ADP101 multifood oral immunotherapy for food-allergic patients: Harmony phase 1/2 randomized clinical trial

The journal of allergy and clinical immunology. Global Pub Date : 2025-02-01 Epub Date: 2024-12-10 DOI:10.1016/j.jacig.2024.100382

Edwin H. Kim MD, MS , Warner W. Carr MD , Amal H. Assa’ad MD , Shaila U. Gogate MD , Daniel H. Petroni MD, PhD , Thomas B. Casale MD , Mei-Lun Wang MD , Amy Sullivan BA , Amy M. Archer MD, PhD , Ouhong Wang PhD , Cheri Piscia-Nichols BS , Lisa Tuomi PharmD , Olga Levin-Young MBA , Ashley Dombkowski PhD , Dana McClintock MD , Harmony investigators

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Abstract

Background

Oral immunotherapy is an established approach to desensitize the immune system in the context of allergic disease; however, the only currently approved product is for peanut allergy. ADP101 is a novel, pharmaceutical-grade, multifood oral immunotherapy in development to simultaneously treat single or multiple food allergies, containing allergenic proteins from 15 foods in equal parts by protein weight.

Objective

The phase 1/2 Harmony trial (NCT04856865) evaluated efficacy and safety of ADP101 in participants with qualifying allergy to 1 to 5 foods in ADP101, defined as dose-limiting symptoms with a ≤100 mg challenge dose during double-blind, placebo-controlled food challenge (DBPCFC).

Methods

Participants were randomized to low-dose (1500 mg/d; 100 mg protein per food) or high-dose (4500 mg/d; 300 mg protein per food) ADP101, or matched placebo, with dose escalation followed by daily maintenance dosing over 40 weeks. The primary endpoint was the proportion of participants tolerating a ≥600 mg challenge dose of a single qualifying food without dose-limiting symptoms at the Week 40 Exit DBPCFC (ie, responders).

Results

In the primary analysis population (61 pediatric participants aged 4-17 years), a greater response rate was observed in both the high-dose ADP101 (55.0%) and low-dose ADP101 (38.1%) groups compared with pooled placebo (20.0%) (nominal P = .048, P = .306, respectively; adjusted for multiple comparisons, P = .097, P = .306, respectively). Desensitization to ≥2 foods was observed in individuals with multiple food allergies, as was desensitization at levels over 600 mg. ADP101-treated participants showed an overall reduction in skin-prick test reactivity, with an increase in maximum tolerated dose across the majority of foods tested. Adverse events were mostly mild or moderate, with no life-threatening events or deaths.

Conclusions

The study did not meet its primary endpoint, but ADP101 demonstrated a favorable safety profile and increased the reactive threshold in DBPCFC in pediatric participants with single or multiple food allergies across multiple endpoints, warranting further clinical investigation.

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ADP101多食口服免疫疗法治疗食物过敏患者：Harmony 1/2期随机临床试验

背景：口服免疫治疗是一种成熟的方法来脱敏免疫系统在过敏性疾病的背景下；然而，目前唯一批准的产品是针对花生过敏的。ADP101是一种新型的药物级多食物口服免疫疗法，可同时治疗单一或多种食物过敏，含有15种食物的致敏蛋白，按蛋白质重量计算为等量。目的：1/2期Harmony试验（NCT04856865）评估ADP101对符合条件的ADP101中1至5种食物过敏的参与者的疗效和安全性，定义为双盲安慰剂对照食物刺激（DBPCFC）期间≤100mg刺激剂量的剂量限制性症状。方法：参与者随机接受低剂量组(1500mg /d；每份食物100毫克蛋白质)或高剂量(4500毫克/天；ADP101或匹配的安慰剂，剂量递增，随后每日维持剂量，持续40周。主要终点是在第40周退出DBPCFC时耐受≥600mg单一合格食物的攻击剂量而无剂量限制性症状的参与者的比例（即应答者）。结果：在主要分析人群（61名4-17岁的儿童参与者）中，高剂量ADP101组（55.0%）和低剂量ADP101组（38.1%）的缓解率均高于联合安慰剂组（20.0%）(名义P = 0.048, P = 0.306；经多重比较调整，P = 0.097, P = 0.306)。在多种食物过敏的个体中观察到对≥2种食物的脱敏，在超过600毫克的水平下也会脱敏。接受adp101治疗的参与者在皮肤点刺试验中的反应性总体上有所降低，在大多数被测试的食物中，最大耐受剂量都有所增加。不良事件大多为轻度或中度，没有危及生命的事件或死亡。结论：该研究没有达到其主要终点，但ADP101显示出良好的安全性，并且在多个终点中增加了单一或多种食物过敏的儿童受试者的DBPCFC反应阈值，值得进一步的临床研究。

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