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首页> 外文期刊>Journal of Medicinal Chemistry >Design of a Chemical Probe for the Bromodomain and Plant Homeodomain Finger-Containing (BRPF) Family of Proteins
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Design of a Chemical Probe for the Bromodomain and Plant Homeodomain Finger-Containing (BRPF) Family of Proteins

机译:溴琼酱和植物同源域的化学探针的设计含有(BRPF)蛋白质

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摘要

The bromodomain and plant homeodomain finger-containing (BRPF) family are scaffolding proteins important for the recruitment of histone acetyltransferases of the MYST family to chromatin. Here, we describe NI-57 (16) as new pan-BRPF chemical probe of the bromodomain (BRD) of the BRPFs. Inhibitor 16 preferentially bound the BRD of BRPF1 and BRPF2 over BRPF3, whereas binding to BRD9 was weaker. Compound 16 has excellent selectivity over nonclass IV BRD proteins. Target engagement of BRPF1B and BRPF2 with 16 was demonstrated in nanoBRET and FRAP assays. The binding of 16 to BRPF1B was rationalized through an X-ray cocrystal structure determination, which showed a flipped binding orientation when compared to previous structures. We report studies that show 16 has functional activity in cellular assays by modulation of the phenotype at low micromolar concentrations in both cancer and inflammatory models. Pharmacokinetic data for 16 was generated in mouse with single dose administration showing favorable oral bioavailability
机译:含有溴癌和植物同源域的手指(BRPF)家族是脚手架蛋白,用于募集Myst家族的组蛋白乙酰转移酶至染色质。在这里,我们描述了BRPFS的溴琼瓜素(BRD)的新泛-57(16)作为新的PAN-BRPF化学探针。抑制剂16优先与BRPF3结合BRPF1和BRPF2的BRD,而与BRD9的结合较弱。化合物16对非CLASS IV BRD蛋白具有优异的选择性。 BRPF1B和BRPF2具有16的目标接合在纳米多元和FRAP测定中证明。通过X射线Cocrystal结构测定,16至BRPF1B的结合通过X射线COCRYSTAL结构测定来合理地,该结构在与先前的结构相比时显示出翻转的结合取向。我们报告了表演16通过癌症和炎症模型的低微摩尔浓度的表型对细胞测定具有功能活性。用单剂量给药,在小鼠中产生16种药代动力学数据,显示出有利的口服生物利用度

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  • 来源
    《Journal of Medicinal Chemistry 》 |2017年第16期| 共14页
  • 作者单位

    UCL UCL Sch Pharm 29-39 Brunswick Sq London WC1N 1AX England;

    UCL UCL Sch Pharm 29-39 Brunswick Sq London WC1N 1AX England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    AstraZeneca Innovat Med &

    Early Dev Pepparedsleden 1 S-43183 Molndal Sweden;

    AstraZeneca Innovat Med &

    Early Dev Pepparedsleden 1 S-43183 Molndal Sweden;

    AstraZeneca Innovat Med &

    Early Dev Pepparedsleden 1 S-43183 Molndal Sweden;

    AstraZeneca Innovat Med &

    Early Dev Pepparedsleden 1 S-43183 Molndal Sweden;

    AstraZeneca Discovery Sci Darwin Bldg Cambridge Sci Pk Cambridge CB4 0FZ England;

    CRT Discovery Labs Jonas Webb Bldg Babraham Res Campus Cambridge CB22 3AT England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    Univ Oxford Nuffield Dept Clin Med Struct Genom Consortium Old Rd Campus Res Bldg Roosevelt Dr Oxford OX3 7DQ England;

    UCL UCL Sch Pharm 29-39 Brunswick Sq London WC1N 1AX England;

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  • 正文语种 eng
  • 中图分类 药学 ;
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