Discovery of a Dihydroisoquinolinone Derivative (NVP-CGM097): A Highly Potent and Selective MDM2 Inhibitor Undergoing Phase 1 Clinical Trials in p53wt Tumors

Philipp Holzer,Keiichi Masuya,Pascal Furet,Joerg Kallen,Therese Valat-Stachyra,Stephane Ferretti,Joerg Berghausen,Michèle Bouisset-Leonard,Nicole Buschmann,Carole Pissot Soldermann,Caroline Rynn,Stephan Ruetz,Stefan Stutz,Patrick Chène,Sébastien Jeay,François Gessier

Discovery of a Dihydroisoquinolinone Derivative (NVP-CGM097): A Highly Potent and Selective MDM2 Inhibitor Undergoing Phase 1 Clinical Trials in p53wt Tumors

2015

Philipp Holzer
Keiichi Masuya
Pascal Furet
Joerg Kallen
Therese Valat-Stachyra
Stephane Ferretti
Joerg Berghausen
Michèle Bouisset-Leonard
Nicole Buschmann
Carole Pissot Soldermann
Caroline Rynn
Stephan Ruetz
Stefan Stutz
Patrick Chène
Sébastien Jeay
François Gessier

As a result of our efforts to discover novel p53:MDM2 protein–protein interaction inhibitors useful for treating cancer, the potent and selective MDM2 inhibitor NVP-CGM097 (1) with an excellent in vivo profile was selected as a clinical candidate and is currently in phase 1 clinical development. This article provides an overview of the discovery of this new clinical p53:MDM2 inhibitor. The following aspects are addressed: mechanism of action, scientific rationale, binding mode, medicinal chemistry, pharmacokinetic and pharmacodynamic properties, and in vivo pharmacology/toxicology in preclinical species.

Keywords:

Mdm2
Phases of clinical research
Cancer
Pharmacology
In vivo
Chemistry
Mechanism of action
Pharmacokinetics
NVP-CGM097

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