Discovery of IPN60090, a Clinical Stage Selective Glutaminase-1 (GLS-1) Inhibitor with Excellent Pharmacokinetic and Physicochemical Properties. Academic Article

Overview

abstract

Inhibition of glutaminase-1 (GLS-1) hampers the proliferation of tumor cells reliant on glutamine. Known glutaminase inhibitors have potential limitations, and in vivo exposures are potentially limited due to poor physicochemical properties. We initiated a GLS-1 inhibitor discovery program focused on optimizing physicochemical and pharmacokinetic properties, and have developed a new selective inhibitor, compound 27 (IPN60090), which is currently in phase 1 clinical trials. Compound 27 attains high oral exposures in preclinical species, with strong in vivo target engagement, and should robustly inhibit glutaminase in humans.

authors

Soth, Michael J

Di Francesco, Maria Emilia

Hamilton, Matthew M

Carroll, Chris L

Kovacs, Jeffrey J

Bardenhagen, Jennifer P

Bristow, Christopher A

de Stanchina, Elisa

Do, Mary K Geck

Greer, Jennifer

Herrera, Zachary

Giuliani, Virginia

Jiang, Yongying

Johnson, Sarah B

Johnson, Troy A

Leonard, Paul G

McAfoos, Timothy

Miller, Meredith

Morlacchi, Pietro

Mullinax, Robert A

Palmer, Wylie S

Rudin, Charles
Shepard, Hannah E
Spencer, Nakia D
Theroff, Jay
Wu, Qi
Xu, Alan
Yau, Ju Anne
Draetta, Giulio
Toniatti, Carlo
Heffernan, Timothy P
Jones, Philip

publication date

October 29, 2020

published in

Journal of medicinal chemistry Journal

Research

keywords

Enzyme Inhibitors
Glutaminase
Triazoles

Identity

PubMed Central ID

PMC9007139

Scopus Document Identifier

85095815489

Digital Object Identifier (DOI)

10.1021/acs.jmedchem.0c01398

PubMed ID

33118821

Additional Document Info

has global citation frequency

59

volume

63

issue

21