Breast Cancer Clinical Trial
Phase 2 Study of AMG 386 Plus Paclitaxel With or Without Bevacizumab as First Line Therapy in Her2-Negative Breast Cancer Patients
Summary
This is a phase 2, randomized, placebo controlled, multi-center study to estimate the treatment effect and evaluate the safety and tolerability of AMG 386 in combination with paclitaxel and paclitaxel/bevacizumab in the treatment of subjects with Her2-negative metastatic or locally recurrent breast cancer.
AMG 386 is a man-made medication that is designed to stop the development of blood vessels in cancer tissues. Cancer tissues rely on the development of new blood vessels, a process called angiogenesis, to obtain a supply of oxygen and nutrients to grow.
Full Description
Primary Objective: To estimate the treatment effect as measured by progression free survival (PFS) of subjects receiving AMG 386 (at 2 doses) in combination with paclitaxel + bevacizumab relative to paclitaxel + bevacizumab + placebo.
Secondary Objective(s):
To compare the treatment effect as measured by PFS of subjects receiving open-label AMG 386 in combination with paclitaxel relative to paclitaxel + bevacizumab + placebo
To compare the treatment effect as measured by PFS of subjects receiving AMG 386 in combination with paclitaxel and bevacizumab relative to paclitaxel + AMG 386
To evaluate the safety and tolerability of the combination and non-bevacizumab regimens
To estimate other measures (RR, DOR, TTR, TTP) of treatment effect
To evaluate the pharmacokinetics (PK) of AMG 386 and bevacizumab when used in combination
To estimate the incidence of anti-AMG386 antibody formation
Exploratory Objective(s):
To explore the pharmacodynamic (PD) response as assessed by changes in blood levels of angiogenic cytokines, tumor apoptosis, and other markers
To explore the association of histological features and selected immunologic, biochemical, pharmacogenetic, or angiogenic markers in tumor biopsies, plasma, or serum samples with safety and/or efficacy outcomes
Study Design:
This is a phase 2, randomized, placebo controlled, multi-center study to estimate the treatment effect and evaluate the safety and tolerability of AMG 386 in combination with paclitaxel and paclitaxel/bevacizumab in the treatment of subjects with Her2-negative metastatic or locally recurrent breast cancer.
Two hundred twenty subjects will be randomized 1:1:1:1 to each of the following arms:
Arm A: Paclitaxel 90 mg/m² IV QW (3 on/1 off) + bevacizumab 10 mg/kg IV Q2W + AMG 386 10 mg/kg IV QW Arm B: Paclitaxel 90 mg/m² IV QW (3 on/1 off) + bevacizumab 10 mg/kg IV Q2W + AMG 386 3 mg/kg IV QW Arm C: Paclitaxel 90 mg/m² IV QW (3 on/1 off) + bevacizumab 10 mg/kg IV Q2W + AMG 386 placebo IV QW Arm D: Paclitaxel 90 mg/m² IV QW (3 on/1 off) + Open Label AMG 386 10 mg/kg IV QW To maintain the double-blind in arms A, B, and C, each subject will be infused weekly with a volume of investigational product equivalent to 10 mg/kg AMG 386 IV. Arm D will receive open label AMG 386 and will not receive a placebo for bevacizumab.
Subjects will be discontinued from study treatment at any time for radiographic disease progression, clinical progression, unacceptable toxicity, subject withdrawal of consent, or death.
Subjects alive at the time of discontinuation of all study medications will be followed for up to 48 months from the date of the last subject enrolled into the trial to evaluate overall survival.
Radiological imaging to assess disease status will be performed every 8 weeks ± 7 days (2 cycles) for 2 years and then every 4 months ± 1 month thereafter during the study until subjects develop radiographic disease progression per the modified RECIST criteria. In addition, any subject who discontinues study drug treatment prior to disease progression will continue to have radiological imaging performed every 8 weeks ± 7 days during the long term follow up period if the subject has not been in the study for 2 years until the subject develops radiographic disease progression or begins a new treatment. If the subject has been on study for 2 years, radiological imaging every 4 months ± 1 month will be performed during long term follow-up period until the subject develops radiographic disease progression or begins a new treatment.
