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Prediction of VH-VL domain orientation for antibody variable domain modeling

机译:预测VH-VL结构域方向以进行抗体可变域建模

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The antigen-binding site of antibodies forms at the interface of their two variable domains, VH and VL, making VH-VL domain orientation a factor that codetermines antibody specificity and affinity. Preserving VH-VL domain orientation in the process of antibody engineering is important in order to retain the original antibody properties, and predicting the correct VH-VL orientation has also been recognized as an important factor in antibody homology modeling. In this article, we present a fast sequence-based predictor that predicts VH-VL domain orientation with Q(2) values ranging from 0.54 to 0.73 on the evaluation set. We describe VH-VL orientation in terms of the six absolute ABangle parameters that have recently been proposed as a means to separate the different degrees of freedom of VH-VL domain orientation. In order to assess the impact of adjusting VH-VL orientation according to our predictions, we use the set of antibody structures of the recently published Antibody Modeling Assessment (AMA) II study. In comparison to the original AMAII homology models, we find an improvement in the accuracy of VH-VL orientation modeling, which also translates into an improvement in the average root-mean-square deviation with regard to the crystal structures. Proteins 2015; 83:681-695. (c) 2015 Wiley Periodicals, Inc.
机译:抗体的抗原结合位点在其两个可变结构域VH和VL的界面处形成,从而使VH-VL结构域定向成为编码抗体特异性和亲和力的因素。为了保留原始抗体特性,在抗体工程化过程中保留VH-VL结构域方向非常重要,并且预测正确的VH-VL方向也已被认为是抗体同源性建模的重要因素。在本文中,我们介绍了一种基于序列的快速预测器,该预测器在评估集上预测QH(2)值在0.54至0.73之间的VH-VL域方向。我们根据六个绝对ABangle参数来描述VH-VL方向,这些参数最近已被提议作为一种手段来分离VH-VL域方向的不同自由度。为了评估根据我们的预测调整VH-VL方向的影响,我们使用了最近发表的《抗体建模评估》(AMA)II研究的一组抗体结构。与原始AMAII同源性模型相比,我们发现VH-VL定向建模的准确性有所提高,这也转化为晶体结构的平均均方根偏差得到了改善。蛋白质2015; 83:681-695。 (c)2015年威利期刊有限公司

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