TBCRC 048: Phase II Study of Olaparib for Metastatic Breast Cancer and Mutations in Homologous Recombination-Related Genes

Ballinger, T.J.; Brufsky, A.; Carey, L.A.; D&apos; DeMeo, M.; Domchek, S.; Garber, J.E.; Hughes, M.E.; Jenkins, C.; Krop, I.E.; Lin, N.U.; Marcom, P.K.; Melisko, M.; Nanda, R.; Robson, M.E.; Santa-Maria, C.A.; Shah, P.D.; Tung, N.M.; Ventz, S.; Vinayak, S.; Wagle, N.; Winer, E.P.; Wolff, A.C.; Wulf, G.M.; Yang, E.S.

TBCRC 048: Phase II Study of Olaparib for Metastatic Breast Cancer and Mutations in Homologous Recombination-Related Genes

Authors: T.J. Ballinger
A. Brufsky
L.A. Carey
D&apos
M. DeMeo
S. Domchek
J.E. Garber
M.E. Hughes
C. Jenkins
I.E. Krop
N.U. Lin
P.K. Marcom
M. Melisko
R. Nanda
M.E. Robson
C.A. Santa-Maria
P.D. Shah
N.M. Tung
S. Ventz
S. Vinayak
N. Wagle
E.P. Winer
A.C. Wolff
G.M. Wulf
E.S. Yang
Publication date: 1 January 2020
Publisher: American Society of Clinical Oncology
Doi

Abstract

PURPOSE Olaparib, a poly (ADP-ribose) polymerase (PARP) inhibitor (PARPi), is approved for the treatment of human epidermal growth factor receptor 2 (HER2)–negative metastatic breast cancer (MBC) in germline (g)BRCA1/2 mutation carriers. Olaparib Expanded, an investigator-initiated, phase II study, assessed olaparib response in patients with MBC with somatic (s)BRCA1/2 mutations or g/s mutations in homologous recombination (HR)–related genes other than BRCA1/2. METHODS Eligible patients had MBC with measurable disease and germline mutations in non-BRCA1/2 HR-related genes (cohort 1) or somatic mutations in these genes or BRCA1/2 (cohort 2). Prior PARPi, platinum-refractory disease, or progression on more than two chemotherapy regimens (metastatic setting) was not allowed. Patients received olaparib 300 mg orally twice a day until progression. A single-arm, two-stage design was used. The primary endpoint was objective response rate (ORR); the null hypothesis (# 5% ORR) would be rejected within each cohort if there were four or more responses in 27 patients. Secondary endpoints included clinical benefit rate and progression-free survival (PFS). RESULTS Fifty-four patients enrolled. Seventy-six percent had estrogen receptor–positive HER2-negative disease. Eighty-seven percent had mutations in PALB2, sBRCA1/2, ATM, or CHEK2. In cohort 1, ORR was 33% (90% CI, 19% to 51%) and in cohort 2, 31% (90% CI, 15% to 49%). Confirmed responses were seen only with gPALB2 (ORR, 82%) and sBRCA1/2 (ORR, 50%) mutations. Median PFS was 13.3 months (90% CI, 12 months to not available/computable [NA]) for gPALB2 and 6.3 months (90% CI, 4.4 months to NA) for sBRCA1/ 2 mutation carriers. No responses were observed with ATM or CHEK2 mutations alone. CONCLUSION PARP inhibition is an effective treatment for patients with MBC and gPALB2 or sBRCA1/2 mutations, significantly expanding the population of patients with breast cancer likely to benefit from PARPi beyond gBRCA1/2 mutation carriers. These results emphasize the value of molecular characterization for treatment decisions in MBC

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