TY - JOUR
T1 - Probiotic peanut oral immunotherapy versus oral immunotherapy and placebo in children with peanut allergy in Australia (PPOIT-003)
T2 - a multicentre, randomised, phase 2b trial
AU - Loke, Paxton
AU - Orsini, Francesca
AU - Lozinsky, Adriana C.
AU - Gold, Michael
AU - O'Sullivan, Michael D.
AU - Quinn, Patrick
AU - Lloyd, Melanie
AU - Ashley, Sarah E.
AU - Pitkin, Sigrid
AU - Axelrad, Christine
AU - Metcalfe, Jessica R.
AU - Su, Ee Lyn
AU - Tey, Dean
AU - Robinson, Marnie N.
AU - Allen, Katrina J.
AU - Prescott, Susan L.
AU - Dunn Galvin, Audrey
AU - Tang, Mimi L.K.
AU - O'Sullivan, Molly
AU - Fahy-Scheer, Susan
AU - Wallace, Rachael
AU - Baldwin, Samara
AU - Abass, Fuad
AU - Hsiao, Kuang Chih
AU - Ponsonby, Anne Louise
AU - PPOIT-003 study group
N1 - Funding Information:
MDO'S reports having received grants from the Government of Western Australia Department of Health and Channel 7 Telethon Trust and is a director of the Australasian Society of Clinical Immunology and Allergy (ASCIA). PQ reports having received grants from DBV Technologies. KJA is currently a member of the Australian Parliament, but all work for this Article was undertaken before April 12, 2019, by which time she had resigned from all paid and honorary appointments listed. SLP reports having received honoraria from Swisse Biostime and Personal Lifestyle Medicine Institute. ADG reports having received consultant fees from Aimmune Therapeutics, DBV Technologies, and Nestle (research grant and advisory panel). MLKT declares consultant fees from Pfizer and Abbott Nutrition; inventorship on patents covering PPOIT; employee and scientific founder of, and holds share interest and options in, Prota Therapeutics; membership of the Medical Advisory Board of Anaphylaxis & Anaphylaxis Australia and past membership of the Board of Directors of the World Allergy Organization (WAO, ended 2019); membership of expert committees of the American Academy of Allergy Asthma and Immunology, Asia Pacific Association of Allergy Asthma and Clinical Immunology, Australasian Society of Clinical Immunology and Allergy, WHO, and past membership of the International Union of Immunological Societies (ended 2019). All other authors declare no competing interests.
Funding Information:
The PPOIT-003 randomised trial is an investigator-initiated study funded by a National Health and Medical Research Council Australia Project Grant (NHMRC 115423). The Murdoch Children's Research Institute is the sponsor of the study. Additional funding support was provided by Prota Therapeutics. Datapharm Australia (Drommoyne, NSW) prepared the statistical analysis plan with FO, PL, and MLKT and performed the data analysis at the 8-week post-treatment timepoint. The probiotic and placebo treatments were provided by Metagenics Australia as in-kind support. Datapharm Australia performed clinical site monitoring, data management, and statistical analysis. The Murdoch Children's Research Institute is supported by the Victorian Government's Operational Infrastructure Support Programme. We acknowledge the contribution of the study clinical teams and supporting departments from the participating hospitals. We thank the children and caregivers who participated in the PPOIT-003 study.
Publisher Copyright:
© 2022 Elsevier Ltd
PY - 2022/3
Y1 - 2022/3
N2 - Background: Oral immunotherapy is effective at inducing desensitisation to allergens and induces sustained unresponsiveness (ie, clinical remission) in a subset of patients, but causes frequent reactions. We aimed to investigate whether addition of a probiotic adjuvant improved the efficacy or safety of peanut oral immunotherapy. Methods: PPOIT-003, a multicentre, randomised, phase 2b trial, was conducted in three tertiary hospitals in Australia (Adelaide [SA], Melbourne [VIC], and Perth [WA]) in children aged 1–10 years, weighing more than 7 kg, with peanut allergy confirmed by a double-blind placebo-controlled food challenge (cumulative 4950 mg dose of peanut protein) and positive peanut skin prick test (≥3 mm) or peanut-specific IgE (≥0·35 kU/L). Children were randomly assigned (2:2:1) to receive probiotic and peanut oral immunotherapy (PPOIT), placebo probiotic and peanut oral immunotherapy (OIT), or placebo probiotic and placebo OIT (placebo) for 18 months, and were followed up until 12 months after completion of treatment. Oral immunotherapy consisted of increasing doses of peanut protein (commercially available food-grade 12% defatted peanut flour [50% peanut protein]) until a 2000 mg daily maintenance dose was reached. The probiotic adjuvant was a daily dose of 2 × 1010 colony-forming units of the probiotic Lactobacillus rhamnosus ATCC 53103. Placebo immunotherapy comprised maltodextrin, brown food colouring, and peanut essence, and placebo probiotic was maltodextrin. Dual primary outcomes were 8-week sustained unresponsiveness, defined as no reaction to a cumulative dose of 4950 mg peanut protein at treatment completion and 8 weeks after treatment completion, in the PPOIT versus placebo groups and the PPOIT versus OIT groups, analysed by intention to treat. Safety endpoints were adverse events during the treatment phase, and peanut ingestion and reactions in the 12-month post-treatment period. This study is registered with the Australian New Zealand Clinical Trials Registry, 12616000322437. Findings: Between July 4, 2016, and Sept 21, 2020, 201 participants were enrolled and included in the intention-to-treat analysis. 36 (46%) of 79 children in the PPOIT group and 42 (51%) of 83 children in the OIT group achieved sustained unresponsiveness compared with two (5%) of 39 children in the placebo group (risk difference 40·44% [95% CI 27·46 to 53·42] for PPOIT vs placebo, p<0·0001), with no difference between PPOIT and OIT (−5·03% [–20·40 to 10·34], p=0·52). Treatment-related adverse events were reported in 72 (91%) of 79 children in the PPOIT group, 73 (88%) of 83 children in the OIT group, and 28 (72%) of 39 children in the placebo group. Exposure-adjusted incidence of adverse events was 10·58 in the PPOIT group, 11·36 in the OIT, and 2·09 in the placebo group (ratio 0·92 [95% CI 0·85 to 0·99] for PPOIT vs OIT, p=0·042; 4·98 [4·11–6·03] for PPOIT vs placebo, p<0·0001; 5·42 [4·48–6·56] for OIT vs placebo, p<0·0001), with differences seen primarily in gastrointestinal symptoms and in children aged 1–5 years. During the 12-month post-treatment period, 60 (85%) of 71 participants in the PPOIT group, 60 (86%) of 70 participants in the OIT group, and six (18%) of 34 participants in the placebo group were eating peanut; rescue epinephrine use was infrequent (two [3%] of 71 in the PPOIT group, four [6%] of 70 in the OIT group, and none in the placebo group). Interpretation: Both PPOIT and OIT were effective at inducing sustained unresponsiveness. Addition of a probiotic did not improve efficacy of OIT, but might offer a safety benefit compared with OIT alone, particularly in preschool children. Funding: National Health and Medical Research Council Australia and Prota Therapeutics.
