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Simulations of mutant p53 DNA binding domains reveal a novel druggable pocket

机译:突变体P53 DNA结合结构域的仿真显示出一种新型可粘袋

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摘要

The DNA binding domain (DBD) of the tumor suppressor p53 is the site of several oncogenic mutations. A subset of these mutations lowers the unfolding temperature of the DBD. Unfolding leads to the exposure of a hydrophobic -strand and nucleates aggregation which results in pathologies through loss of function and dominant negative/gain of function effects. Inspired by the hypothesis that structural changes that are associated with events initiating unfolding in DBD are likely to present opportunities for inhibition, we investigate the dynamics of the wild type (WT) and some aggregating mutants through extensive all atom explicit solvent MD simulations. Simulations reveal differential conformational sampling between the WT and the mutants of a turn region (S6-S7) that is contiguous to a known aggregation-prone region (APR). The conformational properties of the S6-S7 turn appear to be modulated by a network of interacting residues. We speculate that changes that take place in this network as a result of the mutational stress result in the events that destabilize the DBD and initiate unfolding. These perturbations also result in the emergence of a novel pocket that appears to have druggable characteristics. FDA approved drugs are computationally screened against this pocket.
机译:肿瘤抑制器P53的DNA结合结构域(DBD)是几种致癌突变的位点。这些突变的子集降低了DBD的展开温度。展开导致疏水性 - 疏水性的曝光和成核聚集,这通过损失功能和函数效应的显性负/增益导致病理学。灵感灵感来自假设与在DBD中发挥展开的事件相关的结构变化可能呈现抑制的机会,我们通过广泛的所有原子显式溶剂MD模拟研究野生型(WT)和一些聚集突变体的动态。仿真在转向区域(S6-S7)与已知聚合 - 易于区域(APR)上的旋转区域(S6-S7)之间的差异构象采样揭示了差异构象取样。 S6-S7转的构象性质似乎由交互残留的网络调制。我们推测了由于变形应力而导致在该网络中发生的变化导致破坏DBD并启动展开的事件。这些扰动也导致出现一种新的口袋,似乎具有可耐用的特性。 FDA批准的药物在计算上筛查此口袋。

著录项

  • 来源
    《Nucleic Acids Research》 |2019年第4期|共16页
  • 作者单位

    ASTAR Bioinformat Inst 30 Biopolis St 07-01 Matrix Singapore 138671 Singapore;

    ASTAR P53 Lab 8A Biomed Grove 06-04-05 Neuros Immunos Singapore 138648 Singapore;

    ASTAR Bioinformat Inst 30 Biopolis St 07-01 Matrix Singapore 138671 Singapore;

    ASTAR Bioinformat Inst 30 Biopolis St 07-01 Matrix Singapore 138671 Singapore;

    ASTAR Bioinformat Inst 30 Biopolis St 07-01 Matrix Singapore 138671 Singapore;

    Nanyang Technol Univ Sch Comp Engn 50 Nanyang Ave Singapore 639798 Singapore;

    ASTAR P53 Lab 8A Biomed Grove 06-04-05 Neuros Immunos Singapore 138648 Singapore;

    ASTAR P53 Lab 8A Biomed Grove 06-04-05 Neuros Immunos Singapore 138648 Singapore;

    ASTAR Bioinformat Inst 30 Biopolis St 07-01 Matrix Singapore 138671 Singapore;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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