The overall study design is described by a study schema immediately following this synopsis. Amgen Global Safety (AGS) will charter a data review team (DRT) that is independent of the team conducting the study and will review unblinded safety data after 20, 40, and 80 subjects have been randomized and have had the opportunity to receive at least 1 cycle (4 weeks) of study treatment.
Eligibility Criteria
Inclusion Criteria:
Subjects must have histologically or cytologically confirmed adenocarcinoma of the breast with locally recurrent or metastatic disease. Locally recurrent disease must not be amenable to resection with curative intent.
Measurable or non-measurable disease per modified RECIST guidelines
ECOG of 0 or 1 (within 14 days prior to randomization)
Adequate organ and hematological function as evidenced by the following laboratory studies within 14 days prior to randomization:
• Cardiac function, as follows:
Normal sinus rhythm (no significant ECG changes)
Left ventricular ejection fraction ≥ LLN, as determined by echocardiogram or MUGA scan, according to institutional standards within 28 days prior to randomization
Exclusion Criteria:
Inflammatory Breast Cancer
Common Terminology Criteria for Adverse Events (CTCAE) Version 3.0 peripheral neuropathy > grade 1 at randomization
History of arterial or venous thrombosis, including transient ischemic attack (TIA), within 1 year prior to randomization
Adjuvant or neoadjuvant taxane treatment within 12 months of randomization. Any other adjuvant chemotherapy regimen must be discontinued at least 21 days prior to randomization
Prior chemotherapy, vaccine, or biological therapy for locally recurrent or metastatic breast cancer (prior endocrine therapy is permitted)
Prior radiation therapy, radiofrequency ablation, percutaneous cryotherapy or hepatic chemoembolization on all sites of disease unless disease progression was subsequently documented 14 days prior to randomization.
Overexpression of HER-2 (gene amplification by FISH or 3+ over expression by immunohistochemistry).
Current or prior history of central nervous system metastasis
History of bleeding diathesis or clinically significant bleeding within 6 months prior to randomization
Major surgical procedure within 28 days prior to randomization
Open breast biopsy within 14 days prior to randomization
Minor surgical procedure, placement of access device, or fine needle aspiration within 7 days of first dose
Prior malignancy (other than thyroid cancer, in situ cervical cancer, or basal cell cancer of the skin, treated with curative intent and without evidence of disease for ≥ 3 years prior to randomization)
Clinically significant cardiac disease within 12 months prior to randomization, including myocardial infarction, unstable angina, grade 2 or greater peripheral vascular disease, cerebrovascular accident, transient ischemic attack, congestive heart failure, or arrhythmias not controlled by outpatient medication
Non-healing wound, ulcer or fracture
Known hypersensitivity to paclitaxel or drugs using the vehicle cremophor
Known hypersensitivity to bacterial proteins, or any of the drugs required in this study
Known positive test for human immunodeficiency virus (HIV), hepatitis C, or hepatitis B surface antigen
Known active or chronic hepatitis
Uncontrolled hypertension as defined as systolic blood pressure ≥ 150 mm Hg and diastolic blood pressure ≥ 90 mm Hg. Anti-hypertensive medications are allowed if the subject is stable on their current dose at the time of randomization
Currently or previously treated with any VEGF or VEGFr inhibitor, including but not limited to, bevacizumab, SU11248 (sunitinib), PTK787 (vatalinib), AZD 2171, AEE-788, BAY 43-9006 (sorafenib) and AMG 706.
