De novo or acquired resistance to endocrine therapy is a key driver of relapse and tumor progression in patients with estrogen receptor (ER+) breast cancer. Downregulation of the ER? is a well-established yet poorly understand mechanism of endocrine resistance. Currently there are no approved or investigational therapies that can restore ER? expression after downregulation occurs. Our preclinical research was the first to demonstrate in luminal ER+ breast cancer a novel role of Aurora-A kinase (AURKA) in the induction of stemness reprogramming and expansion of a sub-population of CD44high/CD24low breast tumor initiating cells (BTICs). These BTICs have low ER? expression and are resistant to endocrine therapy. They are further characterized by stem cell-like phenotype that mediates tumor properties of invasion, self-renewal, drug resistance, and metastasis. We propose in ER+ breast cancer that activation of AUKRA induces expansion of BTICs during tumor progression that drives ER? downregulation and endocrine resistance. When BTICs are treated with the selective AURKA inhibitor, alisertib, the luminal phenotype, ER? expression and endocrine sensitivity are restored. Our preclinical data demonstrates synergy when alisertib is combined with fulvestrant in endocrine resistant models. We have recently determined the maximum tolerated dose of alisertib in combination with standard dose fulvestrant in a phase I clinical trial in advanced ER+ breast cancer. An excellent safety profile and impressive 6-month clinical benefit rate of 78% were observed. The objective of the proposed research is to explore in preclinical models and clinical biospecimens the molecular mechanisms by which AURKA promotes endocrine resistance through stemness reprogramming and downregulation of ER?. Our central hypothesis is that alisertib selectively targets BTICs and converts them to a CD44low/CD24high luminal phenotype with increased ER? expression and sensitivity to endocrine therapy. The following Aims will assess the central hypothesis:
In Specific Aim 1 we will evaluate AURKA as a novel biomarker and therapeutic target in endocrine resistant, metastatic breast cancer.
In Specific Aim 2 we will determine in vivo the mechanisms underlying AURKA-induced endocrine resistance and tumor progression.
In Specific Aim 3 we will define the role of SMAD5/SOX2 transcriptional network in mediating AURKA-induced enrichment of CD44high/CD24low/ER?low BTICs. Dissecting the mechanisms by which AURKA induces stemness reprogramming is of high translational significance because AURKA inhibitors may represent a novel therapeutic approach to address de novo and acquired endocrine resistance due to ER? downregulation. The proposed research will establish the extent to which targeting AURKA has consequent benefit to delay or prevent tumor progression and improve the survival of patients with ER+ breast cancer. This research is directly relevant to the goals of the NIH because it will enhance our understanding of the mechanisms that drive endocrine resistance and breast cancer progression.

Public Health Relevance

Most breast cancers express the estrogen receptor (ER), and most are sensitive to hormonal (endocrine) treatment. Unfortunately, some ER+ breast tumors frequently progress to a more aggressive state characterized by resistance to therapy, spread to other organs, and poor clinical outcomes. We propose a novel mechanism of resistance to endocrine therapy that results from the growth of a population of cells within the tumor called, breast tumor initiating cells (BTICs). This process is stimulated by the protein, Aurora A Kinase (AURKA). These BTICs have the ability to self-renew and perpetuate the tumor. Furthermore they lose some if not all ER expression which renders them, and thus the entire tumor, resistant to endocrine therapy. Currently there are no approved therapies that can target AURKA or endocrine resistance that results from the loss of ER expression. Experiments proposed in this application will characterize the mechanisms responsible for the initiation and growth of these endocrine resistant BTICs. Experiments will also address whether or not the drug, alisertib, an investigational AURKA inhibitor, will restore ER expression and tumor sensitivity to endocrine therapy in mouse models. Importantly, we will also test this alisertib alone and combined with standard endocrine therapy (fulvestrant) in women with advanced, endocrine resistant breast cancer. Blood and tumor samples will be collected from patients participating in this trial, and they will be utilized to assess whether alisertib suppresses the development of these BTICs and restores tumor ER expression. If these experiments are successful, they may serve as the foundation for a new treatment option to delay or suppress the development of endocrine resistance and cancer spread to other organs in women with ER+ breast cancer.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA214893-02
Application #
9518695
Study Section
Clinical Oncology Study Section (CONC)
Program Officer
Sathyamoorthy, Neeraja
Project Start
2017-08-01
Project End
2022-05-31
Budget Start
2018-06-01
Budget End
2019-05-31
Support Year
2
Fiscal Year
2018
Total Cost
Indirect Cost
Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905
Leontovich, Alexey A; Jalalirad, Mohammad; Salisbury, Jeffrey L et al. (2018) NOTCH3 expression is linked to breast cancer seeding and distant metastasis. Breast Cancer Res 20:105