Discovery of GNE-149 as a Full Antagonist and Efficient Degrader of Estrogen Receptor alpha for ER+ Breast Cancer

Jun Liang; Robert Blake; Jae Chang; Lori S Friedman; Simon Goodacre; Steven Hartman; Ellen Rei Ingalla; James R Kiefer; Tracy Kleinheinz; Sharada Labadie; Jun Li; Kwong Wah Lai; Jiangpeng Liao; Vidhi Mody; Neville McLean; Ciara Metcalfe; Michelle Nannini; Daniel Otwine; Yingqing Ran; Nick Ray; Fabien Roussel; Amy Sambrone; Deepak Sampath; Maia Vinogradova; John Wai; Tao Wang; Kuen Yeap; Amy Young; Jason Zbieg; Birong Zhang; Xiaoping Zheng; Yu Zhong; Xiaojing Wang

doi:10.1021/acsmedchemlett.0c00224

Discovery of GNE-149 as a Full Antagonist and Efficient Degrader of Estrogen Receptor alpha for ER+ Breast Cancer

ACS Med Chem Lett. 2020 May 26;11(6):1342-1347. doi: 10.1021/acsmedchemlett.0c00224. eCollection 2020 Jun 11.

Authors

Jun Liang¹, Robert Blake¹, Jae Chang¹, Lori S Friedman¹, Simon Goodacre², Steven Hartman¹, Ellen Rei Ingalla¹, James R Kiefer¹, Tracy Kleinheinz¹, Sharada Labadie¹, Jun Li¹, Kwong Wah Lai³, Jiangpeng Liao³, Vidhi Mody¹, Neville McLean², Ciara Metcalfe¹, Michelle Nannini¹, Daniel Otwine¹, Yingqing Ran¹, Nick Ray², Fabien Roussel², Amy Sambrone¹, Deepak Sampath¹, Maia Vinogradova¹, John Wai³, Tao Wang³, Kuen Yeap², Amy Young¹, Jason Zbieg¹, Birong Zhang¹, Xiaoping Zheng³, Yu Zhong¹, Xiaojing Wang¹

Affiliations

¹ Genentech, Inc., 1 DNA Way, South San Francisco, California 94080, United States.
² Charles River Discovery Research Services UK Limited, 7-9 Spire Green Center, Flex Meadow, Harlow, Essex CM19 5TR, United Kingdom.
³ WuXi AppTec Co., Ltd, 288 Fute Zhong Road, Waigaoqiao Free Trade Zone, Shanghai 200131, P. R. China.

Abstract

Estrogen receptor alpha (ERα) is a well-validated drug target for ER-positive (ER+) breast cancer. Fulvestrant is FDA-approved to treat ER+ breast cancer and works through two mechanisms-as a full antagonist and selective estrogen receptor degrader (SERD)-but lacks oral bioavailability. Thus, we envisioned a "best-in-class" molecule with the same dual mechanisms as fulvestrant, but with significant oral exposure. Through lead optimization, we discovered a tool molecule 12 (GNE-149) with improved degradation and antiproliferative activity in both MCF7 and T47D cells. To illustrate the binding mode and key interactions of this scaffold with ERα, we obtained a cocrystal structure of 6 that showed ionic interaction of azetidine with Asp351 residue. Importantly, 12 showed favorable metabolic stability and good oral exposure. 12 exhibited antagonist effect in the uterus and demonstrated robust dose-dependent efficacy in xenograft models.