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限制构象肽表位景观。

Circumscribing the conformational peptide epitope landscape.

机构信息

Department of Biochemistry and Molecular Biology, University of Bari, Via Orabona 4, 70126 Bari, Italy.

出版信息

Curr Pharm Des. 2012;18(6):832-9. doi: 10.2174/138161212799277635.

Abstract

The development of vaccines for new and re-emerging pathologies and infections is based on the ability to define immunogenic epitopes. An immunogenic B-cell peptide epitope is a specific restricted antigen region that is capable of eliciting a humoral immune response and of combining with a specific site on antibodies. Using a number of experimental models and based on data from several literature reports, we identified low levels of sequence similarity to the host proteome as one of the main factors modulating the B-cell epitope repertoire in the humoral immune response. In point of fact, a low level of sequence identity to the host proteins is a common denominator unifying the composite, disparate assembly of linear peptide B-cell epitopes that has been experimentally validated and described in the literature. Here, we explore the proteomic similarity of conformational epitopes experimentally validated and described in published reports. Again, discontinuous epitopic structures formed by non-contiguous amino acid residues were found to define peptide sequences with a low level of similarity to the host. The present meta-analysis adds further significance to the immunological low-similarity theory and its clinical implications. Potentially, low-similarity peptide epitopes pave the way for novel effective vaccines in cancer, autoimmunity, and infectious diseases.

摘要

新型和再现病原体和传染病疫苗的开发基于定义免疫原性表位的能力。免疫原性 B 细胞肽表位是一种特定的受限抗原区域,能够引发体液免疫反应,并与抗体上的特定部位结合。使用多种实验模型,并基于来自几份文献报告的数据,我们确定与宿主蛋白质组的序列相似性低是调节体液免疫反应中 B 细胞表位库的主要因素之一。事实上,与宿主蛋白的低序列同一性是统一组合的共同特征,将线性肽 B 细胞表位离散组装,这些表位已经在实验中得到验证并在文献中描述。在这里,我们探讨了实验验证和文献描述的构象表位的蛋白质组相似性。同样,由非连续氨基酸残基形成的不连续表位结构被发现定义了与宿主相似性低的肽序列。目前的荟萃分析为免疫低相似性理论及其临床意义增添了更多意义。潜在地,低相似性肽表位为癌症、自身免疫和传染病中的新型有效疫苗铺平了道路。

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