Phase III randomised trial comparing intense dose-dense chemotherapy to tailored dose-dense chemotherapy in high-risk early breast cancer (GAIN-2)

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RESEARCH PRODUCT

Phase III randomised trial comparing intense dose-dense chemotherapy to tailored dose-dense chemotherapy in high-risk early breast cancer (GAIN-2)

Frederik Marmé Helmut Forstbauer Jens Huober Gbg Bruno Valentin Sinn Michael Untch Jenny Furlanetto Christian Jackisch Jens-uwe Blohmer Hans-joachim Lück Knut Engels Ago-b Grischa Wachsmann Ekkehart Ladda Nicole Burchardi Elmar Stickeler Sabine Schmatloch Sibylle Loibl Mattea Reinisch Theresa Link Volker Möbus Carsten Denkert Eva-maria Grischke Peter Klare Marcus Schmidt Christine Solbach Andreas Schneeweiss Julia Rey Wolfgang Janni

subject

Adult Cancer Research medicine.medical_specialty Time Factors Adolescent Paclitaxel Cyclophosphamide Dose-dense chemotherapy medicine.medical_treatment Breast Neoplasms Docetaxel Risk Assessment Disease-Free Survival Young Adult Risk Factors Albumins Germany Internal medicine Antineoplastic Combined Chemotherapy Protocols medicine Humans Prospective Studies Adverse effect Cyclophosphamide Aged Epirubicin Chemotherapy business.industry Carcinoma Ductal Breast Cancer Middle Aged Interim analysis medicine.disease Neoadjuvant Therapy Carcinoma Lobular Carcinoma Intraductal Noninfiltrating Oncology Docetaxel Chemotherapy Adjuvant Female business medicine.drug Epirubicin

description

Abstract Background The GAIN-2 trial was designed to identify a superior intense dose-dense (idd) strategy for high-risk patients with early breast cancer. Here, we report an interim analysis, at which the predefined futility boundary was crossed. Patients and methods GAIN-2 was an open-label, randomised, multicentre phase III trial. Two thousand eight hundred and eighty seven patients were randomised 1:1 between three courses each of idd epirubicin (E) 150 mg/m2, nab-paclitaxel (nP) 330 mg/m2 and cyclophosphamide (C) 2000 mg/m2 (iddEnPC) versus four cycles of leucocyte nadir-based tailored and dose-dense EC (dtEC) followed by four cycles of tailored and dose-dense docetaxel (dtD) (dtEC-dtD). Results The duration of median follow-up was 45.8 (range 0.0–88.3) months. Trial objectives included invasive disease-free survival (iDFS) as the primary end-point. A total of 593 patients received the treatment as neoadjuvant chemotherapy. At the time of futility interim analysis, 414 events for iDFS were reported. Overall, there was no difference in iDFS between iddEnPC and dtEC-dtD with 4-year iDFS rates of 84.3% (95% confidence interval (CI) 82.0–86.4%). Among all predefined subgroups, hormone receptor-positive and human epidermal growth factor receptor 2-negative (HR+/HER2-), lobular cancer and ≤50 years subgroups predicted for better iDFS in the dtEC-dtD arm. Overall, 88.1% of patients completed all treatment in both arms. Haematological toxicity grade 3/4 and grade 3/4 non-haematological adverse events were significantly higher with iddEnPC (iddEnPC 50.8% vs dtEC-dtD 45.1%, P = 0.002), especially arthralgia and peripheral sensory neuropathy. Two treatment-related deaths occurred during dtEC-dtD, corresponding to a low mortality rate of 0.07%. Conclusions iDFS is equal in both regimens, but tailoring dose-dense chemotherapy improved outcomes in HR+/HER2-, lobular cancer and patients ≤50 years.

year	journal	country	edition	language
2021-10-01	European Journal of Cancer

https://doi.org/10.1016/j.ejca.2021.07.033