Optimization of the phenylurea moiety in a phosphoinositide 3-kinase (PI3K) inhibitor to improve water solubility and the PK profile by introducing a solubilizing group and ortho substituents

Hatsuo Kawada,Hirosato Ebiike,Masao Tsukazaki,Shun Yamamoto,Kohei Koyama,Mitsuaki Nakamura,Kenji Morikami,Kiyoshi Yoshinari,Miyuki Yoshida,Kotaro Ogawa,Nobuo Shimma,Takuo Tsukuda,Jun Ohwada

Optimization of the phenylurea moiety in a phosphoinositide 3-kinase (PI3K) inhibitor to improve water solubility and the PK profile by introducing a solubilizing group and ortho substituents

2016

Hatsuo Kawada
Hirosato Ebiike
Masao Tsukazaki
Shun Yamamoto
Kohei Koyama
Mitsuaki Nakamura
Kenji Morikami
Kiyoshi Yoshinari
Miyuki Yoshida
Kotaro Ogawa
Nobuo Shimma
Takuo Tsukuda
Jun Ohwada

Abstract Phosphoinositide 3-kinase (PI3K) is a promising anti-cancer target, because various mutations and amplifications are observed in human tumors isolated from cancer patients. Our dihydropyrrolopyrimidine derivative with a phenylurea moiety showed strong PI3K enzyme inhibitory activity, but its pharmacokinetic property was poor because of lack of solubility. Herein, we report how we improved the solubility of our PI3K inhibitors by introducing a solubilizing group and ortho substituents to break molecular planarity.

Keywords:

Enzyme
Biochemistry
Solubility
Organic chemistry
Chemistry
PI3K/AKT/mTOR pathway
Moiety
Phosphoinositide 3-kinase
Pharmacokinetics
Aqueous solution
Stereochemistry
enzyme inhibitory

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