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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00879086
Other study ID # E7389-G000-209
Secondary ID
Status Completed
Phase Phase 2
First received
Last updated
Start date March 31, 2009
Est. completion date April 30, 2014

Study information

Verified date October 2021
Source Eisai Inc.
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study in patients with advanced breast cancer is to compare the incidence and severity of neuropathy adverse events for the two treatment groups (eribulin versus ixabepilone) using National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE version 3.0) grading.


Recruitment information / eligibility

Status Completed
Enrollment 104
Est. completion date April 30, 2014
Est. primary completion date April 30, 2013
Accepts healthy volunteers No
Gender Female
Age group 18 Years and older
Eligibility Inclusion criteria: 1. Female subjects with confirmed locally recurrent or metastatic carcinoma of the breast who have received prior taxane therapy and at least one prior cytotoxic chemotherapy regimen for advanced disease. Exclusion criteria: 1. Subjects who have received prior ixabepilone therapy. 2. Subjects with prior participation in an eribulin clinical study, even if not assigned to eribulin treatment. 3. Subjects with pre-existing neuropathy Grade greater than or equal to 2. 4. Subjects with a history of diabetes mellitus Type 1 or 2. 5. Subjects with bilateral mastectomy which included bilateral axillary lymph node dissection. 6. Subjects with missing digits required for vibration assessment. 7. Subjects with any other concurrent diseases or conditions that would be expected to interfere with neuropathy assessments, which may include vitamin deficiency, sequelae of cerebrovascular disease, thyroid insufficiency, lumbar or cervical radiculopathy, or alcoholic or inflammatory neuropathy.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Eribulin Mesylate
E7389 (eribulin mesylate) given at a dose of 1.4 mg/m^2 as a 2 to 5 minute intravenous (IV) bolus on Days 1 and 8 of a 21-day cycle. The Treatment Phase will include six cycles. Patients may enter the Extension Phase for additional cycles following the sixth cycle of treatment.
Ixabepilone
Ixabepilone given at a starting dose of 32 or 40 mg/m^2 (as per approved labeling) as a 3-hour IV infusion on Day 1 of a 21-day cycle. The Treatment Phase will include six cycles. Patients may enter the Extension Phase for additional cycles following the sixth cycle of treatment.

Locations

Country Name City State
United States Lone Star Oncology Austin Texas
United States Summit Medical Group Berkeley Heights New Jersey
United States Comprehensive Cancer Care Specialist of Boca Boca Raton Florida
United States Montefiore Medical Center Bronx New York
United States Josephine Ford Cancer Center Brownstown Michigan
United States Charleston Hematology Oncology Associates PA Charleston North Carolina
United States Hematology Oncology Associates of Illinois Chicago Illinois
United States Maryland Oncology Hematology, PA Columbia Maryland
United States Northwest Cancer Center Corpus Christi Texas
United States South Texas Institute of Cancer Corpus Christi Texas
United States Heartland Oncology Hematology Council Bluffs Iowa
United States Texas Cancer Center at Medical City Dallas Texas
United States Texas Oncology, PA Dallas Texas
United States Texas Oncology-Sammons Cancer Center Dallas Texas
United States Henry Ford Medical Center-Fairlane Dearborn Michigan
United States Decatur Memorial Hospital Decatur Illinois
United States Henry Ford Health Systems Detroit Michigan
United States Robert R. Carroll, MD, PA Gainesville Florida
United States Washington County Hospital Hagerstown Maryland
United States Healing Hands Oncology and Medical Care Hawthorne California
United States Texas Oncology, PA Houston Texas
United States Texas Oncology, PA Bedford Houston Texas
United States Central Indiana Cancer Centers Indianapolis Indiana
United States Queens Cancer Center of Queens Hospital Jamaica New York
United States Hematology Oncology Associates Lake Worth Florida
United States Medical Specialists of the Palm Beaches Lake Worth Florida
United States University of Southern California Los Angeles California
United States Hematology and Oncology Specialists Marrero Louisiana
United States Metairie Institute of Comprehensive Health Metairie Louisiana
United States Joan Knechel Cancer Center Mount Arlington New Jersey
United States Hematology and Oncology Specialists New Orleans Louisiana
United States Saint Vincent's Comprehensive Cancer Center New York New York
United States Weil Cornell Breast Center New York New York
United States Virginia Oncology Associates Newport News Virginia
United States Virginia Oncology Associates Norfolk Virginia
United States Ocala Oncology Center Ocala Florida
United States Northern Utah Associates Ogden Utah
United States Comprehensive Cancer Center Palm Springs California
United States North Texas Regional Cancer Center Plano Texas
United States Hematology Oncology Associates of Treasure Coast Port Saint Lucie Florida
United States Northwest Cancer Specialists Hoyt Portland Oregon
United States Northwest Cancer Specialists Rose Quarter Portland Oregon
United States Cancer Center of North Carolina Raleigh North Carolina
United States Northern AZ Hematology and Oncology Associates Sedona Arizona
United States Oncology and Hematology Associates of West Broward Tamarac Florida
United States Northwest Cancer Specialists Tualatin Oregon
United States Tyler Cancer Center Tyler Texas
United States Northwest Cancer Care Specialists, P.C. Vancouver Washington
United States Northwest Cancer Specialist Vancouver Vancouver Washington
United States Henry Ford Medical Center Farmington West Bloomfield Michigan

Sponsors (1)

Lead Sponsor Collaborator
Eisai Inc.

