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首页> 外文期刊>Journal of Medicinal Chemistry >5-Aryl-1,3,4-oxadiazol-2-ylthioalkanoic Acids: A Highly Potent New Class of Inhibitors of Rho/Myocardin-Related Transcription Factor (MRTF)/Serum Response Factor (SRF)-Mediated Gene Transcription as Potential Antifibrotic Agents for Scleroderma
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5-Aryl-1,3,4-oxadiazol-2-ylthioalkanoic Acids: A Highly Potent New Class of Inhibitors of Rho/Myocardin-Related Transcription Factor (MRTF)/Serum Response Factor (SRF)-Mediated Gene Transcription as Potential Antifibrotic Agents for Scleroderma

机译:5-芳基-1,3,4-恶二唑-2-基烷烃:一种高效的rho /心肌素相关转录因子(MRTF)/血清响应因子(SRF)介导的基因转录作为潜在的抗纤维凝聚剂的高效新类抑制剂 用于硬皮病

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摘要

Through a phenotypic high-throughput screen using a serum response element luciferase promoter, we identified a novel 5-aryl-1,3,4-oxadiazol-2-ylthiopropionic acid lead inhibitor of Rho/myocardin-related transcription factor (MRTF)/serum response factor (SRF)-mediated gene transcription with good potency (IC50 = 180 nM). We were able to rapidly improve the cellular potency by 5 orders of magnitude guided by sharply defined and synergistic SAR. The remarkable potency and depth of the SAR, as well as the relatively low molecular weight of the series, suggests, but does not prove, that binding to the unknown molecular target may be occurring through a covalent mechanism. The series nevertheless has no observable cytotoxicity up to 100 mu M. Ensuing pharmacokinetic optimization resulted in the development of two potent and orally bioavailable anti-fibrotic agents that were capable of dose-dependently reducing connective tissue growth factor gene expression in vitro as well as significantly reducing the development of bleomycin-induced dermal fibrosis in mice in vivo.
机译:通过使用血清响应元素荧光素酶启动子的表型高通量筛网,我们鉴定了一种新的5-芳基-1,3,4-恶二唑-2-基二丙基酸铅抑制作用Rho / Myocardin相关转录因子(MRTF)/血清具有良好效力的响应因子(SRF)介导的基因转录(IC50 = 180nm)。我们能够通过急定定义和协同的SAR引导的5个数量级快速提高细胞效力。 SAR的显着效力和深度以及该系列的相对较低的分子量表明,但不证明,可以通过共价机制发生与未知分子靶标的结合。然而,该系列无可观察到的细胞毒性高达100亩M.随后的药代动力学优化导致两种有效和口服生物可利用的抗纤维化剂的发育,其能够在体外剂量依赖性地减少结缔组织生长因子基因表达以及显着减少减少体内小鼠博莱霉素诱导的皮肤纤维化的发展。

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  • 来源
    《Journal of Medicinal Chemistry》 |2019年第9期|共20页
  • 作者

    Kahl Dylan J.; Hutchings Kim M.; Lisabeth Erika Mathes; Haak Andrew J.; Leipprandt Jeffrey R.; Dexheimer Thomas; Khanna Dinesh; Tsou Pei-Suen; Campbell Phillip L.; Fox David A.; Wen Bo; Sun Duxin; Bailie Marc; Neubig Richard R.; Larsen Scott D.;

  • 作者单位

    Univ Michigan Coll Pharm Vahlteich Med Chem Core Ann Arbor MI 48109 USA;

    Univ Michigan Coll Pharm Vahlteich Med Chem Core Ann Arbor MI 48109 USA;

    Michigan State Univ Dept Pharmacol &

    Toxicol E Lansing MI 48824 USA;

    Michigan State Univ Dept Pharmacol &

    Toxicol E Lansing MI 48824 USA;

    Michigan State Univ Dept Pharmacol &

    Toxicol E Lansing MI 48824 USA;

    Michigan State Univ Dept Pharmacol &

    Toxicol E Lansing MI 48824 USA;

    Univ Michigan Med Ctr Dept Internal Med Div Rheumatol Ann Arbor MI 48109 USA;

    Univ Michigan Med Ctr Dept Internal Med Div Rheumatol Ann Arbor MI 48109 USA;

    Univ Michigan Med Ctr Dept Internal Med Div Rheumatol Ann Arbor MI 48109 USA;

    Univ Michigan Med Ctr Dept Internal Med Div Rheumatol Ann Arbor MI 48109 USA;

    Univ Michigan Coll Pharm UM Pharmcokinet Core Ann Arbor MI 48109 USA;

    Univ Michigan Coll Pharm UM Pharmcokinet Core Ann Arbor MI 48109 USA;

    Michigan State Univ Vivo Facil E Lansing MI 48824 USA;

    Michigan State Univ Dept Pharmacol &

    Toxicol E Lansing MI 48824 USA;

    Univ Michigan Coll Pharm Vahlteich Med Chem Core Ann Arbor MI 48109 USA;

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  • 正文语种 eng
  • 中图分类 药学;
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