Treatment with coumarin-type anticoagulants, (other than low dose prophylaxis for central venous catheters ≤ 1mg/day) within 7 days prior to randomization
Currently or previously treated with angiopoietin inhibitors, or inhibitors of TIE-1 or TIE-2 including, but not limited to, AMG 386, XL880, XL820
Treatment with immune modulators such as cyclosporine and tacrolimus within 30 days prior to randomization
Concomitant therapy with any hormonal agent such as raloxifene, tamoxifen, or other selective estrogen receptor modulators (SERMS), given for breast cancer prevention or for osteoporosis. Subjects must have discontinued these agents 28 days prior to randomization
Pregnant (ie, positive beta-human chorionic gonadotropin test) or is breast feeding
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There are 76 Locations for this study
Litchfield Park Arizona, 85340, United States
Tucson Arizona, 85724, United States
Hot Springs Arkansas, 71913, United States
Little Rock Arkansas, 72205, United States
Campbell California, 95008, United States
Los Angeles California, 90095, United States
Murrieta California, 92562, United States
Santa Maria California, 93454, United States
New Haven Connecticut, 06520, United States
Stamford Connecticut, 06902, United States
Orlando Florida, 32804, United States
Robbinsdale Minnesota, 55422, United States
Henderson Nevada, 89052, United States
Lebanon New Hampshire, 03756, United States
Nashua New Hampshire, 03061, United States
Edison New Jersey, 08820, United States
Mountain Lakes New Jersey, 07046, United States
Asheville North Carolina, 28806, United States
Charlotte North Carolina, 28203, United States
Hershey Pennsylvania, 17033, United States
Philadelphia Pennsylvania, 19106, United States
Columbia South Carolina, 29210, United States
Richardson Texas, 75080, United States
San Antonio Texas, 78229, United States
Sugar Land Texas, 77479, United States
Ogden Utah, 84403, United States
Kurralta Park South Australia, 5037, Australia
Epping Victoria, 3076, Australia
Fitzroy Victoria, 3065, Australia
Footscray Victoria, 3011, Australia
Malvern Victoria, 3144, Australia
Perth Western Australia, 6000, Australia
Innsbruck , 6020, Austria
Wels , 4600, Austria
Wien , 1090, Austria
Leuven , 3000, Belgium
Liege , 4000, Belgium
Wilrijk , 2610, Belgium
Herlev , 2730, Denmark
Helsinki , 00029, Finland
La Roche Sur Yon Cedex 9 , 85925, France
Lyon , 69008, France
Marseille , 13009, France
Montpellier Cedex 5 , 34298, France
Paris Cedex 20 , 75020, France
Paris Cedex 5 , 75248, France
Toulouse Cedex , 31052, France
Vandoeuvre les Nancy , 54511, France
Gyula , 5700, Hungary
Kaposvar , 7400, Hungary
Szombathely , 9700, Hungary
Veszprem , 8200, Hungary
Bangalore Karnataka, 560 0, India
Miraj Maharashtra, 416 4, India
Mumbai Maharashtra, 400 0, India
Nagpur Maharashtra, 440 0, India
Pune Maharashtra, 411 0, India
Jaipur Rajasthan, 302 0, India
Jaipur Rajasthan, 302 0, India
Maastricht , 6229 , Netherlands
Gdansk , 80-95, Poland
Lubin , 59-30, Poland
Poznan , 61-48, Poland
Warszawa , 02-78, Poland
Warszawa , 04-14, Poland
Wroclaw , 53-41, Poland
Jaén AndalucÃ-a, 23007, Spain
Sabadell Cataluña, 08208, Spain
Santiago de Compostela Galicia, 15706, Spain
Madrid , 28033, Spain
Guildford , GU2 7, United Kingdom
Leicester , LE1 5, United Kingdom
London , NW1 2, United Kingdom
London , W6 8R, United Kingdom
Manchester , M20 4, United Kingdom
Northwood , HA6 2, United Kingdom
Nottingham , NG5 1, United Kingdom
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