Oncotarget

Research Papers:

ERpS294 is a biomarker of ligand or mutational ERα activation and a breast cancer target for CDK2 inhibition

Gary K. Scott, David Chu, Ravneet Kaur, Julia Malato, Daniel E. Rothschild, Katya Frazier, Serenella Eppenberger-Castori, Byron Hann, Ben Ho Park and Christopher C. Benz _

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Oncotarget. 2017; 8:83432-83445. https://doi.org/10.18632/oncotarget.12735

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Abstract

Gary K. Scott1,*, David Chu2,*, Ravneet Kaur1, Julia Malato3, Daniel E. Rothschild1, Katya Frazier1, Serenella Eppenberger-Castori4, Byron Hann3, Ben Ho Park2, and Christopher C. Benz1,3

1 Buck Institute for Research on Aging, Novato, CA, USA

2 The Johns Hopkins University School of Medicine, Baltimore, MD, USA

3 Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, CA, USA

4 Institute for Pathology, Basel University Hospital, Basel, Switzerland

* These authors made equal contribution to this work

Correspondence to:

Christopher C. Benz, email:

Keywords: ERα phosphorylation, ESR1 mutations, cyclin-dependent kinase-2 inhibitors

Received: September 15, 2016 Accepted: September 25, 2016 Published: October 18, 2016

Abstract

ERα phosphorylation at hinge site S294 (pS294) was recently shown to be essential for ER-dependent gene transcription and mediated by an unknown cyclin-dependent kinase (CDK). This study was undertaken to identify the exact CDK pathway mediating pS294 formation, and to determine if this phosphorylation event occurs with, and can be targeted to treat, the ligand-independent growth of breast cancers expressing endocrine-refractory ESR1 mutations. Using a newly developed anti-pS294 monoclonal antibody, a combination of CDK specific siRNA knockdown studies and a broad panel of CDK selective inhibitors against ligand (E2)-stimulated MCF7 cells, we first identified CDK2 as the primary mediator of pS294 formation and showed that CDK2-selective inhibitors like Dinaciclib, but not CDK4/6 inhibitors like Palbociclib, can selectively prevent pS294 formation and repress ER-dependent gene expression. We then expressed the ER-activating mutations ERmut(Y537S) and ERmut(D538G) in MCF7 cells, and demonstrated their ability to induce ligand-independent and tamoxifen-resistant growth, associated with constitutive and CDK2-dependent pS294 expression. Following robust growth of E2-independent and TAM-resistant MCF7mutER(Y537S) tumors in vivo, nude mice were also treated with either Dinaciclib or Palbociclib at doses and injection schedules unable to retard tumor growth as single agents; the TAM plus Palbociclib combination arrested further tumor growth without affecting pS294 formation, while the TAM plus Dinaciclib combination produced tumor regression associated with loss of pS294 expression. These findings, and our proposed mechanistic model, provide new rationale for the clinical evaluation of CDK2 inhibitors given in combination with endocrine agents as a new treatment strategy against ESR1 mutation expressing breast cancers.


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