Synergy between Androgen Receptor Antagonism and Inhibition of mTOR and HER2 in Breast Cancer

Gordon, Michael A.; D’Amato, Nicholas C.; Gu, Haihua; Babbs, Beatrice; Wulfkuhle, Julia; Petricoin, Emanuel F.; Gallagher, Rosa I.; Dong, Ting; Torkko, Kathleen C.; Liu, Bolin; Elias, Anthony; Richer, Jennifer K.

doi:10.1158/1535-7163.mct-17-0111

Cited by 50 publications

(41 citation statements)

References 42 publications

(45 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…However, abiraterone acetate activity in prostate preclinical model was demonstrated to be also linked to a competitive binding to the AR (45,46). Although the additive effects we measured in vitro were not as pronounced as the ones described using chemotherapy combinations, they were in-line with the effects of combinations using antiandrogens reported in MDA-MB-453 cells (11,47).…”

Section: Discussionsupporting

confidence: 82%

Enhancing Abiraterone Acetate Efficacy in Androgen Receptor–positive Triple-negative Breast Cancer: Chk1 as a Potential Target

Grellety

Callens

Richard

et al. 2019

Clinical Cancer Research

View full text Add to dashboard Cite

Purpose: Our aim was to identify predictive factors of abiraterone acetate efficacy and putative new druggable targets in androgen receptor (AR)-positive triple-negative breast cancer (TNBC) treated in the UCBG 2012-1 trial.Experimental Design: We defined abiraterone acetate response as either complete or partial response, or stable disease at 6 months. We sequenced 91 general and breast cancer-associated genes from the tumor DNA samples. We analyzed transcriptomes from the extracted RNA samples on a NanoString platform and performed IHC using tissue microarrays. We assessed abiraterone acetate and Chk1 inhibitors (GDC-0575 and AZD7762) efficacies, either alone or in combination, on cell lines grown in vitro and in vivo.Results: Classic IHC apocrine markers including AR, FOXA1, GGT1, and GCDFP15, from patients' tumors allowed identifying abiraterone acetate-responders and nonrespon-ders. All responders had clear apocrine features. Transcriptome analysis revealed that 31 genes were differentially expressed in the two subgroups, 9 of them being linked to proliferation and DNA damage repair. One of the most significant differences was the overexpression, in nonresponders, of CHEK1, a gene encoding Chk1, a protein kinase that can be blocked by specific inhibitors. On the basis of cell line experiments, abiraterone acetate and Chk1 inhibitor combination showed at least additive effect on cell viability, cell cycle, apoptosis, and accumulation of DNA damages. In vivo, orthotopic xenograft experiments confirmed the efficacy of this combination therapy.Conclusions: This study suggests that apocrine features can be helpful in the identification of abiraterone acetateresponders. We identified Chk1 as a putative drug target in AR-positive TNBCs.

show abstract

Section: Discussionsupporting

confidence: 82%

Enhancing Abiraterone Acetate Efficacy in Androgen Receptor–positive Triple-negative Breast Cancer: Chk1 as a Potential Target

Grellety

Callens

Richard

et al. 2019

Clinical Cancer Research

View full text Add to dashboard Cite

show abstract

“…For both examples, there is prior evidence for a role in resistance to trastuzumab but persistent controversy regarding the clinical actionability of these proposed mechanisms 29,39,40 .…”

Section: Articlementioning

confidence: 99%

Microscaled proteogenomic methods for precision oncology

et al. 2020

View full text Add to dashboard Cite

Cancer proteogenomics promises new insights into cancer biology and treatment efficacy by integrating genomics, transcriptomics and protein profiling including modifications by mass spectrometry (MS). A critical limitation is sample input requirements that exceed many sources of clinically important material. Here we report a proteogenomics approach for core biopsies using tissue-sparing specimen processing and microscaled proteomics. As a demonstration, we analyze core needle biopsies from ERBB2 positive breast cancers before and 48-72 h after initiating neoadjuvant trastuzumab-based chemotherapy. We show greater suppression of ERBB2 protein and both ERBB2 and mTOR target phosphosite levels in cases associated with pathological complete response, and identify potential causes of treatment resistance including the absence of ERBB2 amplification, insufficient ERBB2 activity for therapeutic sensitivity despite ERBB2 amplification, and candidate resistance mechanisms including androgen receptor signaling, mucin overexpression and an inactive immune microenvironment. The clinical utility and discovery potential of proteogenomics at biopsyscale warrants further investigation.

show abstract

“…Interestingly, antiandrogen treatment of ER + /AR + breast cancer cell lines reduces ER-mediated proliferation both in vitro and in xenograft models (115), again indicating a complex crosstalk between AR and ER signaling. Furthermore, AR/HER2 crosstalk has been reported: antiandrogen treatment suppresses HER2 phosphorylation and activation in vitro, and combined antiandrogen/anti-HER2 suppresses xenograft growth more than either treatment individually (116,117).…”

Section: Androgen Action In Womenmentioning

confidence: 99%