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Percentage of Participants With Treatment-Emergent Neuropathy Adverse Events (AEs) Neuropathy AEs were graded according to National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) version 3.0 and coded according to the current version of the Medical Dictionary for Regulatory Activities (MedDRA). Neuropathy AEs included the broad list of preferred terms (PTs) defined in the Standard MedDRA Query for Neuropathy and the following additional PTs: neuropathy, hyperesthesia, painful response to normal stimuli, pallanesthesia, and allodynia. If the post-baseline maximum CTCAE grade of the combined term "neuropathy" was greater than the baseline maximum CTCAE grade of the combined term, then the event was considered as treatment emergent neuropathy adverse events per CTCAE grade. For a single participant, 1) a neuropathy AE occurring more than once during the study, whether defined with the same or different MedDRA PTs, was counted only once, 2) a neuropathy AE with different CTCAE grades had only the highest grade AE counted. From administration of first dose up to approximately 5 years
Secondary Percentage of Participants With an Incidence of Treatment-emergent Myalgia/Arthralgia The incidence rate of TE myalgia/arthralgia was calculated as the percent of participants with TE myalgia/arthralgia. A participant who had an arthralgia or myalgia AE more than once over the course of the study was counted only once in the incidence calculation for myalgia/arthralgia AEs. A participant who had myalgia/arthralgia AEs with different CTCAE grades was counted with the highest CTCAE grade over the course of the evaluation period. If the post-baseline CTCAE grade of the combined term "Myalgia/Arthralgia" was greater than the baseline maximum CTCAE grade of the combined term, the participant had TE myalgia/arthralgia. The 2-sided 95% confidence interval (CI) for incidence rate of TE myalgia/arthralgia was calculated using the Clopper-Pearson method (i.e., the exact method) for each treatment group. From administration of first dose up to approximately 5 years
Secondary Change From Baseline in Vibration Perception Threshold (VPT) The participant-reported questionnaire was used to compare the incidence and severity of neuropathy AEs. Sensory and motor scores were to be analyzed separately using a generalized linear model. Separate subgroup analyses were performed by each stratification variable. VPAT was measured using a Vibratron II device (Physitemp, Inc.) and a modified Two Alternative Forced Choice psychophysical algorithm. VPT was assessed on the ventral surface of the distal index finger (side opposite the nail), contralateral to the side of the mastectomy or primary disease and on the distal fleshy pad of both the right and left great toes (side opposite the nail). If the mastectomy was bilateral, the index finger on the side without axillary lymph node dissection was tested. Data ranged from 0 (invalid) to 20 vu. A lower VPT indicated a greater sensitivity. Baseline, Treatment Phase: Cycles 2 to 6 (Day 1); Extension Phase: Cycle 9 Day 1, Cycle 12 Day 1, Cycle 15 Day 1 (Each Cycle length=21 days), End of Treatment, Post-treatment Follow-up, Worst Post-baseline result (Up to approximately 5 years)
Secondary Number of Participants With Shift From Baseline to Worst Post-baseline Participant Neurotoxicity Questionnaire (PNQ) Score for Item 1 (Sensory) The PNQ consisted of 3 parts; Item 1 (sensory) measured numbness, pain, burning or tingling in hands or feet, Item 2 (motor) measured weakness in arms or legs, and Item 3 (activities) measured activities that interfered with daily life. The participant was told that there was no right or wrong answer and their answer should reflect how they currently felt since last completing the PNQ. Sensory scores were analyzed separately. Letter scores (A= none, B=mild, C=moderate, D=moderate to severe, and E=severe) for PNQ were converted to numeric scores A (none)=0, B (mild)=1, C (moderate)=2, D (moderate to severe)=3 and E (severe)=4). Total scores ranged from 0 (minimum severity) to 10 (maximum severity). Higher scores indicated greater severity. Neuropathy AEs that were sensory were evaluated with the PNQ Item 1 (sensory). Categories where no participant showed any shift from baseline to post-baseline for both the arms were not included in the presentation. Baseline up to approximately 5 years
Secondary Number of Participants With Shift From Baseline to Worst Post-baseline Participant Neurotoxicity Questionnaire (PNQ) Score for Item 2 (Motor) The PNQ consisted of 3 parts; Item 1 (sensory) measured numbness, pain, burning or tingling in hands or feet, Item 2 (motor) measured weakness in arms or legs, and Item 3 (activities) measured activities that interfered with daily life. The participant was told that there was no right or wrong answer and their answer should reflect how they currently felt since last completing the PNQ. Motor scores were analyzed separately. Letter scores (A= none, B=mild, C=moderate, D=moderate to severe, and E=severe) for PNQ were converted to numeric scores A (none)=0, B (mild)=1, C (moderate)=2, D (moderate to severe)=3 and E (severe)=4). Total scores ranged from 0 (minimum severity) to 10 (maximum severity). Higher scores indicated greater severity. Neuropathy AEs that were motor were evaluated with the PNQ Item 2 (motor). Categories where no participant showed any shift from baseline to post-baseline for both the arms were not included in the presentation. Baseline up to approximately 5 years
