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Identification and Optimization of Novel Cathepsin C Inhibitors Derived from EGFR Inhibitors

机译:EGFR抑制剂新型组织蛋白酶C抑制剂的鉴定和优化

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摘要

In the course of developing the biochemistry to chemistry activity-based protein profiling (BTC-ABPP) method, we herein unexpectedly discovered that the epidermal growth factor receptor irreversible inhibitor WZ4002 also functioned as a low micromolar inhibitor of cathepsin C (CatC), a promising target for the treatment of numerous inflammatory and autoimmune diseases. Building on from this discovery, and following structure-activity relationship investigations guided by computational modeling, a novel series of pyridine scaffold compounds were developed as irreversible CatC inhibitors, further culminated in identifying a highly potent and selective inhibitor 22, which displays good metabolic stability and oral bioavailability. In vivo studies revealed that compound 22 clearly displays the ability to inhibit CatC, consequently leading to efficient inhibition of downstream neutrophil serine proteases in both bone marrow and blood. The overall excellent profile of compound 22 made it an interesting candidate for further preclinical investigation.
机译:在发展基于化学活性的蛋白质分析(BTC-ABPP)方法的生物化学过程中,我们意外地发现表皮生长因子受体不可逆抑制剂WZ4002还用作小组蛋白C(CATC)的低微胆抑制剂,这是一个有效的靶向治疗众多炎症和自身免疫疾病。从该发现的构建,并在计算模型引导的结构 - 活动关系调查之后,开发了一种新颖的吡啶支架化合物作为不可逆的CATC抑制剂,进一步升高,鉴定了高效和选择性抑制剂22,其显示出良好的代谢稳定性和口腔生物利用度。在体内研究表明,化合物22清楚地显示了抑制CATC的能力,从而导致骨髓和血液中的下游中性粒细胞丝氨酸蛋白酶有效抑制。化合物22的总体优异形状使其成为进一步的临床前调查的有趣候选者。

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  • 来源
    《Journal of Medicinal Chemistry》 |2019年第12期|共19页
  • 作者单位

    NIBS 7 Sci Pk Rd ZGC Life Sci Pk Beijing 102206 Peoples R China;

    NIBS 7 Sci Pk Rd ZGC Life Sci Pk Beijing 102206 Peoples R China;

    NIBS 7 Sci Pk Rd ZGC Life Sci Pk Beijing 102206 Peoples R China;

    NIBS 7 Sci Pk Rd ZGC Life Sci Pk Beijing 102206 Peoples R China;

    NIBS 7 Sci Pk Rd ZGC Life Sci Pk Beijing 102206 Peoples R China;

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