Abstract 462P
Background
Treatment of HER2- metastatic breast cancer (MBC) is driven by biomarker status (HR+ vs. triple negative [TNBC]). Single agent chemotherapy (ChT) is recommended for patients relapsing on targeted therapies including endocrine therapy or immunotherapies, with ChTs optimal sequence not yet established. The study objective was to compare the health outcomes (life years [LYs], quality adjusted LYs [QALYs]) in sequences starting ChT with eribulin (ERI), capecitabine (CAP) or treatment of physician choice (TPC), in second-line (2L) to fourth-line (4L) settings.
Methods
A stochastic microsimulation was developed tracking a MBC cohort through 2L-4L, with patients starting the next line of therapy due to progression or serious adverse events (SAEs) discontinuation. After each line, patients could receive another active therapy or best supportive care. Treatment sequences across three treatment pathways, capturing ChT initiation in 2L, 3L or 4L (the table), were based on clinical guidelines, real-world data and clinical interviews. Clinical inputs were stratified by biomarker and treatment line, with QALYs driven by progression status, response rates and SAEs. The analysis time horizon was 20 years, with outcomes discounted at 3.5%.
Results
In the HR+ subgroup, sequences with ERI used earlier than CAP/TPC led to higher LYs (1.62 - 2.24 vs. 1.57 - 2.22) and QALYs (0.75 -1.28 vs. 0.69 – 1.27), across the three pathways, driven by improved ERI efficacy and safety profile vs. CAP/TPC. Similarly, in the TNBC subgroup, earlier use of ERI vs. CAP/TPC led to higher LYs (1.19 - 1.64 vs. 1.16 - 1.63) and QALYs (0.55 - 0.86 vs. 0.49 - 0.85) when used in 2L or 4L, while 3L ERI vs. 3L TPC led to higher QALYs (0.70 vs. 0.67 - 0.68), but comparable LYs (1.40). The results were consistent across the sensitivity analyses conducted. Table: 462P
2L | 3L | 4L | 2L | 3L | 4L | |
Pathway | HR+ | TNBC | ||||
ChT post taxane/anthracycline in 1L or post adjuvant settings | CAP | TPC | ERI | CAP | TPC | ERI |
CAP | ERI | TPC | CAP | ERI | TPC | |
ERI | CAP | TPC | ERI | CAP | TPC | |
ERI | TPC | CAP | ERI | TPC | CAP | |
ChT post 2L taxane | PAC | CAP | TPC | PAC | CAP | TPC |
PAC | CAP | ERI | PAC | CAP | ERI | |
PAC | TPC | CAP | PAC | TPC | CAP | |
PAC | TPC | ERI | PAC | TPC | ERI | |
PAC | ERI | CAP | PAC | ERI | CAP | |
PAC | ERI | TPC | PAC | ERI | TPC | |
HR+: ChT post 2L CDK4/6 inhibitors and 3L taxane TNBC: ChT post 2L taxane and 3L SAC | FUL + PAL | PAC | CAP | PAC | SAC | ERI |
FUL + PAL | PAC | ERI | PAC | SAC | CAP | |
FUL + PAL | PAC | TPC | PAC | SAC | TPC |
CDK = cyclin-dependent kinase; FUL = fulvestrant; PAC = paclitaxel; PAL = palbociclib; SAC = sacituzumab. Note: TPC includes vinorelbine, gemcitabine, capecitabine, taxanes, anthracyclines and hormonal therapy.
Conclusions
Starting single agent ChT with ERI vs. CAP or TPC is associated with improved health outcomes for 2L-4L HER2- MBC management.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Eisai.
Disclosure
S. Rivolo: Other, Institutional, Research Funding, Simone Rivolo is employed by Evidera, a part of Thermo Fisher Scientific, which received consulting fees for research activities from Eisai.: Eisai. K. Ndirangu: Financial Interests, Institutional, Full or part-time Employment, Kerigo Ndirangu is an employee of Eisai Inc.: Eisai. D. Teloian: Other, Institutional, Research Funding, Diana Teloian is employed by Evidera, a part of Thermo Fisher Scientific, which received consulting fees for research activities from Eisai.: Eisai. A. Ambavane: Other, Institutional, Research Funding, Apoorva Ambavane is employed by Evidera, a part of Thermo Fisher Scientific, which received consulting fees for research activities from Eisai.: Eisai. C. Jackisch: Financial Interests, Personal, Invited Speaker: Roche, Exact Sciences, Gilead, Molecular Health; Financial Interests, Personal, Advisory Board: AstraZeneca, Novartis, Daiichi Sankyo, Pfizer. P.S. Hall: Financial Interests, Institutional, Research Funding: Lilly, Eisai, Novartis, Merk, Gilead, Sanofi, Roche, SeaGen.
Resources from the same session
1288P - Neoadjuvant therapy with anti-PD-1/PD-L1 plus platinum-base chemotherapy for resectable stage II-III non-small cell lung cancer: A systematic review and meta-analysis of randomized clinical trials
Presenter: Maria Dacoregio
Session: Poster session 04
1289TiP - LANTERN study: A multi-omics digital human avatar for integrating precision medicine into clinical practice for lung cancer patients
Presenter: Emilio Bria
Session: Poster session 04
1294P - A final analysis of a phase II study of durvalumab immediately after completion of chemoradiotherapy in unresectable stage III non–small-cell lung cancer: TORG1937 (DATE study)
Presenter: Tetsuro Kondo
Session: Poster session 04
1296P - Neoadjuvant camrelizumab and apatinib in patients with resectable non-small-cell lung cancer: One-year update from a phase II trial
Presenter: Wei Guo
Session: Poster session 04
1297P - An open-label, prospective phase II study of tislelizumab in combination with chidamide as consolidation therapy in locally advanced, unresectable, stage III NSCLC
Presenter: Yi Hu
Session: Poster session 04
1298P - Chemotherapy with concurrent proton vs. photon radiotherapy in stage III NSCLC: Effects on hematological toxicity and immune therapy
Presenter: Francesco Cortiula
Session: Poster session 04
1299P - The role of radiotherapy in extensive-stage small cell lung cancer after durvalumab-based immunochemotherapy: A retrospective study
Presenter: Lingjuan Chen
Session: Poster session 04
1300P - Treatment and clinical outcome in recurrent/refractory locally advanced NSCLC following chemoradiotherapy and consolidative durvalumab
Presenter: Georg Evers
Session: Poster session 04