The BRCA1ness signature is associated significantly with response to PARP inhibitor treatment versus control in the I-SPY 2 randomized neoadjuvant setting

Publication date

2017-08-25

Authors

Severson, Tesa M
Wolf, Denise M.
Yau, Christina
Peeters, Justine K
Wehkam, Diederik
Schouten, Philip C
Chin, Suet-Feung
Majewski, Ian J
Michaut, Magali
Bosma, Astrid J

Editors

Advisors

Supervisors

Document Type

Article

Collections

Open Access logo

License

Abstract

Background: Patients with BRCA1-like tumors correlate with improved response to DNA double-strand break-inducing therapy. A gene expression-based classifier was developed to distinguish between BRCA1-like and non-BRCA1-like tumors. We hypothesized that these tumors may also be more sensitive to PARP inhibitors than standard treatments. Methods: A diagnostic gene expression signature (BRCA1ness) was developed using a centroid model with 128 triple-negative breast cancer samples from the EU FP7 RATHER project. This BRCA1ness signature was then tested in HER2-negative patients (n=116) from the I-SPY 2 TRIAL who received an oral PARP inhibitor veliparib in combination with carboplatin (V-C), or standard chemotherapy alone. We assessed the association between BRCA1ness and pathologic complete response in the V-C and control arms alone using Fisher's exact test, and the relative performance between arms (biomarker×treatment interaction, likelihood ratio p<0.05) using a logistic model and adjusting for hormone receptor status (HR). Results: We developed a gene expression signature to identify BRCA1-like status. In the I-SPY 2 neoadjuvant setting the BRCA1ness signature associated significantly with response to V-C (p=0.03), but not in the control arm (p=0.45). We identified a significant interaction between BRCA1ness and V-C (p=0.023) after correcting for HR. Conclusions: A genomic-based BRCA1-like signature was successfully translated to an expression-based signature (BRC1Aness). In the I-SPY 2 neoadjuvant setting, we determined that the BRCA1ness signature is capable of predicting benefit of V-C added to standard chemotherapy compared to standard chemotherapy alone. Trial registration: I-SPY 2 TRIAL beginning December 31, 2009: Neoadjuvant and Personalized Adaptive Novel Agents to Treat Breast Cancer (I-SPY 2), NCT01042379.

Keywords

BRCAness, Breast cancer, Neoadjuvant, PARP inhibition, Triple-negative breast cancer, Oncology, Cancer Research, Journal Article

Citation

Severson, T M, Wolf, D M, Yau, C, Peeters, J K, Wehkam, D, Schouten, P C, Chin, S-F, Majewski, I J, Michaut, M, Bosma, A J, Pereira, B, Bismeijer, T, Wessels, L F A, Caldas, C, Bernards, R, Simon, I M, Glas, A M, Linn, S & Van't Veer, L J 2017, 'The BRCA1ness signature is associated significantly with response to PARP inhibitor treatment versus control in the I-SPY 2 randomized neoadjuvant setting', Breast Cancer Research, vol. 19, no. 1, 99. https://doi.org/10.1186/s13058-017-0861-2