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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00246571
Other study ID # A6181077
Secondary ID
Status Completed
Phase Phase 2
First received October 27, 2005
Last updated July 2, 2012
Start date January 2006
Est. completion date June 2011

Study information

Verified date July 2012
Source Pfizer
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

The purpose of this study is to compare progression free survival for SU011248 [sutent (sunitinib malate)] versus standard of care therapy in patients with previously treated, advanced, triple receptor negative (ER, PR, HER2) locally recurrent or metastatic breast cancer.


Recruitment information / eligibility

Status Completed
Enrollment 217
Est. completion date June 2011
Est. primary completion date May 2010
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion Criteria:

- Recurrent or metastatic breast cancer

- Estrogen receptor (ER), progestin receptor (PR) and HER2/neu receptor (HER2) negative status

- Prior treatment with an anthracycline and a taxane in the adjuvant or advanced disease setting

- Relapse following adjuvant chemotherapy within 6 months of last treatment and/or received one or two chemotherapy regimens for advanced disease

Exclusion Criteria:

- More than two chemotherapy regimens for advanced disease

- Uncontrolled/symptomatic spread of cancer to the brain

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
SU011248
SU011248 capsules administered orally, daily in a continuous regimen, 3-week cycles, starting dose of 37.5 mg daily. 1-week treatment rests and dose reductions allowed for dose-limiting toxicity. Dose escalate SU011248 to 50-mg daily if minimal toxicities . Study will continue until disease progression. Patients randomized to or crossed over to SU011248 may continue beyond the time of Response Evaluation Criterion in Solid Tumors (RECIST) -defined progression at the discretion of the investigator in the case of clinical benefit.
Chemotherapy
The choice of chemotherapy will be at the discretion of the investigator within the limits outlined below. Capecitabine - 1000-1250 mg/m2 twice daily days 1-14 every 3 weeks Vinorelbine - 25-30 mg/m2 rapid intravenous infusion or 60-80 mg/m2 oral weekly, expressed in 3-week cycles Docetaxel - 75-100 mg/m2 every 3 weeks Paclitaxel - 175-200 mg/m2 every 3 weeks Paclitaxel - 80-90 mg/m2 weekly, in a continuous regimen expressed in 3-week cycles or administration of 3 weeks of treatment followed by 1 week of rest. Use of the 3/1 regimen will require extra care in scheduling disease assessments. Gemcitabine - 800-1250 mg/m2 Days 1 and 8 every 3 weeks Study will continue until disease progression or it is in the best interest of the patient to discontinue based on achievement of maximum benefit or tolerability issues. At the time of progression patients randomized to chemotherapy will be offered crossover to single agent SU011248.

