José Baselga1, Serafin M Morales2, Ahmad Awada3, Joanne L Blum4, Antoinette R Tan5,6, Marianne Ewertz7, Javier Cortes8, Beverly Moy9, Kathryn J Ruddy10, Tufia Haddad11, Eva M Ciruelos12, Peter Vuylsteke13, Scot Ebbinghaus14, Ellie Im14, Lamar Eaton14, Kumudu Pathiraja14, Christine Gause14, David Mauro14,15, Mary Beth Jones14, Hope S Rugo16. 1. Memorial Sloan Kettering Cancer Center, New York, NY, USA. 2. H. de Lleida Arnau de Vilanova, Lérida, Spain. 3. Institut Jules Bordet, Brussels, Belgium. 4. Baylor Sammons Cancer Center, Texas Oncology, US Oncology, Dallas, TX, USA. 5. Rutgers Cancer Institute of New Jersey, New Brunswick, NJ, USA. 6. Levine Cancer Institute, Carolinas HealthCare System, Charlotte, NC, USA. 7. Institute of Clinical Research, Odense University Hospital, University of Southern Denmark, Odense, Denmark. 8. Ramon y Cajal University Hospital, Madrid and Vall d´Hebron Institute of Oncology (VHIO), Barcelona, Spain. 9. Massachusetts General Hospital, Boston, MA, USA. 10. Mayo Clinic, Rochester, MN, USA. 11. University of Minnesota Masonic Clinical Cancer Center, Minneapolis, MN, USA. 12. Hospital 12 de Octubre, Madrid, Spain. 13. Clinique Sainte Elisabeth, Namur, Belgium. 14. Merck & Co., Inc., Kenilworth, NJ, USA. 15. Checkmate Pharmaceuticals, Cambridge, MA, USA. 16. UCSF Helen Diller Family Comprehensive Cancer Center, 1600 Divisadero St., San Francisco, CA, USA. Hope.Rugo@ucsf.edu.
Abstract
PURPOSE: Combining the mTOR inhibitor ridaforolimus and the anti-IGFR antibody dalotuzumab demonstrated antitumor activity, including partial responses, in estrogen receptor (ER)-positive advanced breast cancer, especially in high proliferation tumors (Ki67 > 15%). METHODS: This randomized, multicenter, international, phase II study enrolled postmenopausal women with advanced ER-positive breast cancer previously treated with anonsteroidal aromatase inhibitor (NCT01234857). Patients were randomized to either oral ridaforolimus 30 mg daily for 5 of 7 days (once daily [qd] × 5 days/week) plus intravenous dalotuzumab 10 mg/kg/week or oral exemestane 25 mg/day, and stratified by Ki67 status. Due to a high incidence of stomatitis in the ridaforolimus-dalotuzumab group, two sequential, nonrandomized, reduced-dose cohorts were explored with ridaforolimus 20 and 10 mg qd × 5 days/week. The primary endpoint was progression-free survival (PFS). RESULTS:Median PFS was 21.4 weeks for ridaforolimus 30 mg qd × 5 days/week plus dalotuzumab 10 mg/kg (n = 29) and 24.3 weeks for exemestane (n = 33; hazard ratio = 1.00; P = 0.5). Overall survival and objective response rates were similar between treatment arms. The incidence of drug-related, nonserious, and serious adverse events was higher with ridaforolimus/dalotuzumab (any ridaforolimus dose) than with exemestane. Lowering the ridaforolimus dose reduced the incidence of grade 3 stomatitis, but overall toxicity remained higher than acceptable at all doses without improved efficacy. CONCLUSIONS: The combination of ridaforolimus plus dalotuzumab was no more effective than exemestane in patients with advanced ER-positive breast cancer, and the incidence of adverse events was higher. Therefore, the combination is not being further pursued.
RCT Entities:
PURPOSE: Combining the mTOR inhibitor ridaforolimus and the anti-IGFR antibody dalotuzumab demonstrated antitumor activity, including partial responses, in estrogen receptor (ER)-positive advanced breast cancer, especially in high proliferation tumors (Ki67 > 15%). METHODS: This randomized, multicenter, international, phase II study enrolled postmenopausal women with advanced ER-positive breast cancer previously treated with a nonsteroidal aromatase inhibitor (NCT01234857). Patients were randomized to either oral ridaforolimus 30 mg daily for 5 of 7 days (once daily [qd] × 5 days/week) plus intravenous dalotuzumab 10 mg/kg/week or oral exemestane 25 mg/day, and stratified by Ki67 status. Due to a high incidence of stomatitis in the ridaforolimus-dalotuzumab group, two sequential, nonrandomized, reduced-dose cohorts were explored with ridaforolimus 20 and 10 mg qd × 5 days/week. The primary endpoint was progression-free survival (PFS). RESULTS: Median PFS was 21.4 weeks for ridaforolimus 30 mg qd × 5 days/week plus dalotuzumab 10 mg/kg (n = 29) and 24.3 weeks for exemestane (n = 33; hazard ratio = 1.00; P = 0.5). Overall survival and objective response rates were similar between treatment arms. The incidence of drug-related, nonserious, and serious adverse events was higher with ridaforolimus/dalotuzumab (any ridaforolimus dose) than with exemestane. Lowering the ridaforolimus dose reduced the incidence of grade 3 stomatitis, but overall toxicity remained higher than acceptable at all doses without improved efficacy. CONCLUSIONS: The combination of ridaforolimus plus dalotuzumab was no more effective than exemestane in patients with advanced ER-positive breast cancer, and the incidence of adverse events was higher. Therefore, the combination is not being further pursued.
Entities:
Keywords:
Breast cancer; Dalotuzumab; IGF1R; Ridaforolimus; mTOR
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