Abstract GS6-07: EMBRACA: A phase 3 trial comparing talazoparib, an oral PARP inhibitor, to physician's choice of therapy in patients with advanced breast cancer and a germline  <i>BRCA</i> mutation

Litton, Jennifer K.; Rugo, HS; Ettl, Johannes; Hurvitz, Sara A.; Gonçalvès, Anthony; Kh, Lee; Fehrenbacher, L.; Yerushalmi, Rinat; Mina, LA; Martín, M.; Roché, Henri; Im, Y-H.; Quek, R.G.W.; Tudor, IC; Hannah, A.; Eiermann, W.; Blum, JL

doi:10.1158/1538-7445.sabcs17-gs6-07

Cited by 47 publications

(47 citation statements)

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“…Both studies showed improvement of median PFS with the PARP inhibitor of ~ 3 months and greater tolerability, with no overall survival benefit evident as yet. Among patients with measurable disease, the objective response rates were approximately 60% with the PARP inhibitor compared to approximately 30% in physician choice (need to check talazaparib) [18,19]. The FDA approved olaparib for the treatment of germline BRCA1/2 metastatic breast cancer in January 2018.…”

Section: Germline Brca1 and Brca2 Mutation Status As A Hr Deficiency mentioning

confidence: 99%

Homologous recombination deficiency and host anti-tumor immunity in triple-negative breast cancer

Telli

Stover

Loi

et al. 2018

Breast Cancer Res Treat

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Purpose Triple-negative breast cancer (TNBC) is associated with worse outcomes relative to other breast cancer subtypes. Chemotherapy remains the standard-of-care systemic therapy for patients with localized or metastatic disease, with few biomarkers to guide benefit. Methods We will discuss recent advances in our understanding of two key biological processes in TNBC, homologous recombination (HR) DNA repair deficiency and host anti-tumor immunity, and their intersection. Results Recent advances in our understanding of homologous recombination (HR) deficiency, including FDA approval of PARP inhibitor olaparib for BRCA1 or BRCA2 mutation carriers, and host anti-tumor immunity in TNBC offer potential for new and biomarker-driven approaches to treat TNBC. Assays interrogating HR DNA repair capacity may guide treatment with agents inducing or targeting DNA damage repair. Tumor infiltrating lymphocytes (TILs) are associated with improved prognosis in TNBC and recent efforts to characterize infiltrating immune cell subsets and activate host anti-tumor immunity offer promise, yet challenges remain particularly in tumors lacking pre-existing immune infiltrates. Advances in these fields provide potential biomarkers to stratify patients with TNBC and guide therapy: induction of DNA damage in HR-deficient tumors and activation of existing or recruitment of host anti-tumor immune cells. Importantly, these advances provide an opportunity to guide use of existing therapies and development of novel therapies for TNBC. Efforts to combine therapies that exploit HR deficiency to enhance the activity of immune-directed therapies offer promise. Conclusions HR deficiency remains an important biomarker target and potentially effective adjunct to enhance immunogenicity of 'immune cold' TNBCs.

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Section: Germline Brca1 and Brca2 Mutation Status As A Hr Deficiency mentioning

confidence: 99%

Homologous recombination deficiency and host anti-tumor immunity in triple-negative breast cancer

Telli

Stover

Loi

et al. 2018

Breast Cancer Res Treat

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“…Several early phase studies with the other PARPis demonstrated similar signals of efficacy in BRCAmutant breast cancer ( Table 2). [29][30][31][32][33][34][35][36][37][38][39][40][41][42][43][44][45][46][47] Multiple phase 2 studies further demonstrated activity of olaparib in patients who had metastatic breast cancer with germline BRCA mutations. [30][31][32] In a phase 2 study, Tutt et al investigated the effects of olaparib monotherapy in 54 patients who had centrally confirmed, germline BRCA-mutant breast cancer.…”

Section: Single-agent Parpis In Metastatic Breast Cancermentioning

confidence: 99%

“…Recently, the activity of talazoparib in BRCA ‐mutant breast cancer was demonstrated in the phase 3 EMBRACA trial . Initial results from that trial demonstrated a median PFS of 8.6 months in patients who received talazoparib compared with 5.6 months in those who received chemotherapy ( P < .0001).…”

Section: Clinical Development In Breast Cancermentioning

confidence: 99%

“…Overall, patient-reported qualityof-life metrics (the European Organization for Research and Treatment of Cancer Core 30 Quality-of-Life Recently, the activity of talazoparib in BRCAmutant breast cancer was demonstrated in the phase 3 EMBRACA trial. 39 Initial results from that trial demonstrated a median PFS of 8.6 months in patients who received talazoparib compared with 5.6 months in those who received chemotherapy (P < .0001). In addition, the ORR in the talazoparib group was more than twice that of the control arm (62.6% vs 27.2% for chemotherapy; P < .0001).…”