AB - Background: Oral immunotherapy is effective at inducing desensitisation to allergens and induces sustained unresponsiveness (ie, clinical remission) in a subset of patients, but causes frequent reactions. We aimed to investigate whether addition of a probiotic adjuvant improved the efficacy or safety of peanut oral immunotherapy. Methods: PPOIT-003, a multicentre, randomised, phase 2b trial, was conducted in three tertiary hospitals in Australia (Adelaide [SA], Melbourne [VIC], and Perth [WA]) in children aged 1–10 years, weighing more than 7 kg, with peanut allergy confirmed by a double-blind placebo-controlled food challenge (cumulative 4950 mg dose of peanut protein) and positive peanut skin prick test (≥3 mm) or peanut-specific IgE (≥0·35 kU/L). Children were randomly assigned (2:2:1) to receive probiotic and peanut oral immunotherapy (PPOIT), placebo probiotic and peanut oral immunotherapy (OIT), or placebo probiotic and placebo OIT (placebo) for 18 months, and were followed up until 12 months after completion of treatment. Oral immunotherapy consisted of increasing doses of peanut protein (commercially available food-grade 12% defatted peanut flour [50% peanut protein]) until a 2000 mg daily maintenance dose was reached. The probiotic adjuvant was a daily dose of 2 × 1010 colony-forming units of the probiotic Lactobacillus rhamnosus ATCC 53103. Placebo immunotherapy comprised maltodextrin, brown food colouring, and peanut essence, and placebo probiotic was maltodextrin. Dual primary outcomes were 8-week sustained unresponsiveness, defined as no reaction to a cumulative dose of 4950 mg peanut protein at treatment completion and 8 weeks after treatment completion, in the PPOIT versus placebo groups and the PPOIT versus OIT groups, analysed by intention to treat. Safety endpoints were adverse events during the treatment phase, and peanut ingestion and reactions in the 12-month post-treatment period. This study is registered with the Australian New Zealand Clinical Trials Registry, 12616000322437. Findings: Between July 4, 2016, and Sept 21, 2020, 201 participants were enrolled and included in the intention-to-treat analysis. 36 (46%) of 79 children in the PPOIT group and 42 (51%) of 83 children in the OIT group achieved sustained unresponsiveness compared with two (5%) of 39 children in the placebo group (risk difference 40·44% [95% CI 27·46 to 53·42] for PPOIT vs placebo, p<0·0001), with no difference between PPOIT and OIT (−5·03% [–20·40 to 10·34], p=0·52). Treatment-related adverse events were reported in 72 (91%) of 79 children in the PPOIT group, 73 (88%) of 83 children in the OIT group, and 28 (72%) of 39 children in the placebo group. Exposure-adjusted incidence of adverse events was 10·58 in the PPOIT group, 11·36 in the OIT, and 2·09 in the placebo group (ratio 0·92 [95% CI 0·85 to 0·99] for PPOIT vs OIT, p=0·042; 4·98 [4·11–6·03] for PPOIT vs placebo, p<0·0001; 5·42 [4·48–6·56] for OIT vs placebo, p<0·0001), with differences seen primarily in gastrointestinal symptoms and in children aged 1–5 years. During the 12-month post-treatment period, 60 (85%) of 71 participants in the PPOIT group, 60 (86%) of 70 participants in the OIT group, and six (18%) of 34 participants in the placebo group were eating peanut; rescue epinephrine use was infrequent (two [3%] of 71 in the PPOIT group, four [6%] of 70 in the OIT group, and none in the placebo group). Interpretation: Both PPOIT and OIT were effective at inducing sustained unresponsiveness. Addition of a probiotic did not improve efficacy of OIT, but might offer a safety benefit compared with OIT alone, particularly in preschool children. Funding: National Health and Medical Research Council Australia and Prota Therapeutics.
UR - http://www.scopus.com/inward/record.url?scp=85124912326&partnerID=8YFLogxK
U2 - 10.1016/S2352-4642(22)00006-2
DO - 10.1016/S2352-4642(22)00006-2
M3 - Article
C2 - 35123664
AN - SCOPUS:85124912326
SN - 2352-4642
VL - 6
SP - 171
EP - 184
JO - The Lancet Child & Adolescent Health
JF - The Lancet Child & Adolescent Health
IS - 3
ER -