DNA Repair Deficiency Biomarkers and the 70-gene Ultra-high Risk Signature As Predictors of Veliparib/carboplatin Response in the I-SPY 2 Breast Cancer Trial

Overview

Journal NPJ Breast Cancer

Date 2017 Sep 27

PMID 28948212

Citations 48

Authors

Denise M Wolf

Christina Yau

Ashish Sanil

Annuska Glas

Emanuel Petricoin

Julia Wulfkuhle

Tesa M Severson

Sabine Linn

Lamorna Brown-Swigart

Gillian Hirst

Meredith Buxton

Angela DeMichele

Nola Hylton

Fraser Symmans

Doug Yee

Melissa Paoloni

Laura Esserman

Don Berry

Hope Rugo

Olufunmilayo Olopade

Laura van t Veer

Affiliations

Soon will be listed here.

Abstract

Veliparib combined with carboplatin (VC) was an experimental regimen evaluated in the biomarker-rich neoadjuvant I-SPY 2 trial for breast cancer. VC showed improved efficacy in the triple negative signature. However, not all triple negative patients achieved pathologic complete response and some HR+HER2- patients responded. Pre-specified analysis of five DNA repair deficiency biomarkers (BRCA1/2 germline mutation; PARPi-7, ness, and CIN70 expression signatures; and PARP1 protein) was performed on 116 HER2- patients (VC: 72 and concurrent controls: 44). We also evaluated the 70-gene ultra-high risk signature (MP1/2), one of the biomarkers used to define subtype in the trial. We used logistic modeling to assess biomarker performance. Successful biomarkers were combined using a simple voting scheme to refine the 'predicted sensitive' group and Bayesian modeling used to estimate the pathologic complete response rates. BRCA1/2 germline mutation status associated with VC response, but its low prevalence precluded further evaluation. PARPi-7, ness, and MP1/2 specifically associated with response in the VC arm but not the control arm. Neither CIN70 nor PARP1 protein specifically predicted VC response. When we combined the PARPi-7 and MP1/2 classifications, the 42% of triple negative patients who were PARPi7-high and MP2 had an estimated pCR rate of 75% in the VC arm. Only 11% of HR+/HER2- patients were PARPi7-high and MP2; but these patients were also more responsive to VC with estimated pathologic complete response rates of 41%. PARPi-7, ness and MP1/2 signatures may help refine predictions of VC response, thereby improving patient care.

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