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小麦麦醇溶蛋白 α- 醇溶蛋白复合体的多样性:一个具有六个重叠表位的 33 肽,在多倍化后进化而来。

Diversification of the celiac disease α-gliadin complex in wheat: a 33-mer peptide with six overlapping epitopes, evolved following polyploidization.

机构信息

Departamento de Mejora Genética, Instituto de Agricultura Sostenible (IAS), Consejo Superior de Investigaciones Científicas (CSIC), Córdoba, E-14080, Spain.

Departamento de Genética, Escuela Superior de Ingenieros Agrónomos y Montes, Universidad de Córdoba, Córdoba, E-14071, Spain.

出版信息

Plant J. 2015 Jun;82(5):794-805. doi: 10.1111/tpj.12851. Epub 2015 May 11.

Abstract

The gluten proteins from wheat, barley and rye are responsible both for celiac disease (CD) and for non-celiac gluten sensitivity, two pathologies affecting up to 6-8% of the human population worldwide. The wheat α-gliadin proteins contain three major CD immunogenic peptides: p31-43, which induces the innate immune response; the 33-mer, formed by six overlapping copies of three highly stimulatory epitopes; and an additional DQ2.5-glia-α3 epitope which partially overlaps with the 33-mer. Next-generation sequencing (NGS) and Sanger sequencing of α-gliadin genes from diploid and polyploid wheat provided six types of α-gliadins (named 1-6) with strong differences in their frequencies in diploid and polyploid wheat, and in the presence and abundance of these CD immunogenic peptides. Immunogenic variants of the p31-43 peptide were found in most of the α-gliadins. Variants of the DQ2.5-glia-α3 epitope were associated with specific types of α-gliadins. Remarkably, only type 1 α-gliadins contained 33-mer epitopes. Moreover, the full immunodominant 33-mer fragment was only present in hexaploid wheat at low abundance, probably as the result of allohexaploidization events from subtype 1.2 α-gliadins found only in Aegilops tauschii, the D-genome donor of hexaploid wheat. Type 3 α-gliadins seem to be the ancestral type as they are found in most of the α-gliadin-expressing Triticeae species. These findings are important for reducing the incidence of CD by the breeding/selection of wheat varieties with low stimulatory capacity of T cells. Moreover, advanced genome-editing techniques (TALENs, CRISPR) will be easier to implement on the small group of α-gliadins containing only immunogenic peptides.

摘要

小麦、大麦和黑麦中的 gluten 蛋白既能引起乳糜泻(celiac disease,CD),也能引起非乳糜泻麸质敏感性(non-celiac gluten sensitivity),这两种疾病影响着全世界高达 6-8%的人口。小麦 α-醇溶蛋白包含三个主要的 CD 免疫原性肽:p31-43,诱导先天免疫反应;33 肽,由六个高度刺激表位的重叠拷贝组成;以及一个额外的与 33 肽部分重叠的 DQ2.5-glia-α3 表位。二倍体和多倍体小麦的 α-醇溶蛋白基因的下一代测序(next-generation sequencing,NGS)和 Sanger 测序提供了六种类型的 α-醇溶蛋白(命名为 1-6),它们在二倍体和多倍体小麦中的频率以及这些 CD 免疫原性肽的存在和丰度方面存在显著差异。p31-43 肽的免疫原性变体在大多数 α-醇溶蛋白中都有发现。DQ2.5-glia-α3 表位的变体与特定类型的 α-醇溶蛋白有关。值得注意的是,只有 1 型 α-醇溶蛋白含有 33 肽表位。此外,完整的免疫显性 33 肽片段仅在六倍体小麦中低丰度存在,可能是由于来自仅在 Aegilops tauschii 中发现的 1.2 型 α-醇溶蛋白的亚类的 allohexaploidization 事件的结果。六倍体小麦的 D 基因组供体。3 型 α-醇溶蛋白似乎是原始类型,因为它们存在于大多数表达 α-醇溶蛋白的小麦属物种中。这些发现对于通过选择或培育低 T 细胞刺激能力的小麦品种来降低 CD 的发病率非常重要。此外,先进的基因组编辑技术(TALENs、CRISPR)将更容易在仅包含免疫原性肽的少数 α-醇溶蛋白上实施。

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