Identification and development of a subtype-selective allosteric AKT inhibitor suitable for clinical development

Author:

Page Natalie,Wappett Mark,O’Dowd Colin R.,O’Rourke Martin,Gavory Gerald,Zhang Lixin,Rountree J. S. Shane,Jordan Linda,Barker Oliver,Gibson Hayley,Boyd Caroline,Feutren-Burton Stephanie,McLean Estelle,Trevitt Graham,Harrison Timothy

Abstract

AbstractThe serine/threonine protein kinase AKT plays a pivotal role within the PI3K pathway in regulating cellular proliferation and apoptotic cellular functions, and AKT hyper-activation via gene amplification and/or mutation has been implicated in multiple human malignancies. There are 3 AKT isoenzymes (AKT1-3) which mediate critical, non-redundant functions. We present the discovery and development of ALM301, a novel, allosteric, sub-type selective inhibitor of AKT1/2. ALM301 binds in an allosteric pocket created by the combined movement of the PH domain and the catalytic domain, resulting in a DFG out conformation. ALM301 was shown to be highly selective against a panel of over 450 kinases and potently inhibited cellular proliferation. These effects were particularly pronounced in MCF-7 cells containing a PI3KCA mutation. Subsequent cellular downstream pathway analysis in this sensitive cell line revealed potent inhibition of pAKT signalling up to 48 h post dosing. ALM301 treatment was well tolerated in an MCF-7 xenograft model and led to a dose-dependent reduction in tumour growth. Enhanced efficacy was observed in combination with tamoxifen. In summary, ALM301 is a highly specific AKT 1/2 inhibitor with an excellent pharmacological profile suitable for further clinical development.

Funder

Invest Northern Ireland

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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