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Abemaciclib as initial therapy for advanced breast cancer: MONARCH 3 updated results in prognostic subgroups
被引:0
|作者:
Stephen Johnston
Joyce O’Shaughnessy
Miguel Martin
Jens Huober
Masakazu Toi
Joohyuk Sohn
Valérie A. M. André
Holly R. Martin
Molly C. Hardebeck
Matthew P. Goetz
机构:
[1] The Royal Marsden NHS Foundation Trust,Breast Unit
[2] Texas Oncology,Baylor University Medical Center
[3] US Oncology,Medical Oncology Service, Hospital General Universitario Gregorio Marañón
[4] Universidad Complutense,Breast Cancer Unit, Kyoto University Hospital
[5] University of Ulm,Department of Oncology
[6] Kyoto University,undefined
[7] Yonsei Cancer Center,undefined
[8] Eli Lilly and Company,undefined
[9] Eli Lilly and Company,undefined
[10] Mayo Clinic,undefined
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摘要:
In MONARCH 3, continuous dosing of abemaciclib with an aromatase inhibitor (AI) conferred significant clinical benefit to postmenopausal women with HR+, HER2− advanced breast cancer. We report data for clinically prognostic subgroups: liver metastases, progesterone receptor status, tumor grade, bone-only disease, ECOG performance status, and treatment-free interval (TFI) from an additional 12-month follow-up (after final progression-free survival [PFS] readout). In the intent-to-treat population, after median follow-up of approximately 39 months, the updated PFS was 28.2 versus 14.8 months (hazard ratio [HR], 0.525; 95% confidence interval, 0.415–0.665) in abemaciclib versus placebo arms, respectively. Time to chemotherapy (HR, 0.513), time to second disease progression (HR, 0.637), and duration of response (HR, 0.466) were also statistically significantly prolonged with the addition of abemaciclib to AI. Treatment benefit was observed across all subgroups, as evidenced by objective response rate change from the addition of abemaciclib to AI, with the largest effects observed in patients with liver metastases, progesterone receptor-negative tumors, high-grade tumors, or TFI < 36 months. Extended follow-up in the MONARCH 3 trial further confirmed that the addition of abemaciclib to AI conferred significant treatment benefit to all subgroups, including those with poorer prognosis.
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