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Assessment of fully automated antibody homology modeling protocols in molecular operating environment

机译:在分子操作环境中评估全自动抗体同源性建模方案

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摘要

The success of antibody-based drugs has led to an increased demand for predictive computational tools to assist antibody engineering efforts surrounding the six hypervariable loop regions making up the antigen binding site. Accurate computational modeling of isolated protein loop regions can be quite difficu consequently, modeling an antigen binding site that includes six loops is particularly challenging. In this work, we present a method for automatic modeling of the FV region of an immunoglobulin based upon the use of a precompiled antibody x-ray structure database, which serves as a source of framework and hypervariable region structural templates that are grafted together. We applied this method (on common desktop hardware) to the Second Antibody Modeling Assessment (AMA-II) target structures as well as an experimental specialized CDR-H3 loop modeling method. The results of the computational structure predictions will be presented and discussed.
机译:基于抗体的药物的成功导致对预测计算工具的需求增加,以辅助围绕构成抗原结合位点的六个高变环区域的抗体工程工作。对分离的蛋白质环区域进行精确的计算建模可能非常困难。因此,对包括六个环的抗原结合位点进行建模特别具有挑战性。在这项工作中,我们提出了一种基于使用预编译的抗体X射线结构数据库自动建模免疫球蛋白FV区域的方法,该数据库用作框架和嫁接在一起的高变区结构模板的来源。我们将此方法(在常见的台式机硬件上)应用于第二抗体建模评估(AMA-II)目标结构以及实验性的专用CDR-H3环路建模方法。将介绍和讨论计算结构预测的结果。

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