Validation of a New Methodology to Create Oral Drugs beyond the Rule of 5 for Intracellular Tough Targets.

Atsushi Ohta,Tatsuya Kato,Takashi Emura,Taiji Miyake,Kenichi Nomura,Shojiro Shinohara,Shiho Ishikawa,Yoshikazu Nishimura,Tatsuhiko Tachibana,Hitoshi Sase,Mikimasa Tanada,Ryuuichi Takeyama,Toshiya Ito,Shiori Kariyuki,Terushige Muraoka,Yasufumi Kikuchi,Aya Chiyoda,Kazuhiko Nakano,Atsushi Matsuo,Takuya Torizawa,Miki Kojima,Shota Tanaka,Hitoshi Iikura,Nozomi Hisada,Tetsuo Kojima,Kazuhisa Ozeki,Kaori Kimura,Masahiko Tanaka,Hatsuo Kawada,Ryuji Hayashi,Takeo Iida,Atsuko Higashida,Minoru Tamiya,Naoaki Murao,Kotaro Ogawa,Yuuji Sakurai,Ryusuke Takano,Koji Takano,Sho Akai,Tomoya Kotake,Satoshi Kuramoto ,Takeshi Shiraishi ,Yosuke Morita ,Masayasu Irie ,Michiyoshi Arai ,Yoshio Yamagishi ,Kenichi Ohara

doi:10.1021/jacs.3c07145

Abstract

Establishing a technological platform for creating clinical compounds inhibiting intracellular protein-protein interactions (PPIs) can open the door to many valuable drugs. Although small molecules and antibodies are mainstream modalities, they are not suitable for a target protein that lacks a deep cavity for a small molecule to bind or a protein found in intracellular space out of an antibody's reach. One possible approach to access these targets is to utilize so-called middle-size cyclic peptides (defined here as those with a molecular weight of 1000-2000 g/mol). In this study, we validated a new methodology to create oral drugs beyond the rule of 5 for intracellular tough targets by elucidating structural features and physicochemical properties for drug-like cyclic peptides and developing library technologies to afford highly N-alkylated cyclic peptide hits. We discovered a KRAS inhibitory clinical compound (LUNA18) as the first example of our platform technology.

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