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披萨饼底模拟胃肠道消化过程中IgE表位和乳糜泻毒性基序的命运

The Fate of IgE Epitopes and Coeliac Toxic Motifs during Simulated Gastrointestinal Digestion of Pizza Base.

作者信息

Daly Matthew E, Wang Kai, Pan Xiaoyan, Depau Rosa L, Marsh Justin, Capozzi Francesco, Johnson Phil, Gethings Lee A, Mills E N Clare

机构信息

Manchester Institute of Biotechnology, School of Biological Sciences, Manchester Academic Health Sciences Centre, The University of Manchester, Princess Street, Manchester M1 7DN, UK.

Department of Food Sciences, University of Bologna, 40126 Bologna, Italy.

出版信息

Foods. 2022 Jul 6;11(14):2000. doi: 10.3390/foods11142000.

Abstract

Understanding how food processing may modify allergen bioaccessibility and the evolution of immunologically active peptides in the gastrointestinal tract is essential if knowledge-based approaches to reducing the allergenicity of food are to be realised. A soy-enriched wheat-based pizza base was subjected to in vitro oral-gastro-duodenal digestion and resulting digests analysed using a combination of sodium dodecyl sulphate-polyacrylamide gel electrophoresis (SDS-PAGE) and mass spectrometry (MS). The digestion profile of pizza base resembled that of bread crust where higher temperatures during baking reduced protein solubility but still resulted in the generation of a complex mixture of peptides. MS profiling showed numerous peptides carrying IgE epitopes, and coeliac toxic motifs were in excess of 20-30 residues long and were only released after either 120 min of gastric digestion or a combination of gastric and duodenal digestion. In silico prediction tools showed an overestimated number of cleavage sites identified experimentally, with low levels of atypical peptic and chymotryptic cleavage sites identified particularly at glutamine residues. These data suggest that such alternative pepsin cleavage sites may play a role in digestion of glutamine-rich cereal foods. They also contribute to efforts to provide benchmarks for mapping in vitro digestion products of novel proteins which form part of the allergenicity risk assessment.

摘要

如果要实现基于知识的降低食物过敏原性的方法,了解食品加工如何改变过敏原的生物可及性以及胃肠道中免疫活性肽的演变至关重要。对一种富含大豆的小麦基披萨饼底进行体外口腔-胃-十二指肠消化,并使用十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)和质谱(MS)相结合的方法对所得消化物进行分析。披萨饼底的消化特征与面包皮相似,烘焙过程中较高的温度降低了蛋白质的溶解度,但仍产生了复杂的肽混合物。质谱分析显示有许多携带IgE表位的肽,乳糜泻毒性基序长度超过20 - 30个残基,仅在胃消化120分钟后或胃和十二指肠消化相结合后才会释放。计算机预测工具显示实验鉴定出的切割位点数量被高估,特别是在谷氨酰胺残基处鉴定出的非典型胃蛋白酶和胰凝乳蛋白酶切割位点水平较低。这些数据表明,此类替代性胃蛋白酶切割位点可能在富含谷氨酰胺的谷物食品消化中起作用。它们也有助于为绘制新型蛋白质的体外消化产物提供基准,而这是过敏原性风险评估的一部分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c5dc/9318710/1cab1682bad2/foods-11-02000-g001.jpg

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