Investigation of Biaryl Heterocycles As Inhibitors of Wee1 Kinase

Overview

Journal Bioorg Med Chem Lett

Specialty Biochemistry

Date 2019 Apr 25

PMID 31014911

Citations 2

Authors

Anthony Mastracchio

Chunqiu Lai

Maricel Torrent

Kenneth Bromberg

Fritz G Buchanan

Debra Ferguson

Velitchka Bontcheva

Eric F Johnson

Loren Lasko

David Maag

Alexander R Shoemaker

Thomas D Penning

Affiliations

Soon will be listed here.

Abstract

In continuation of our previous research towards the discovery of potent, selective and drug-like Wee1 inhibitors, 2 novel series of biaryl heterocycles were designed, synthesized and evaluated. The new biaryl cores were designed to enable structure-activity exploration of substituents at C-8 or N-8 which were used for tuning compound properties and to improve compound profiles. The lead molecule 33 demonstrated a desirable pharmacokinetic profile and potentiated the anti-proliferative activity of irinotecan in vivo when dosed orally in the human breast MX-1 xenograft model.

Citing Articles

Live cell screening to identify RNA-binding small molecule inhibitors of the pre-let-7-Lin28 RNA-protein interaction.

Rosenblum S, Soueid D, Giambasu G, Vander Roest S, Pasternak A, DiMauro E RSC Med Chem. 2024; 15(5):1539-1546.

PMID: 38784453 PMC: 11110735. DOI: 10.1039/d4md00123k.

Synthetic and Medicinal Chemistry Approaches Toward WEE1 Kinase Inhibitors and Its Degraders.

Alli V, Yadav P, Suresh V, Jadav S ACS Omega. 2023; 8(23):20196-20233.

PMID: 37323408 PMC: 10268025. DOI: 10.1021/acsomega.3c01558.