Secondary Number of Participants With Shift From Baseline to Worst Post-baseline Participant Neurotoxicity Questionnaire (PNQ) Composite Score The PNQ consisted of 3 parts; Item 1 (sensory) measured numbness, pain, burning or tingling in hands or feet, Item 2 (motor) measured weakness in arms or legs, and Item 3 (activities) measured activities that interfered with daily life. Sensory scores, motor scores and composite scores were analyzed separately. For both item 1 and item 2, letter scores (A=none, B=mild, C=moderate, D=moderate to severe, and E=severe) for PNQ were converted to numeric scores A(none)=0, B(mild)=1, C(moderate)=2, D(moderate to severe)=3 and E (severe)=4. Total scores ranged from 0 (minimum severity) to 10 (maximum severity). Higher scores indicated greater severity. PNQ composite score was defined as the worst of Item 1 and Item 2 score. If neither Item 1 or item 2 score was D or E, but if a box was checked in Item 3, PNQ composite score would be D. Categories where no participant showed any shift from baseline to post-baseline for both the arms were not included in the presentation. Baseline up to approximately 5 years
Secondary Objective Response Rate (ORR) ORR was defined as the percentage of participants with a confirmed complete response (CR) or confirmed partial response (PR) based on Response Evaluation Criteria in Solid Tumors (RECIST) v.1.0 for target lesions assessed by magnetic resonance imaging and computed tomography and investigator assessment. Participants with unknown or missing responses were treated as non-responders. CR was defined as disappearance of all target lesions. PR was defined as at least a 30 percent (%) decrease in the sum of the longest diameter of target lesions, taking as reference the baseline sum of the longest diameter. ORR=CR+PR, was presented with 2-sided 95% confidence interval (CI) by the method of Clopper-Pearson method for calculating the exact binomial intervals. From date of treatment start until disease progression (PD) (Up to approximately 5 years)
Secondary Progression-Free Survival (PFS) PFS was defined as the time from randomization until PD or death due to any cause as determined by the investigator. Disease progression per RECIST v1.0 was defined as at least a 20% relative increase and 5 millimeter absolute increase in the sum of diameters of target lesions (taking as reference the smallest sum on study) recorded since the treatment started or the appearance of 1 or more new lesions. The duration of PFS was calculated as the end date minus date of first drug plus 1. For participants who did not have an event (those lost to follow-up or who had not progressed at the date of data cut-off) PFS was censored. The median PFS and corresponding 95% CI was estimated for each treatment group using the Kaplan-Meier method. From date of treatment start until the date of PD or death from any cause (Up to approximately 5 years)
Secondary Clinical Benefit Rate (CBR) CBR was defined as the number of participants (CR + PR + stable disease (SD) greater than or equal to 6 months) divided by the number of participants in the analysis population. The 95% CI was generated for the clinical benefit rate for each treatment group, and it was based on the Clopper-Pearson method for calculating the exact binomial intervals. From date of treatment start until PD or death from any cause, whichever occurred first (Up to approximately 5 years)
Secondary Duration of Response (DoR) DoR was defined as the time from first documented CR or PR until PD or death from any cause. It was measured from the time that measurement criteria were met for CR or PR (whichever status was recorded first) until the first date that recurrent or PD was objectively documented. It was defined for participants with a confirmed CR or a confirmed PR. Participants without progressive disease or death were censored. Median duration and 95% CI of the median were estimated for each treatment group, using the Kaplan-Meier method. From date of first CR or PR until the first documentation of PD or date of death (Up to approximately 5 years)
Secondary Percentage of Participants With Treatment-emergent Adverse Events (TEAEs) and Serious Adverse Events (SAEs) as a Measure of Safety and Tolerability of Eribulin and Ixabepilone General safety was assessed by monitoring all TEAEs and SAEs. TEAEs were reported at a frequency of 0% or greater in the study population. For each participant, from the first dose till 42 days after the last dose of study treatment (Up to approximately 5 years)
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