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Discovery and SAR of JTE-151: A Novel RORγ Inhibitor for Clinical Development

化学 临床试验 不利影响 药物发现 人类健康 计算生物学 药物开发 药品 药理学 内科学 医学 生物化学 生物 环境卫生
作者
Takaki Maeba,Kazuyuki Hirata,Masayuki Kotoku,Noriyoshi Seki,Katsuya Maeda,Shintaro Hirashima,Hiroshi Yamanaka,Takayuki Sakai,Shingo Obika,Akimi Hori,Yoshinori Hara,Satoru Noji,Yoshihiro Suwa,Masahiro Yokota,Shingo Fujioka,Takayuki Yamaguchi,Yoshiaki Katsuda,Takahiro Hata,Naoki Miyagawa,Kojo Arita,Yukihiro Nomura,Toshio Taniguchi,Kota Asahina,Yusuke Aratsu,Yuichi Naka,Tsuyoshi Adachi,Akihiro Nomura,Shota Akai,Shin-ichi Oshida,Sudhakar M. Pai,Paul D. Crowe,Erin K. Bradley,Ruo Steensma,Hai‐Yan Tao,Morgan Fenn,Robert E. Babine,Xiaolin Li,Scott M. Thacher,Takahiro Soeta,Yutaka Ukaji,Makoto Shiozaki
出处
期刊:Journal of Medicinal Chemistry [American Chemical Society]
卷期号:67 (2): 952-970
标识
DOI:10.1021/acs.jmedchem.3c01933
摘要

A number of RORγ inhibitors have been reported over the past decade. There were also several examples advancing to human clinical trials, however, none of them has reached the market yet, suggesting that there could be common obstacles for their future development. As was expected from the general homology of nuclear receptor ligands, insufficient selectivity as well as poor physicochemical properties were identified as potential risks for a RORγ program. Based on such considerations, we conducted a SAR investigation by prioritizing drug-like properties to mitigate such potential drawbacks. After an intensive SAR exploration with strong emphasis on "drug-likeness" indices, an orally available RORγ inhibitor, JTE-151, was finally generated and was advanced to a human clinical trial. The compound was confirmed to possess highly selective profiles along with good metabolic stability, and most beneficially, no serious adverse events (SAE) and good PK profiles were observed in the human clinical trial.
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