Identification of Clinical Candidate M2698, a Dual p70S6K and Akt Inhibitor, for Treatment of PAM Pathway-Altered Cancers

Authors :: Brian H. Heasley
Jing Lin
Thomas F. N. Haxell
Igor Mochalkin
Constantin Neagu
Felix Rohdich
Ruoxi Lan
Amanda E. Sutton
Jennifer Jackson
Potnick Justin
Bayard R. Huck
Andreas Machl
Katrin Georgi
Xiaoling Chen
Sherer Brian A
Erik Wilker
Thomas E. Richardson
Anderson Clark
Reinaldo Jones
Johnson Theresa L
Lizbeth Celeste Deselm
Andreas Goutopoulos
Hui Tian
Yufang Xiao
Joseph A. Moore
Lindsey Crowley
Source :: Journal of Medicinal Chemistry. 64:14603-14619
Publication Year :: 2021
Publisher :: American Chemical Society (ACS), 2021.
Abstract: Herein, we report the discovery of a novel class of quinazoline carboxamides as dual p70S6k/Akt inhibitors for the treatment of tumors driven by alterations to the PI3K/Akt/mTOR (PAM) pathway. Through the screening of in-house proprietary kinase library, 4-benzylamino-quinazoline-8-carboxylic acid amide 1 stood out, with sub-micromolar p70S6k biochemical activity, as the starting point for a structurally enabled p70S6K/Akt dual inhibitor program that led to the discovery of M2698, a dual p70S6k/Akt inhibitor. M2698 is kinase selective, possesses favorable physical, chemical, and DMPK profiles, is orally available and well tolerated, and displayed tumor control in multiple in vivo studies of PAM pathway-driven tumors.

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