Abstract 435P
Background
PARP inhibitors (PARPis) induce STING-cGAS activation and increase tumor mutational load in TNBC preclinical models, making TNBC sensitive to immune checkpoint blockade. The MEDIOLA phase II study demonstrated a 63.3% overall response rate (ORR) defined as CR+PR with D+O in PARPi naïve gBRCAm BC (1 median number of prior therapies [range 0-4]). We evaluated D+O activity in heavily pretreated TNBC.
Methods
Key eligibility criteria include metastatic TNBC, adequate performance status and organ function. Patients (pts) with prior use of D or PARPi, and active CNS or leptomeningeal disease were not eligible. No limit on the number of prior systemic therapies. For germline BRCA wild type (gBRCAwt), Simon’s 2-stage design with a target of 30% ORR with α=0.1 and β=0.1 was used. If ≥ 2 responses in the first stage (16 pts), 9 additional pts were planned to enroll. 5 ≥ of 25 responses warrant a further later stage study. For gBRCAm, a pilot single stage design was used with a stopping rule. If 1≥ response in the first 5 pts, another 5 pts were planned to enroll. RP2D determined in our earlier phase I study; D 1500 mg iv q4w and O 300 mg BID po (28-day cycle) was administered until PD or intolerable toxicity. The primary endpoint was ORR by RECIST v1.1 (CT q2mo). Secondary objectives were safety by CTCAE v4.03, clinical benefit rate (CBR) defined by CR+PR+SD≥4mo, and PFS.
Results
14 of 15 pts were RECIST evaluable (11 gBRCAwt and 3 gBRCAm). The median number of prior therapies are 3 (range 0-9). A majority of pts (78.6%; 11/14) had ≥ 3 prior systemic therapies and 64.3% (9/14) had previous platinum. Of note, 4 pts had either HR+/HER2-BC (n=3) or HR+/HER2+BC (n=1) at diagnosis which converted to TNBC at recurrence. ORR was 28.5% (3/3 gBRCAm [3 PR] and 1/11 gBRCAwt [PR for 10.3 mo]). One pt with gBRCAm remains on the study with PR >4 yr (96% reduction at best). CBR was 42.9% (3/3 gBRCAm and 3/11 gBRCAwt). Median PFS was 3.7 mo (IQR 1.9-10.3). There were no new safety signals. Accrual is ongoing.
Conclusions
D+O exhibited modest clinical activity in heavily pretreated TNBC pts with or without gBRCAm. Comprehensive biomarker and pharmacodynamic studies are ongoing for the exceptional responder with gBRCAm.
Clinical trial identification
NCT02484404 Release date: June 29, 2015.
Editorial acknowledgement
No editorial assistance
Legal entity responsible for the study
J-M. Lee.
Funding
Intramural Research Program of the NCI, CCR (grant number: #ZIA BC011525; to J-M. Lee) Durvalumab and olaparib were supplied to the CCR, NCI under a Cooperative Research and Development Agreement between the CCR/NCI and AstraZeneca. Research funding was also provided by AstraZeneca to the institution.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
359P - Unveiling the factors influencing exercise engagement in breast cancer patients: Insights from the early recovery phase
Presenter: Sujin Yeon
Session: Poster session 03
360P - Neoadjuvant inetetamab combined with pertuzumab, paclitaxel and carboplatin for locally advanced HER2-positive breast cancer: Primary analysis of a phase II study
Presenter: Yue Chai
Session: Poster session 03
361P - A phase II study of fulvestrant combined with chemotherapy in the neoadjuvant treatment of HR+/HER2- locally advanced breast cancer
Presenter: Jing Wu
Session: Poster session 03
362P - CYBERNEO trial: Update of results at 14 years of follow-up
Presenter: Syrine Ben Dhia
Session: Poster session 03
363P - High adipocytokines and IL-18bp serum levels are associated with lower objective response rate after neoadjuvant treatment in breast cancer patients with metabolic syndrome
Presenter: Larissa Mont'Alverne Arruda
Session: Poster session 03
365P - Effectiveness and safety of human type 5 recombinant adenovirus (H101) in malignant tumor with malignant pleural effusion and ascites: A multicenter, observational, real-world study
Presenter: Baocheng Wang
Session: Poster session 03
366P - Artificial intelligence (AI)-powered assessment of complete and intense human epidermal growth factor receptor 2 (HER2)-positive tumor cell proportion in breast cancer: Predicting fluorescence in situ hybridization (FISH) positivity and response to HER2-targeted therapy
Presenter: Minsun Jung
Session: Poster session 03
367P - Sentinel lymph node biopsy (SLNB) in patients with locally advanced breast cancer (LABC): Descriptive, inferential and survival analysis
Presenter: Johanna Espejo Niño
Session: Poster session 03
368P - Impact of PET-CT-determined sarcopenia on survival and pathological complete response in breast cancer patients with neoadjuvant chemotherapy
Presenter: Gözde Tahtaci
Session: Poster session 03
369P - The impact of germline BRCA mutations in locally advanced, triple-negative breast cancer (TNBC) treated with platinum- based neoadjuvant chemotherapy
Presenter: Hadar Goldvaser
Session: Poster session 03