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首页> 外文期刊>Clinical & developmental immunology. >Model for Vaccine Design by Prediction of B-Epitopes of IEDB Given Perturbations in Peptide Sequence, In Vivo Process, Experimental Techniques, and Source or Host Organisms
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Model for Vaccine Design by Prediction of B-Epitopes of IEDB Given Perturbations in Peptide Sequence, In Vivo Process, Experimental Techniques, and Source or Host Organisms

机译:通过预测肽序列的IEDB扰动的B-epitupation,体内工艺,实验技术和源儿或宿主生物体通过预测IEDB扰动的模型

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Perturbation methods add variation terms to a known experimental solution of one problem to approach a solution for a related problem without known exact solution. One problem of this type in immunology is the prediction of the possible action of epitope of one peptide after a perturbation or variation in the structure of a known peptide and/or other boundary conditions (host organism, biological process, and experimental assay). However, to the best of our knowledge, there are no reports of general-purpose perturbation models to solve this problem. In a recent work, we introduced a new quantitative structure-property relationship theory for the study of perturbations in complex biomolecular systems. In this work, we developed the first model able to classify more than 200,000 cases of perturbations with accuracy, sensitivity, and specificity >90% both in training and validation series. The perturbations include structural changes in >50000 peptides determined in experimental assays with boundary conditions involving >500 source organisms, >50 host organisms, >10 biological process, and >30 experimental techniques. The model may be useful for the prediction of new epitopes or the optimization of known peptides towards computational vaccine design.
机译:扰动方法将变化术语添加到一个问题的已知实验解决方案中,以在没有已知精确解决方案的情况下接近相关问题的解决方案。免疫学中这种类型的一个问题是在已知肽和/或其他边界条件(宿主生物,生物学过程和实验测定)的结构中扰动或变化后,预测一种肽的表位的可能作用。然而,据我们所知,没有关于通用扰动模型的报道来解决这个问题。在最近的一项工作中,我们向复杂生物分子系统扰动研究了一种新的定量结构 - 性质关系理论。在这项工作中,我们开发了第一个能够在训练和验证系列中以准确性,敏感性和特异性进行分类为200,000多个扰动案例的模型。扰动包括在实验测定中测定的具有涉及> 500个源生物,> 50次宿主生物,> 10生物过程的实验测定中的结构变化,> 10个实验技术。该模型可用于预测新表位或已知肽朝向计算疫苗设计的优化。

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