耐受性
化学
临床试验
药理学
治疗指标
医学
癌症研究
加药
体内
内科学
不利影响
药品
生物
生物技术
作者
Ulrich Lücking,Dirk Kosemund,Niels Böhnke,Philip Lienau,Gerhard Siemeister,Karsten Denner,Rolf Bohlmann,Hans Briem,Ildiko Terebesi,Ulf Bömer,Martina Schäfer,Stuart Ince,Dominik Mumberg,Arne Scholz,Raquel Izumi,Stuart Hwang,Franz von Nussbaum
标识
DOI:10.1021/acs.jmedchem.1c01000
摘要
Selective inhibition of exclusively transcription-regulating positive transcription elongation factor b/CDK9 is a promising new approach in cancer therapy. Starting from atuveciclib, the first selective CDK9 inhibitor to enter clinical development, lead optimization efforts aimed at identifying intravenously (iv) applicable CDK9 inhibitors with an improved therapeutic index led to the discovery of the highly potent and selective clinical candidate VIP152. The evaluation of various scaffold hops was instrumental in the identification of VIP152, which is characterized by the underexplored benzyl sulfoximine group. VIP152 exhibited the best preclinical overall profile in vitro and in vivo, including high efficacy and good tolerability in xenograft models in mice and rats upon once weekly iv administration. VIP152 has entered clinical trials for the treatment of cancer with promising longterm, durable monotherapy activity in double-hit diffuse large B-cell lymphoma patients.
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