Locations

Country Name City State
Bulgaria Pfizer Investigational Site Sofia
Bulgaria Pfizer Investigational Site Sofia
Bulgaria Pfizer Investigational Site Sofia
Bulgaria Pfizer Investigational Site Stara Zagora
Bulgaria Pfizer Investigational Site Varna
Canada Pfizer Investigational Site Edmonton Alberta
Canada Pfizer Investigational Site Toronto Ontario
Czech Republic Pfizer Investigational Site Brno Ceska Republika
Czech Republic Pfizer Investigational Site Brno
Czech Republic Pfizer Investigational Site Praha 8
Czech Republic Pfizer Investigational Site Praha 8 Ceska Republika
France Pfizer Investigational Site BESANCON cedex
France Pfizer Investigational Site BESANCON Cedex 5
France Pfizer Investigational Site NANTES cedex
France Pfizer Investigational Site Paris Cedex 20
Germany Pfizer Investigational Site Berlin
Hungary Pfizer Investigational Site Budapest
Hungary Pfizer Investigational Site Budapest
Italy Pfizer Investigational Site Aviano (PN)
Italy Pfizer Investigational Site Milano
Italy Pfizer Investigational Site Prato, FI
Spain Pfizer Investigational Site Barcelona
Spain Pfizer Investigational Site Gerona
Spain Pfizer Investigational Site Lleida
Spain Pfizer Investigational Site Malaga
Spain Pfizer Investigational Site Sevilla
Turkey Pfizer Investigational Site Adana Balcali
Turkey Pfizer Investigational Site Ankara Besevler
Turkey Pfizer Investigational Site Ankara Sihhiye
Turkey Pfizer Investigational Site Istanbul Pendik
Ukraine Pfizer Investigational Site Dnipropetrovsk
Ukraine Pfizer Investigational Site Kyiv
Ukraine Pfizer Investigational Site Odessa
United Kingdom Pfizer Investigational Site Edinburgh
United Kingdom Pfizer Investigational Site Oxfordshire
United Kingdom Pfizer Investigational Site Southampton
United States Pfizer Investigational Site Atlanta Georgia
United States Pfizer Investigational Site Atlanta Georgia
United States Pfizer Investigational Site Aurora Colorado
United States Pfizer Investigational Site Biloxi Mississippi
United States Pfizer Investigational Site Bloomfield Hills Michigan
United States Pfizer Investigational Site Boca Raton Florida
United States Pfizer Investigational Site Bronx New York
United States Pfizer Investigational Site Bronx New York
United States Pfizer Investigational Site Brownstown Michigan
United States Pfizer Investigational Site Clarkson Valley Missouri
United States Pfizer Investigational Site Clinton North Carolina
United States Pfizer Investigational Site Corona California
United States Pfizer Investigational Site Dallas Texas
United States Pfizer Investigational Site Dallas Texas
United States Pfizer Investigational Site Dearborn Michigan
United States Pfizer Investigational Site Decatur Georgia
United States Pfizer Investigational Site Del City Oklahoma
United States Pfizer Investigational Site Detroit Michigan
United States Pfizer Investigational Site Federal Way Washington
United States Pfizer Investigational Site Fort Worth Texas
United States Pfizer Investigational Site Fullerton California
United States Pfizer Investigational Site Gainesville Florida
United States Pfizer Investigational Site Glendora California
United States Pfizer Investigational Site Goldsboro North Carolina
United States Pfizer Investigational Site Greensburg Pennsylvania
United States Pfizer Investigational Site Hershey Pennsylvania
United States Pfizer Investigational Site Houston Texas
United States Pfizer Investigational Site Houston Texas
United States Pfizer Investigational Site Indianapolis Indiana
United States Pfizer Investigational Site Lakewood Washington
United States Pfizer Investigational Site Los Angeles California
United States Pfizer Investigational Site Los Angeles California
United States Pfizer Investigational Site Los Angeles California
United States Pfizer Investigational Site Macon Georgia
United States Pfizer Investigational Site Marietta Georgia
United States Pfizer Investigational Site Memphis Tennessee
United States Pfizer Investigational Site Memphis Tennessee
United States Pfizer Investigational Site Memphis Tennessee
United States Pfizer Investigational Site Midland Park New Jersey
United States Pfizer Investigational Site Mission Hills California
United States Pfizer Investigational Site Morristown New Jersey
United States Pfizer Investigational Site Northridge California
United States Pfizer Investigational Site Palm Springs California
United States Pfizer Investigational Site Paramus New Jersey
United States Pfizer Investigational Site Pasadena California
United States Pfizer Investigational Site Pittsburgh Pennsylvania
United States Pfizer Investigational Site Pittsburgh Pennsylvania
United States Pfizer Investigational Site Plano Texas
United States Pfizer Investigational Site Plano Texas
United States Pfizer Investigational Site Pomona California
United States Pfizer Investigational Site Pompton Plains New Jersey
United States Pfizer Investigational Site Puyallup Washington
United States Pfizer Investigational Site Rancho Cucamonga California
United States Pfizer Investigational Site Richardson Texas
United States Pfizer Investigational Site Ridgewood New Jersey
United States Pfizer Investigational Site San Antonio Texas
United States Pfizer Investigational Site San Antonio Texas
United States Pfizer Investigational Site San Antonio Texas
United States Pfizer Investigational Site San Antonio Texas
United States Pfizer Investigational Site San Atonio Texas
United States Pfizer Investigational Site Santa Monica California
United States Pfizer Investigational Site Seattle Washington
United States Pfizer Investigational Site Seattle Washington
United States Pfizer Investigational Site St. Louis Missouri
United States Pfizer Investigational Site St. Louis Missouri
United States Pfizer Investigational Site Summit New Jersey
United States Pfizer Investigational Site Tacoma Washington
United States Pfizer Investigational Site Tucker Georgia
United States Pfizer Investigational Site Tyler Texas
United States Pfizer Investigational Site Valencia California
United States Pfizer Investigational Site Washington District of Columbia
United States Pfizer Investigational Site West Bloomfield Michigan
United States Pfizer Investigational Site West Covina California
United States Pfizer Investigational Site Westwood New Jersey
United States Pfizer Investigational Site Wexford Pennsylvania
United States Pfizer Investigational Site Wilson North Carolina
United States Pfizer Investigational Site Zion Illinois

