Identification of isoquinolinone DHODH inhibitor isosteres

Lindsey G DeRatt; Zhuming Zhang; E Christine Pietsch; Justin Cisar; Aihua Wang; Chao-Yuan Wang; Alexandra Tanner; Paul Shaffer; Edgar Jacoby; Faraz Kazmi; Neetu Shukla; Ulrike Philippar; Ricardo M Attar; James P Edwards; Scott D Kuduk

doi:10.1016/j.bmcl.2024.129965

Identification of isoquinolinone DHODH inhibitor isosteres

Bioorg Med Chem Lett. 2024 Sep 14:129965. doi: 10.1016/j.bmcl.2024.129965. Online ahead of print.

Authors

Affiliations

¹ Janssen Research and Development, Spring House, PA 19477, USA. Electronic address: lderatt@its.jnj.com.
² Janssen Research and Development, Spring House, PA 19477, USA.
³ Janssen Research and Development, Turnhoutseweg 30, B-2340 Beerse, Belgium.
⁴ Janssen Research and Development, Spring House, PA 19477, USA. Electronic address: skuduk@its.jnj.com.

PMID: 39284456
DOI: 10.1016/j.bmcl.2024.129965

Abstract

DHODH inhibition represents an attractive approach to overcome differentiation blockade for the treatment of AML. In a previous communication, we described our efforts leading to the discovery of compound 3 (JNJ-74856665), an orally bioavailable, potent, and selective DHODH inhibitor for clinical development. Guided by the co-crystal structures bound to human DHODH, other fused six-membered constructs were explored as isosteric replacements of the isoquinolinone central core. The correct positioning of the nitrogen in these core systems proved to be essential in modulating potency. Herein is described the synthesis of these complexly functionalized cores and their profiling, leading to DHODH inhibitors that possess favorable properties suitable for further development.

Keywords: 6,6-Fused bicyclic; AML; DHODH; Differentiation therapy; Dihydroorotate; Isosteric; Phthalazinone; Pyrimidine.