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Specificity quantification of biomolecular recognition and its implication for drug discovery

机译:生物分子识别的特异性定量及其在药物开发中的意义

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摘要

Highly efficient and specific biomolecular recognition requires both affinity and specificity. Previous quantitative descriptions of biomolecular recognition were mostly driven by improving the affinity prediction, but lack of quantification of specificity. We developed a novel method SPA (SPecificity and Affinity) based on our funneled energy landscape theory. The strategy is to simultaneously optimize the quantified specificity of the “native” protein-ligand complex discriminating against “non-native” binding modes and the affinity prediction. The benchmark testing of SPA shows the best performance against 16 other popular scoring functions in industry and academia on both prediction of binding affinity and “native” binding pose. For the target COX-2 of nonsteroidal anti-inflammatory drugs, SPA successfully discriminates the drugs from the diversity set, and the selective drugs from non-selective drugs. The remarkable performance demonstrates that SPA has significant potential applications in identifying lead compounds for drug discovery.
机译:高效和特异性的生物分子识别需要亲和力和特异性。以前对生物分子识别的定量描述主要是通过改善亲和力预测来实现的,但是缺乏特异性的量化。我们根据漏斗能量景观理论开发了一种新颖的方法SPA(特异性和亲和力)。该策略是同时优化区分“非天然”结合模式和亲和力预测的“天然”蛋白-配体复合物的定量特异性。 SPA的基准测试在预测结合亲和力和“天然”结合姿势方面均显示出优于行业和学术界其他16种流行评分功能的最佳性能。对于非甾体抗炎药的目标COX-2,SPA成功地从多样性集中区分了药物,将选择性药物与非选择性药物区分开。出色的性能表明,SPA在鉴定用于药物发现的先导化合物方面具有重要的潜在应用。

著录项

  • 期刊名称 Scientific Reports
  • 作者

    Zhiqiang Yan; Jin Wang;

  • 作者单位
  • 年(卷),期 -1(2),-1
  • 年度 -1
  • 页码 309
  • 总页数 7
  • 原文格式 PDF
  • 正文语种
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