Sponsors (1)

Lead Sponsor Collaborator
Pfizer

Countries where clinical trial is conducted

United States,  Bulgaria,  Canada,  Czech Republic,  France,  Germany,  Hungary,  Italy,  Spain,  Turkey,  Ukraine,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Progression-Free Survival (PFS) Time in months from start of study treatment to first documentation of objective tumor progression (per RECIST) or death due to any cause. PFS was calculated as (first event date minus first randomization date plus 1) divided by 30.4. Tumor progression was determined from oncologic assessment data (where data meet the criteria for progressive disease [PD]), or from adverse event (AE) data (where the outcome was "Death"). Baseline, every 6 weeks until disease progression or death (up to 3 years from first dose) No
Secondary Proportion of Participants With Objective Response Objective response based assessment of confirmed response (CR) or confirmed partial response (PR) according to RECIST. CR are those that persist on repeat imaging study at least 4 weeks after initial documentation of response. PR are those with a greater than or equal to (=) 30% decrease in the sum of the longest dimensions (SLD) of the target lesions taking as a reference the baseline SLD. Baseline until response or disease progression (up to 3 years from first dose) No
Secondary Duration of Response (DR) Time in months from the first documentation of objective tumor response (CR or PR) to objective tumor progression or death. Duration of tumor response was calculated as (the date of the first documentation of objective tumor progression or death due to cancer minus the date of the first CR or PR that was subsequently confirmed plus 1) divided by 30.4. DR was calculated for the subgroup of participants with a confirmed objective tumor response. Time from first response to disease progression up to 3 years from first dose No
Secondary Survival Probability at 1 Year Probability that the participants will survive at end of 1 year from the first dose of study treatment. Calculated using data collected from baseline until death (up to 3 years after first dose of study medication). Probability calculated from Kaplan-Meier estimate. Baseline until death (up to 3 years after first dose of study medication) No
Secondary Overall Survival (OS) Time in months from the date of randomization to date of death due to any cause. OS was calculated as (date of death minus randomization date plus 1) divided by 30.4. Death was determined from adverse event data (where outcome was death) or from follow-up contact data (where the participant current status was death). Baseline until death (up to 3 years after first dose of study medication) No
Secondary Health Related Quality of Life (HRQoL) and Disease Related Symptoms as Measured by European Organization for Research and Treatment of Cancer (EORTC) Quality of Life (QoL) Questionnaire (EORTC-QLQ-C30) EORTC QLQ-C30: global health/QoL, functional domains (physical, role, cognitive, emotional, social), and symptom scales/items (fatigue, nausea and vomiting, pain, dyspnea, insomnia, appetite loss, constipation, diarrhea). Recall period: past week; response range: not at all to very much; global/QoL range: very poor to excellent. Scale score range: 0 to 100. Higher functional/global QoL score = better functioning and higher symptom score = greater degree of symptoms. Day 1, Cycle 1; Day 1, odd number cycles; and end of treatment (EOT)/withdrawal No
Secondary HRQoL and Disease Related Symptoms as Measured by EORTC-QLQ-C30 Breast Cancer Module (BR23) Score BR23: measured disease related symptoms of dry mouth, eye pain, hair loss, hot flushes, attractiveness, future health, sexual activity, arm/shoulder pain, breast pain, swollen breast, and skin problems on the breast. Recall period: past week; response range: not at all to very much. Scale score range: 0 to 100. Higher symptom score = greater degree of symptoms. Day 1, Cycle 1; Day 1, odd number cycles; and EOT/withdrawal No
