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Identification of Thiourea-Based Inhibitors of the B-Cell Lymphoma 6 BTB Domain via NMR-Based Fragment Screening and Computer-Aided Drug Design

机译:基于NMR基片筛选和计算机辅助药物设计鉴定B细胞淋巴瘤6 BTB结构域的硫脲抑制剂

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摘要

Protein-protein interactions (PPI) between the transcriptional repressor B-cell lymphoma 6 (BCL6) BTB domain (BCL6(BTB)) and its corepressors have emerged as a promising target for anticancer therapeutics. However, identification of potent, drug-like inhibitors of BCL6(BTB) has remained challenging. Using NMR-based screening of a library of fragment-like small molecules, we have identified a thiourea compound (7CC5) that binds to BCL6(BTB). From this hit, the application of computer-aided drug design (CADD), medicinal chemistry, NMR spectroscopy, and X-ray crystallography has yielded an inhibitor, 15f, that demonstrated over 100-fold improved potency for BCL6(BTB). This gain in potency was achieved by a unique binding mode that mimics the binding mode of the corepressor SMRT in the aromatic and the HDCH sites. The structure-activity relationship based on these new inhibitors will have a significant impact on the rational design of novel BCL6 inhibitors, facilitating the identification of therapeutics for the treatment of BCL6-dependent tumors.
机译:转录抑制剂B细胞淋巴瘤6(BCL6)BTB结构域(BCL6(BCL6)的蛋白质 - 蛋白质相互作用(PPI)及其核心投降被作为抗癌治疗剂的有希望的靶标。然而,稳定性的Bcl6(BTB)的药物状抑制剂仍然挑战。使用基于NMR的筛选的片段状小分子库,我们已经确定了与BCl6(BTB)结合的硫脲化合物(7cc5)。从这种命中,计算机辅助药物设计(CADD),药物化学,NMR光谱和X射线晶体学的应用产生了抑制剂,15F,其显示为BCL6(BTB)的100倍改善效力。通过一种独特的绑定模式实现了这种效力的增益,其模拟了芳族和HDCH位点中的铁心SMRT的结合模式。基于这些新抑制剂的结构 - 活性关系将对新型BCL6抑制剂的合理设计产生重大影响,促进了治疗BCL6依赖性肿瘤的治疗方法。

著录项

  • 来源
    《Journal of Medicinal Chemistry》 |2018年第17期|共16页
  • 作者单位

    Univ Maryland Sch Pharm Dept Pharmaceut Sci 20 Penn St Baltimore MD 21201 USA;

    Univ Michigan Dept Pathol Ann Arbor MI 48109 USA;

    Univ Maryland Sch Pharm Dept Pharmaceut Sci 20 Penn St Baltimore MD 21201 USA;

    Weill Cornell Med Coll Dept Hematol Oncol New York NY 10021 USA;

    Univ Maryland Sch Pharm Dept Pharmaceut Sci 20 Penn St Baltimore MD 21201 USA;

    Univ Maryland Sch Pharm Dept Pharmaceut Sci 20 Penn St Baltimore MD 21201 USA;

    Univ Michigan Dept Pathol Ann Arbor MI 48109 USA;

    Weill Cornell Med Coll Dept Hematol Oncol New York NY 10021 USA;

    Weill Cornell Med Coll Dept Hematol Oncol New York NY 10021 USA;

    Univ Maryland Sch Pharm Dept Pharmaceut Sci 20 Penn St Baltimore MD 21201 USA;

    Univ Michigan Dept Pathol Ann Arbor MI 48109 USA;

    Univ Maryland Sch Pharm Dept Pharmaceut Sci 20 Penn St Baltimore MD 21201 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学;
  • 关键词

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