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Template-based scoring functions for visualizing biological insights of H-2Kb-peptide-TCR complexes

机译:基于模板的评分功能,用于可视化H-2K b -肽-TCR复合物的生物学见解

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Class-I major histocompatibility complex (MHC), peptide, and T-cell receptor (TCR) play an essential role of adaptive immune responses. Many prediction servers are available for identification of peptides that bind to MHC class I molecules. These servers are often lack of detailed interacting residues and binding models for analyzing MHC-peptide-TCR interaction mechanisms. This study numerously enhanced the template-based scoring function derived from protein-protein interactions for identifying MHC-peptide-TCR binding models. The scoring function considers both the template similarity and interacting force to ensure the statistically significant interface similarity between the peptide candidates and structure templates. The result shows that our scoring function is comparative to the public websites for identifying MHC binding peptides. Our model, considering both the MHC-peptide and peptide-TCR interfaces, is able to provide visualization and the biological insights of MHC-peptide-TCR binding models. We believe that our model is useful for the development of peptide-based vaccines.
机译:I类主要组织相容性复合物(MHC),肽和T细胞受体(TCR)发挥了适应性免疫反应的重要作用。许多预测服务器可用于鉴定与I类MHC分子结合的肽。这些服务器通常缺乏详细的相互作用残基和用于分析MHC-肽-TCR相互作用机制的结合模型。这项研究大量增强了基于模板的评分功能,该功能源自蛋白质-蛋白质相互作用,用于鉴定MHC-肽-TCR结合模型。评分功能同时考虑了模板相似性和相互作用力,以确保候选肽和结构模板之间的统计学上显着的界面相似性。结果表明,我们的评分功能与鉴定MHC结合肽的公共网站相比具有可比性。我们的模型同时考虑了MHC-肽和肽-TCR界面,能够提供MHC-肽-TCR结合模型的可视化和生物学见解。我们认为,我们的模型可用于开发基于肽的疫苗。

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