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Disjoint combinations profiling (DCP): a new method for the prediction of antibody CDR conformation from sequence

机译:脱节组合图谱(DCP):一种从序列预测抗体CDR构象的新方法

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摘要

The accurate prediction of the conformation of Complementarity-Determining Regions (CDRs) is important in modelling antibodies for protein engineering applications. Specifically, the Canonical paradigm has proved successful in predicting the CDR conformation in antibody variable regions. It relies on canonical templates which detail allowed residues at key positions in the variable region framework or in the CDR itself for 5 of the 6 CDRs. While no templates have as yet been defined for the hypervariable CDR-H3, instead, reliable sequence rules have been devised for predicting the base of the CDR-H3 loop. Here a new method termed Disjoint Combinations Profiling (DCP) is presented, which contributes a considerable advance in the prediction of CDR conformations. This novel method is explained and compared with canonical templates and sequence rules in a 3-way blind prediction. DCP achieved 93 accuracy over 951 blind predictions and showed an improvement in cumulative accuracy compared to predictions with canonical templates or sequence rules. In addition to its overall improvement in prediction accuracy, it is suggested that DCP is open to better implementations in the future and that it can improve as more antibody structures are deposited in the databank. In contrast, it is argued that canonical templates and sequence rules may have reached their peak.
机译:互补决定区(CDR)构象的准确预测对于蛋白质工程应用的抗体建模非常重要。具体而言,规范范式已被证明可成功预测抗体可变区的CDR构象。它依赖于规范模板,该模板详细描述了6个CDR中的5个CDR可变区框架或CDR本身中关键位置的允许残基。尽管尚未为高变CDR-H3定义任何模板,但已设计出可靠的序列规则来预测CDR-H3环的碱基。在这里,提出了一种称为脱节组合分析(DCP)的新方法,该方法在CDR构象的预测中做出了巨大贡献。解释了这种新颖的方法,并将其与规范模板和序列规则进行了三向盲预测。 DCP在951个盲预测中达到了93个准确度,并且与使用标准模板或序列规则的预测相比,累积准确度有所提高。除了在预测准确性方面的整体改进外,还建议DCP在将来可以更好地实施,并且随着数据库中沉积更多抗体结构而可以改善。相反,有人认为规范模板和序列规则可能已达到顶峰。

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