Discovery and SAR Studies of Potent Modulators of BMI‐1 Expression

Author:

Baiazitov Ramil Y.1ORCID,Sydorenko Nadiya1,Du Wu2,Ren Hongyu1,Cao Liang1,Davis Thomas3,Cintron‐Lue Katherine1ORCID,Kim Min‐Jung1,Zhuo Jin1,Mody Shreshtha1,Weetall Marla1ORCID,Sheedy Josephine1ORCID,Risher Nicole1,Almstead Neil4,Moon Young‐Choon1ORCID

Affiliation:

1. PTC USA – NJ Center of Excellence Campus 1013 Route 202/206 Bridgewater NJ 08807 USA

2. Hinova Pharmaceuticals Inc. 4th FL Rongyao Building 5 Keyuan South Road Chengdu Sichuan 610041 P. R. China

3. 268 Prospect St South Orange NJ 07079 USA

4. PTC USA – Hopewell 311 Pennington Rocky Hill Rd. Pennington NJ 08534 USA

Abstract

AbstractIn our efforts to identify molecules that selectively reduce the expression of BMI1, a stem cell gene, we discovered and characterized the first‐in‐class series of small molecules that modulate the expression of BMI1 protein in cancer cells. Structure–activity and structure–property relationships associated with this series were investigated through medicinal chemistry efforts. These studies revealed important structural features required for achieving anti‐tumor activity and acceptable pharmacokinetic properties within this series. The 4‐CF3−Ph at the left‐side of the molecule, a proper placement of the N‐atom on the six‐membered heterocycle in the middle, combined with a properly substituted C(2)‐methyl benzimidazole on the right‐hand side were required to achieve potency, microsomal stability, and exposure upon oral dosing. A compound (PTC‐02) with acceptable pharmacological properties and efficacious in vivo in several tumor animal models was identified.

Publisher

Wiley

Subject

Inorganic Chemistry,Organic Chemistry,Physical and Theoretical Chemistry,Drug Discovery,Biochemistry,Catalysis

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