Dose and route of administration determine the efficacy of prophylactic immunotherapy for peanut allergy in a Brown Norway rat model

Tiffany Kirkaldy Spaanager Sztuk; Neil Marcus Rigby; Lasse Nørskov-Nielsen; Stef J Koppelman; Ana Isabel Sancho; Niels-Peter Hell Knudsen; Justin Marsh; Philip Johnson; Shashank Gupta; Alan Robert Mackie; Jeppe Madura Larsen; Katrine Lindholm Bøgh

doi:10.3389/fimmu.2023.1121497

Dose and route of administration determine the efficacy of prophylactic immunotherapy for peanut allergy in a Brown Norway rat model

Front Immunol. 2023 Feb 23:14:1121497. doi: 10.3389/fimmu.2023.1121497. eCollection 2023.

Affiliations

¹ National Food Institute, Technical University of Denmark, Kgs. Lyngby, Denmark.
² School of Food Science & Nutrition, University of Leeds, Leeds, United Kingdom.
³ Institute of Agriculture and Natural Resources, Food Science and Technology, University of Nebraska-Lincoln, Lincoln, NE, United States.
⁴ Immunology, ALK, Hørsholm, Denmark.

Abstract

Introduction: Allergen-specific immunotherapy (IT) is emerging as a viable option for treatment of peanut allergy. Yet, prophylactic IT remains unexplored despite early introduction of peanut in infancy was shown to prevent allergy. There is a need to understand how allergens interact with the immune system depending on the route of administration, and how different dosages of allergen may protect from sensitisation and a clinical active allergy. Here we compared peanut allergen delivery via the oral, sublingual (SL), intragastric (IG) and subcutaneous (SC) routes for the prevention of peanut allergy in Brown Norway (BN) rats.

Methods: BN rats were administered PBS or three different doses of peanut protein extract (PPE) via either oral IT (OIT), SLIT, IGIT or SCIT followed by intraperitoneal (IP) injections of PPE to assess the protection from peanut sensitisation. The development of IgE and IgG1 responses to PPE and the major peanut allergens were evaluated by ELISAs. The clinical response to PPE was assessed by an ear swelling test (EST) and proliferation was assessed by stimulating splenocytes with PPE.

Results: Low and medium dose OIT (1 and 10 mg) and all doses of SCIT (1, 10, 100 µg) induced sensitisation to PPE, whereas high dose OIT (100 mg), SLIT (10, 100 or 1000 µg) or IGIT (1, 10 and 100 mg) did not. High dose OIT and SLIT as well as high and medium dose IGIT prevented sensitisation from the following IP injections of PPE and suppressed PPE-specific IgE levels in a dose-dependent manner. Hence, administration of peanut protein via different routes confers different risks for sensitisation and protection from peanut allergy development. Overall, the IgE levels toward the individual major peanut allergens followed the PPE-specific IgE levels.

Discussion: Collectively, this study showed that the preventive effect of allergen-specific IT is determined by the interplay between the specific site of PPE delivery for presentation to the immune system, and the allergen quantity, and that targeting and modulating tolerance mechanisms at specific mucosal sites may be a prophylactic strategy for prevention of peanut allergy.

Keywords: IgE; animal model; food allergy; gastric immunotherapy; oral immunotherapy; peanut allergy; subcutaneous immunotherapy; sublingual immunotherapy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Administration, Oral
Allergens
Animals
Arachis
Desensitization, Immunologic
Immunoglobulin E
Peanut Hypersensitivity*
Rats
Rats, Inbred BN

Substances

Allergens
Immunoglobulin E

Grants and funding

The presented work was supported by Innovation Fund Denmark as part of the ALLEVIATE project with grant number 6159-00005B. Size exclusion chromatography (SEC) data was generated through accessing research infrastructure at National Food Institute, Technical University of Denmark funded by FOODHAY (Food and Health Open Innovation Laboratory, Danish Roadmap for Research Infrastructure).