Annelot G J van Rossum1, Ingrid A M Mandjes2, Erik van Werkhoven3, Harm van Tinteren3, A Elise van Leeuwen-Stok4, Petra Nederlof5, Johanna E A Portielje6,7, Robbert J van Alphen8, Els Platte9, Daan van den Broek9, Alwin Huitema10, Marleen Kok11,12, Sabine C Linn1,12,13, Hendrika M Oosterkamp14. 1. Division of Molecular Pathology, Netherlands Cancer Institute, Amsterdam, The Netherlands. 2. Data Center, Netherlands Cancer Institute, Amsterdam, The Netherlands. 3. Biometrics Department, Netherlands Cancer Institute, Amsterdam, The Netherlands. 4. Dutch Breast Cancer Research Group, BOOG Study Center, Amsterdam, The Netherlands. 5. Department of Molecular Diagnostics, Netherlands Cancer Institute, Amsterdam, The Netherlands. 6. Department of Medical Oncology, HagaZiekenhuis, The Hague, The Netherlands. 7. Department of Medical Oncology, Leiden University Medical Center, Leiden, The Netherlands. 8. Department of Medical Oncology, Elisabeth-TweeSteden Hospital, Tilburg, The Netherlands. 9. Clinical Chemical Laboratory, Netherlands Cancer Institute, Amsterdam, The Netherlands. 10. Pharmacy, Netherlands Cancer Institute, Amsterdam, The Netherlands. 11. Division of Molecular Oncology and Immunology, Netherlands Cancer Institute, Amsterdam, The Netherlands. 12. Department of Medical Oncology, Netherlands Cancer Institute, Amsterdam, The Netherlands. 13. Department of Pathology, University Medical Center, Utrecht, The Netherlands. 14. Department of Medical Oncology, Haaglanden Medisch Centrum, The Hague, The Netherlands.
Abstract
BACKGROUND: The addition of bevacizumab to chemotherapy conferred a modest progression-free survival (PFS) benefit in metastatic triple-negative breast cancer (mTNBC). However, no overall survival (OS) benefit has been reported. Also, its combination with carboplatin-cyclophosphamide (CC) has never been investigated. METHODS: The Triple-B study is a multicenter, randomized phase IIb trial that aims to prospectively validate predictive biomarkers, including baseline plasma vascular endothelial growth factor receptor-2 (pVEGFR-2), for bevacizumab benefit. mTNBC patients were randomized between CC and paclitaxel (P) without or with bevacizumab (CC ± B or P ± B). Here we report on a preplanned safety and preliminary efficacy analysis after the first 12 patients had been treated with CC+B and on the predictive value of pVEGFR-2. RESULTS: In 58 patients, the median follow-up was 22.1 months. Toxicity was manageable and consistent with what was known for each agent separately. There was a trend toward a prolonged PFS with bevacizumab compared to chemotherapy only (7.0 vs. 5.2 months; adjusted HR = 0.60; 95% CI 0.33-1.08; p = 0.09), but there was no effect on OS. In this small study, pVEGFR-2 concentration did not predict a bevacizumab PFS benefit. Both the intention-to-treat analysis and the per-protocol analysis did not yield a significant treatment-by-biomarker test for interaction (pinteraction = 0.69). CONCLUSIONS: CC and CC+B are safe first-line regimens for mTNBC and the side effects are consistent with those known for each individual agent. pVEGFR-2 concentration did not predict a bevacizumab PFS benefit.
BACKGROUND: The addition of bevacizumab to chemotherapy conferred a modest progression-free survival (PFS) benefit in metastatic triple-negative breast cancer (mTNBC). However, no overall survival (OS) benefit has been reported. Also, its combination with carboplatin-cyclophosphamide (CC) has never been investigated. METHODS: The Triple-B study is a multicenter, randomized phase IIb trial that aims to prospectively validate predictive biomarkers, including baseline plasma vascular endothelial growth factor receptor-2 (pVEGFR-2), for bevacizumab benefit. mTNBC patients were randomized between CC and paclitaxel (P) without or with bevacizumab (CC ± B or P ± B). Here we report on a preplanned safety and preliminary efficacy analysis after the first 12 patients had been treated with CC+B and on the predictive value of pVEGFR-2. RESULTS: In 58 patients, the median follow-up was 22.1 months. Toxicity was manageable and consistent with what was known for each agent separately. There was a trend toward a prolonged PFS with bevacizumab compared to chemotherapy only (7.0 vs. 5.2 months; adjusted HR = 0.60; 95% CI 0.33-1.08; p = 0.09), but there was no effect on OS. In this small study, pVEGFR-2 concentration did not predict a bevacizumab PFS benefit. Both the intention-to-treat analysis and the per-protocol analysis did not yield a significant treatment-by-biomarker test for interaction (pinteraction = 0.69). CONCLUSIONS: CC and CC+B are safe first-line regimens for mTNBC and the side effects are consistent with those known for each individual agent. pVEGFR-2 concentration did not predict a bevacizumab PFS benefit.
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