An open-label, randomized phase II study of adecatumumab, a fully human anti-EpCAM antibody, as monotherapy in patients with metastatic breast cancer

doi:10.1093/annonc/mdp314

Annals of Oncology Advance Access published online on July 24, 2009
Annals of Oncology, doi:10.1093/annonc/mdp314

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© The Author 2009. Published by Oxford University Press on behalf of the European Society for Medical Oncology. All rights reserved. For permissions, please email: journals.permissions@oxfordjournals.org

An open-label, randomized phase II study of adecatumumab, a fully human anti-EpCAM antibody, as monotherapy in patients with metastatic breast cancer

M. Schmidt¹, M. E. Scheulen², C. Dittrich³^,4, P. Obrist⁵, N. Marschner⁶, L. Dirix⁷, M. Schmidt⁸, D. Rüttinger⁸, M. Schuler², C. Reinhardt⁸^,* and A. Awada⁹

¹ Department of Obstetrics and Gynecology, Johannes Gutenberg University, Mainz
² Department of Medicine (Cancer Research), West German Cancer Center, University Hospital Essen, Essen, Germany
³ Third Medical Department, Centre for Oncology and Hematology, CEADDP, Applied Cancer Research, Institution for Translational Research Vienna, Vienna
⁴ Ludwig Boltzmann-Institute for Applied Cancer Research, Vienna
⁵ Department of Pathology, St Vinzenz Hospital, Zams, Austria
⁶ Practice for Oncology and Hematology, Freiburg, Germany
⁷ Medical Oncology Unit, Oncologisch Centrum Sint-Augustinus, Antwerp, Belgium
⁸ Clinical Development, Micromet AG, Munich, Germany
⁹ Institut Jules Bordet, Unité Chemiothérapie, Université Libre de Bruxelles, Brussels, Belgium

^* Correspondence to: Dr C. Reinhardt, Staffelseestrasse 2, D-81477 Munich, Germany. Tel: +49-89-895277-301; Fax: +49-89-895277-205; E-mail: carsten.reinhardt{at}micromet.de

Background: High-level expression of epithelial cell adhesionmolecule (EpCAM) is associated with unfavorable prognosis inbreast cancer. This study was designed to investigate two dosesof the fully human IgG1 anti-EpCAM antibody adecatumumab (MT201)in patients with metastatic breast cancer (MBC).

Methods: A total of 109 patients were stratified into high-and low-level EpCAM expression by immunohistochemical stainingof primary tumors and subsequently randomly assigned to receivemonotherapy with either high- (6 mg/kg every two weeks (q2w))or low-dose adecatumumab (2 mg/kg/ q2w) until disease progression.

Results: No complete or partial tumor responses could be confirmedby central RECIST assessment. The probability for tumor progressionwas significantly lower in patients receiving high-dose adecatumumaband expressing high levels of EpCAM (hazard ratio 0.43; P =0.0057 versus low dose and low EpCAM). Three of 18 patientswith highest EpCAM expression treated with adecatumumab developednew metastases up to week 6, compared with 14 of 29 patientswith low EpCAM. Most frequent treatment-related adverse events(high dose/low dose) were chills (59%/20%), nausea (55%/18%),fatigue (39%/23%) and diarrhea (43%/7%).

Conclusions: Single-agent adecatumumab shows dose- and target-dependentclinical activity in EpCAM-positive MBC, albeit no objectivetumor regression. Further investigation of adecatumumab in patientswith EpCAM-overexpressing tumors and lower tumor burden is warranted.

adecatumumab, CD326, EpCAM, human mAb, metastatic breast cancer, MT201

Received for publication February 19, 2009. Revision received May 8, 2009. Accepted for publication May 11, 2009.

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