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FPIES患者中髓样细胞反应模式与安全食物预测的关联

Association of myeloid cell reactivity patterns with safe food predictions in FPIES patients.

作者信息

Sanders Georgiana M, Hua Alexandra, Hudson Elizabeth, Troost Jonathan P, Kamada Nobuhiko, Kao John Y, Schuler Charles F, El-Zaatari Mohamad

机构信息

Division of Allergy and Immunology, Department of Internal Medicine, University of Michigan, 24 Frank Lloyd Wright Drive, Ann Arbor, MI, 48105, USA.

Mary H. Weiser Food Allergy Center, University of Michigan, 24 Frank Lloyd Wright Drive, Ann Arbor, MI, 48105, USA.

出版信息

Allergy Asthma Clin Immunol. 2025 May 21;21(1):24. doi: 10.1186/s13223-025-00968-1.

Abstract

BACKGROUND

Food protein-induced enterocolitis syndrome (FPIES) is an understudied non-IgE-mediated food allergy, which is distinct from and lacks diagnostic testing akin to IgE testing. FPIES affects infants and toddlers but can persist into adulthood. As there are no extant methods to identify safe foods for FPIES patients, food ingestion trials are performed at home and often lead to reactions and development of food aversions, which may lead to failure-to-thrive and gastric feeding tube requirements. We hypothesized that foods that fail to elicit responses in immune cells of FPIES patients would be safe to ingest, which could support development of a diagnostic method to headstart safe food identification in patients.

METHODS

We developed an ex vivo model of FPIES using food-stimulated white blood cells (WBCs) from pediatric FPIES patients and controls by defining a 9-gene panel representative of FPIES ex vivo responses and conducted a single-arm pilot clinical trial.

RESULTS

Myeloid cells of FPIES patients displayed variable individual-specific myeloid cell reactivity patterns (iMCRPs) to different foods. Foods that failed to elicit repsonses in patients' immune cells were safe to ingest with a negative predictive value of 98.5%. This, when utilized in prospective predictions, reduced newly introduced food reaction rates from 19.5 to 0% while increasing food repertoire diversity.

CONCLUSIONS

iMCRPs represent a novel and potentially useful tool that associates with safe food ingestion in FPIES patients for foods that fail to elicit immune cell reactions. Trial Registration The trial has been registered at registered at ClinicalTrials.gov # NCT04644783.

摘要

背景

食物蛋白诱导的小肠结肠炎综合征(FPIES)是一种研究不足的非IgE介导的食物过敏,它与IgE检测不同且缺乏类似的诊断测试。FPIES影响婴幼儿,但可能持续到成年期。由于目前尚无确定FPIES患者安全食物的方法,在家中进行食物摄入试验往往会导致反应和食物厌恶的产生,这可能导致发育不良和需要胃饲管。我们假设,在FPIES患者免疫细胞中未能引发反应的食物摄入是安全的,这可能有助于开发一种诊断方法,以便在患者中率先确定安全食物。

方法

我们通过定义一个代表FPIES体外反应的9基因panel,利用儿科FPIES患者和对照的食物刺激白细胞(WBC)建立了FPIES的体外模型,并进行了一项单臂先导临床试验。

结果

FPIES患者的髓样细胞对不同食物表现出可变的个体特异性髓样细胞反应模式(iMCRPs)。在患者免疫细胞中未能引发反应的食物摄入是安全的,阴性预测值为98.5%。当用于前瞻性预测时,这将新引入食物的反应率从19.5%降低到0%,同时增加了食物种类的多样性。

结论

iMCRPs代表了一种新的且可能有用的工具,对于未能引发免疫细胞反应的食物,它与FPIES患者的安全食物摄入相关。试验注册该试验已在ClinicalTrials.gov上注册,注册号为#NCT04644783。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d258/12093898/b5ba3b965aae/13223_2025_968_Fig1_HTML.jpg

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