Secondary Observed Plasma Trough Concentrations (Ctrough) of Sunitinib Predose Day 1, Cycles 1, 2, 3, 4, 5 and 7 and Day 15 of Cycles 1, 2, and 3 No
Secondary Ctrough of SU012662 (Metabolite of Sunitinib) Predose Day 1, Cycles 1, 2, 3, 4, 5 and 7 and Day 15 of Cycles 1, 2, and 3 No
Secondary Ctrough of Total Drug (Sunitinib + SU012662) Predose Day 1, Cycles 1, 2, 3, 4, 5 and 7 and Day 15 of Cycles 1, 2, and 3 No
Secondary Dose-corrected Ctrough of Sunitinib Ctrough = plasma concentration of sunitinib prior to study drug administration, dose corrected using the following formula Intended Dose/Actual Dose, where Actual Dose: the dose the participant received over the last 10 consecutive days and Intended Dose: the starting dose per study protocol. Predose Day 1, Cycles 1, 2, 3, 4, 5 and 7 and Day 15 of Cycles 1, 2, and 3 No
Secondary Dose-corrected Ctrough of SU012662 (Metabolite of Sunitinib) Ctrough = plasma concentration of SU012662 prior to study drug administration, dose corrected using the following formula Intended Dose/Actual Dose, where Actual Dose: the dose the participant received over the last 10 consecutive days and Intended Dose: the starting dose per study protocol. Predose Day 1, Cycles 1, 2, 3, 4, 5 and 7 and Day 15 of Cycles 1, 2, and 3 No
Secondary Dose-corrected Ctrough of Total Drug (Sunitinib + SU012662) Ctrough = plasma concentration of total drug (Sunitinib + SU012662) prior to study drug administration dose corrected using the following formula Intended Dose/Actual Dose, where Actual Dose: the dose the participant received over the last 10 consecutive days and Intended Dose: the starting dose per study protocol. Predose Day 1, Cycles 1, 2, 3, 4, 5 and 7 and Day 15 of Cycles 1, 2, and 3 No
Secondary Plasma Concentration of Soluble Vascular Endothelial Growth Factor Receptor 2 (sVEGFR2) Plasma concentrations of sVEGFR2 were examined as a potential pharmacodynamic marker Baseline (Cycle 1, Day 1), Day 1 (Cycles 2, 3, 4, 5, and 7), and EOT/withdrawal No
Secondary Plasma Concentration of Soluble Vascular Endothelial Growth Factor Receptor 3 (sVEGFR3) Plasma concentrations of sVEGFR3 were examined as a potential pharmacodynamic marker Baseline (Cycle 1, Day 1), Day 1 (Cycles 2, 3, 4, 5, and 7), and EOT/withdrawal No
Secondary Plasma Concentration of Soluble Vascular Endothelial Growth Factor A (sVEGF-A) Plasma concentrations of sVEGF-A were examined as a potential pharmacodynamic marker Baseline (Cycle 1, Day 1), Day 1 (Cycles 2, 3, 4, 5, and 7), and EOT/withdrawal No
Secondary Plasma Concentration of Soluble Placental Growth Factor (sPlGF) Plasma concentrations of sPlGF were examined as a potential pharmacodynamic marker Baseline (Cycle 1, Day 1), Day 1 (Cycles 2, 3, 4, 5 and 7), and EOT/withdrawal No
Secondary Plasma Concentration of Soluble Kinase Insert Domain for Tyrosine (sKIT), a Stem Cell Factor Receptor Plasma concentrations of sKIT were examined as a potential pharmacodynamic marker Baseline (Cycle 1, Day 1), Day 1 (Cycles 2, 3, 4, 5 and 7), and EOT/withdrawal No
Secondary Circulating Endothelial Cells (CEC) Blood samples were collected to enumerate the number of total CECs and sVEGFR1, sVEGFR2 and sVEGFR3 protein expression and/or cellular viability. Days 1 and 15 of Cycles 1, 2 and 3, Day 1 of Cycles 4 and 5, and every odd cycle thereafter, and EOT/withdrawal No
Secondary Circulating Tumor Cells (CTC) Blood samples were collected to enumerate the number of total CTCs and insulin growth factor 1R positive (IGF-1R+) CTCs Days 1 and 15 of Cycles 1, 2 and 3, Day 1 of Cycles 4 and 5, and every odd cycle thereafter, and EOT/withdrawal No
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