Section: Single-agent Parpis In Metastatic Breast Cancermentioning

confidence: 99%

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PARP inhibitors in breast cancer: Bringing synthetic lethality to the bedside

Turk

Wisinski

2018

Cancer

112

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Individuals with breast and ovarian cancer susceptibility gene 1 (BRCA1) or BRCA2 germline mutations have a significantly increased lifetime risk for breast and ovarian cancers. BRCA-mutant cancer cells have abnormal homologous recombination (HR) repair of DNA. In these tumors, the base excision repair (BER) pathway is important for cell survival. The poly(adenosine diphosphate-ribose) polymerase (PARP) enzymes play a key role in BER, and PARP inhibitors are effective in causing cell death in BRCA-mutant cells while sparing normal cells-a concept called synthetic lethality. PARP inhibitors are the first cancer therapeutics designed to exploit synthetic lethality. Recent clinical trials in BRCA-mutant, metastatic breast cancer demonstrated improved outcomes with single-agent PARP inhibitors (olaparib and talazoparib) over chemotherapy. However, resistance to PARP inhibitors remains a challenge. Primarily due to myelosuppression, the combination of PARP inhibitors with chemotherapy has been difficult. Novel combinations with chemotherapy, immunotherapy, and other targeted therapies are being pursued. In this review, the authors discuss current knowledge of PARP inhibitors in BRCA-mutant breast cancer and potential future directions for these agents. Cancer 2018;124:2498-506. © 2018 American Cancer Society.

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“…Despite longer PFS and higher response rates, the median duration of response was only 5.4 months and OS, at an interim analysis after 51% of the projected events, was not significantly different between groups (hazard ratio, 0.76; P = .10). 13 Despite impressive responses and PFS benefit, development of resistance to PARPi was almost ubiquitous, hampering the duration of response and perhaps even OS. Furthermore, PFS benefit was in the range of 2-4 months with PARPi, even in germline BRCA-mutant patients.…”

Section: P Oly ( Adp -Ribos E) P Olymer a S E Inhib Itor S In B Re mentioning

confidence: 99%

Optimizing poly (ADP‐ribose) polymerase inhibition through combined epigenetic and immunotherapy

Prasanna

Khanna

et al. 2018

Cancer Science

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Triple‐negative breast cancer (TNBC) is an aggressive breast cancer subtype with poor survival outcomes. Currently, there are no targeted therapies available for TNBCs despite remarkable progress in targeted and immune‐directed therapies for other solid organ malignancies. Poly (ADP‐ribose) polymerase inhibitors (PARPi) are effective anticancer drugs that produce good initial clinical responses, especially in homologous recombination DNA repair‐deficient cancers. However, resistance is the rule rather than the exception, and recurrent tumors tend to have an aggressive phenotype associated with poor survival. Many efforts have been made to overcome PARPi resistance, mostly by targeting genes and effector proteins participating in homologous recombination that are overexpressed during PARPi therapy. Due to many known and unknown compensatory pathways, genes, and effector proteins, overlap and shared resistance are common. Overexpression of programmed cell death‐ligand 1 (PD‐L1) and cancer stem cell (CSC) sparing are novel PARPi resistance hypotheses. Although adding programmed cell death‐1 (PD‐1)/PD‐L1 inhibitors to PARPi might improve immunogenic cell death and be crucial for durable responses, they are less likely to target the CSC population that drives recurrent tumor growth. Lysine‐specific histone demethylase‐1A and histone deacetylase inhibitors have shown promising activity against CSCs. Combining epigenetic drugs such as lysine‐specific histone demethylase‐1A inhibitors or histone deacetylase inhibitors with PARPi/anti‐PD‐1/PD‐L1 is a novel, potentially synergistic strategy for priming tumors and overcoming resistance. Furthermore, such an approach could pave the way for the identification of new upstream epigenetic and genetic signatures.

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Abstract GS6-07: EMBRACA: A phase 3 trial comparing talazoparib, an oral PARP inhibitor, to physician's choice of therapy in patients with advanced breast cancer and a germline BRCA mutation

Cited by 47 publications

References 0 publications

Homologous recombination deficiency and host anti-tumor immunity in triple-negative breast cancer

Homologous recombination deficiency and host anti-tumor immunity in triple-negative breast cancer

PARP inhibitors in breast cancer: Bringing synthetic lethality to the bedside

Optimizing poly (ADP‐ribose) polymerase inhibition through combined epigenetic and immunotherapy

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