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乳糜泻免疫优势表位的排序:新型食品蛋白安全性评估可靠参数的鉴定。

Ranking of immunodominant epitopes in celiac disease: Identification of reliable parameters for the safety assessment of innovative food proteins.

机构信息

European Food Safety Authority (EFSA), via Carlo Magno 1A, 43021, Parma, Italy.

Instituto de Investigación en Ciencias de la Alimentación, CIAL (CSIC-UAM), C/Nicolás Cabrera, 9, Campus de la Universidad Autónoma de Madrid, 28049, Madrid, Spain.

出版信息

Food Chem Toxicol. 2021 Nov;157:112584. doi: 10.1016/j.fct.2021.112584. Epub 2021 Sep 25.

DOI:10.1016/j.fct.2021.112584
PMID:34582965
Abstract

A ranking of gluten T-cell epitopes triggering celiac disease (CD) for its potential application in the safety assessment of innovative food proteins is developed. This ranking takes into account clinical relevance and information derived from key steps involved in the CD pathogenic pathway: enzymatic digestion, epitope binding to HLA-DQ receptors of the antigen-presenting cells and activation of pro-inflammatory CD4 T-cells, which recognizes the HLA-DQ-epitope complex and initiates the inflammatory response. In silico chymotrypsin digestion was the most discriminatory tool for the ranking of gluten T-cell epitopes among all digestive enzymes studied, classifying 81% and 60% of epitopes binding HLA-DQ2.5 and HLA-DQ8 molecules, respectively, with a high risk. A positive relationship between the number of prolines and the risk of gluten T-cell epitopes was identified. HLA-binding data analysis revealed the additional role played by the flanking regions of the 9-mer epitopes whereas the integration of T-cell activation data into the ranking strategy was incomplete because it was difficult to combine results from different studies. The overall ranking proposed in decreasing order of immunological relevance was: α-gliadins > ω-gliadins > hordeins > γ-gliadins ∼ avenins ∼ secalins > glutenins. This novel approach can be considered as a first step to reshape the risk assessment strategy of innovative proteins and their potential to trigger CD.

摘要

开发了一种用于评估新型食品蛋白安全性的基于谷蛋白 T 细胞表位的乳糜泻(CD)风险排序方法。该排序方法考虑了临床相关性和源自 CD 发病途径关键步骤的信息:酶消化、抗原呈递细胞中 HLA-DQ 受体与表位结合以及促炎 CD4 T 细胞的激活,该细胞识别 HLA-DQ-表位复合物并引发炎症反应。在所有研究的消化酶中,糜蛋白酶消化是对谷蛋白 T 细胞表位进行排序的最具区分力的工具,可将分别与 HLA-DQ2.5 和 HLA-DQ8 分子结合的 81%和 60%的表位分类为高风险,这表明脯氨酸数量与谷蛋白 T 细胞表位的风险之间存在正相关关系。HLA 结合数据分析揭示了侧翼区域在 9 -mer 表位中的额外作用,而将 T 细胞激活数据纳入排序策略的工作并不完整,因为难以结合来自不同研究的结果。按照免疫相关性降序排列的总体排序为:α-麦醇溶蛋白>ω-麦醇溶蛋白>大麦醇溶蛋白>γ-麦醇溶蛋白~燕麦醇溶蛋白~醇溶谷蛋白>麦谷蛋白。这种新方法可以被视为重塑新型蛋白风险评估策略及其引发 CD 潜力的第一步。

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