Discovery of a Slow Tight Binding LPA1 Antagonist (ONO-0300302) for the Treatment of Benign Prostatic Hyperplasia

Masahiko Terakado; Hidehiro Suzuki; Kazuya Hashimura; Motoyuki Tanaka; Hideyuki Ueda; Keisuke Hirai; Masaki Asada; Masahiro Ikura; Naoki Matsunaga; Hiroshi Saga; Koji Shinozaki; Naoko Karakawa; Yuka Takada; Masashi Minami; Hiromu Egashira; Yoshihiro Sugiura; Masanori Yamada; Shinji Nakade; Yoshikazu Takaoka

doi:10.1021/acsmedchemlett.7b00383

Discovery of a Slow Tight Binding LPA1 Antagonist (ONO-0300302) for the Treatment of Benign Prostatic Hyperplasia

ACS Med Chem Lett. 2017 Nov 20;8(12):1281-1286. doi: 10.1021/acsmedchemlett.7b00383. eCollection 2017 Dec 14.

Authors

Masahiko Terakado¹, Hidehiro Suzuki¹, Kazuya Hashimura¹, Motoyuki Tanaka¹, Hideyuki Ueda¹, Keisuke Hirai¹, Masaki Asada¹, Masahiro Ikura¹, Naoki Matsunaga¹, Hiroshi Saga¹, Koji Shinozaki¹, Naoko Karakawa¹, Yuka Takada¹, Masashi Minami¹, Hiromu Egashira¹, Yoshihiro Sugiura¹, Masanori Yamada¹, Shinji Nakade¹, Yoshikazu Takaoka¹

Affiliation

¹ Medicinal Chemistry Research Laboratories, Exploratory Research Laboratories, and Discovery Research Laboratories, ONO Pharmaceutical Co., Ltd., 3-1-1 Sakurai, Shimamoto, Mishima, Osaka 618-8585, Japan.

Abstract

Scaffold hopping from the amide group of lead compound ONO-7300243 (1) to a secondary alcohol successfully gave a novel chemotype lysophosphatidic acid receptor 1 (LPA₁) antagonist 4. Wash-out experiments using rat isolated urethra showed that compound 4 possesses a tight binding feature to the LPA₁ receptor. Further modification of two phenyl groups of 1 to pyrrole and an indane moiety afforded an optimized compound ONO-0300302 (19). Despite its high i.v. clearance, 19 inhibited significantly an LPA-induced increase of intraurethral pressure (IUP) in rat (3 mg/kg, p.o.) and dog (1 mg/kg, p.o.) over 12 h. Binding experiments with [³H]-ONO-0300302 suggest that the observed long duration action is because of the slow tight binding character of 19.