Sep;78(9):2467-2476.
doi: 10.1111/all.15709. Epub 2023 May 11.

Immune response evolution in peanut epicutaneous immunotherapy for peanut-allergic children

Marie Bastin  1 Warner W Carr  2 Carla M Davis  3 David M Fleischer  4 Jay A Lieberman  5 S Shahzad Mustafa  6 Thibault Helleputte  1 Timothée Bois  7 Dianne E Campbell  7 Todd D Green  7   8 Matthew Greenhawt  4
Affiliations
Randomized Controlled Trial

Immune response evolution in peanut epicutaneous immunotherapy for peanut-allergic children

Marie Bastin et al. Allergy. 2023 Sep.

Abstract

Background: Epicutaneous immunotherapy with investigational Viaskin™ Peanut 250 μg (DBV712) has demonstrated statistically superior desensitization versus placebo in peanut-allergic children in clinical trials. It is unclear whether serologic biomarkers predict response.

Methods: Serum-specific IgG4 and IgE (whole peanut and components) from subjects enrolled in the phase 3 Efficacy and Safety of Viaskin Peanut in Children With IgE-Mediated Peanut Allergy study were examined by exploratory univariate and multivariate analyses to determine trajectories and predictors of treatment response, based upon peanut protein eliciting dose (ED) at Month (M) 12 double-blind placebo-controlled food challenge.

Results: Among Viaskin Peanut-treated subjects, peanut sIgG4 significantly increased from baseline through M12 and peanut sIgE peaked at M3 and fell below baseline by M12, with sIgG4 and sIgE peanut components mirroring these trajectories. Placebo subjects had no significant changes. By univariate analysis, M12 peanut sIgG4/sIgE was higher in treatment responders (p < 0.001) and had highest area under the curve (AUC) for predicting ED ≥300 mg and ≥1000 mg (AUC 69.5% and 69.9%, respectively). M12 peanut sIgG4/sIgE >20.1 predicted M12 ED ≥300 mg (80% positive predictive value). The best performing component was Ara h 1 sIgE <15.7 kUA /L (AUC 66.5%). A multivariate model combining Ara h 1 and peanut sIgG4/sIgE had an AUC of 68.2% (ED ≥300 mg) and 67.8% (ED ≥1000 mg).

Conclusions: Peanut sIgG4 rise most clearly differentiated Viaskin Peanut versus placebo subjects. sIgG4/sIgE ratios >20.1 and the combination of Ara h 1 and peanut sIgG4/sIgE had moderate ability to predict treatment response and could potentially be useful for clinical monitoring. Additional data are needed to confirm these relationships.

Keywords: IgE; IgG4; Viaskin Peanut; epicutaneous immunotherapy; peanut allergy.

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References

REFERENCES

    1. Peters R, Koplin J, Ponsonby AL, Perret K, Dharmage SC, Allen K. The natural history of peanut and egg allergy and predictors of persistence: the Healthnuts longitudinal study, 6-year-old follow-up. J Allergy Clin Immunol. 2019;143:AB421.
    1. Gupta RS, Warren CM, Smith BM, et al. The public health impact of parent-reported childhood food allergies in the United States. Pediatrics. 2018;142(6):e20181235.
    1. Sampson HA, Aceves S, Bock SA, et al. Food allergy: a practice parameter update-2014. J Allergy Clin Immunol. 2014;134(5):1016-1025.e43.
    1. Pajno GB, Fernandez-Rivas M, Arasi S, et al. EAACI guidelines on allergen immunotherapy: IgE-mediated food allergy. Allergy. 2018;73(4):799-815.
    1. PALISADE Group of Clinical Investigators, Vickery BP, Vereda A, et al. AR101 oral immunotherapy for peanut allergy. N Engl J Med. 2018;379(21):1991-2001.

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