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Trial details imported from ClinicalTrials.gov
For full trial details, please see the original record at
https://clinicaltrials.gov/study/NCT01102426
Registration number
NCT01102426
Ethics application status
Date submitted
31/03/2010
Date registered
13/04/2010
Date last updated
10/11/2020
Titles & IDs
Public title
Aplidin - Dexamethasone in Relapsed/Refractory Myeloma
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Scientific title
Randomized, Multicenter, Open-label, Phase III Study of Plitidepsin in Combination With Dexamethasone vs. Dexamethasone Alone in Patients With Relapsed/Refractory Multiple Myeloma
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Secondary ID [1]
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APL-C-001-09
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Universal Trial Number (UTN)
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Trial acronym
ADMYRE
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Linked study record
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Health condition
Health condition(s) or problem(s) studied:
Relapsed/Refractory Multiple Myeloma
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Condition category
Condition code
Cancer
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Other cancer types
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Intervention/exposure
Study type
Interventional
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Description of intervention(s) / exposure
Treatment: Drugs - Plitidepsin
Treatment: Drugs - Dexamethasone
Experimental: Plitidepsin+Dexamethasone - plitidepsin + dexamethasone combination
Active comparator: Dexamethasone - dexamethasone single agent
Treatment: Drugs: Plitidepsin
plitidepsin: powder and solvent for concentrate for solution for infusion. 2 mg vial + 4 ml ampoule. 5 mg/m2 intravenously (i.v.) over three hours on Day 1 and 15 every 4 weeks. dexamethasone: 4 mg tablet. 40 mg orally on Day 1, 8, 15 and 22 every four weeks at least one hour before plitidepsin infusion.
Treatment: Drugs: Dexamethasone
4 mg tablet. 40 mg orally on Day 1, 8, 15 and 22 every four weeks.
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Intervention code [1]
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Treatment: Drugs
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Comparator / control treatment
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Control group
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Outcomes
Primary outcome [1]
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Progression Free Survival (PFS) as Per Intention-to-treat (ITT)
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Assessment method [1]
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To compare the efficacy of plitidepsin in combination with dexamethasone vs. dexamethasone alone as measured by progression-free survival (PFS) in patients with relapsed/refractory multiple myeloma (MM).
Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions
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Timepoint [1]
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From date of randomization until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 5 years
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Primary outcome [2]
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Percentage of Participants With Progression Free Survival (PFS) as Per Intention-to-treat (ITT) at 6 Months
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Assessment method [2]
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To compare the efficacy of plitidepsin in combination with dexamethasone vs. dexamethasone alone as measured by progression-free survival (PFS) in patients with relapsed/refractory multiple myeloma (MM).
Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions
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Timepoint [2]
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From date of randomization until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 6 months
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Secondary outcome [1]
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Progression-free Survival (Investigator Assessment)
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Assessment method [1]
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The secondary study analysis was based on Investigator's assessment PFS data in the ITT efficacy population, defined as all patients randomized to either treatment arm. PFS was calculated from randomization to the first evidence of PD or death due to any cause. Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions If the patient received further antitumor therapy before PD and within the timeframe expected for first follow-up, PFS was censored on the date of the last disease assessment prior to the administration of this antitumor therapy.
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Timepoint [1]
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From date of randomization until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 5 years
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Secondary outcome [2]
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Percentage of Participants With Progression-free Survival (Investigator Assessment) at 6 Months
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Assessment method [2]
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The secondary study analysis was based on Investigator's assessment PFS data in the ITT efficacy population, defined as all patients randomized to either treatment arm. PFS was calculated from randomization to the first evidence of PD or death due to any cause. Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions If the patient received further antitumor therapy before PD and within the timeframe expected for first follow-up, PFS was censored on the date of the last disease assessment prior to the administration of this antitumor therapy.
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Timepoint [2]
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From date of randomization until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 6 months
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Secondary outcome [3]
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Overall Survival
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Assessment method [3]
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Overall Survival (OS) is defined as the time from the date of randomization to the date of death or last contact
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Timepoint [3]
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From randomization to the death due to any cause,assessed up to 5 years
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Secondary outcome [4]
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Percentage of Participants With Overall Survival at 12 Months
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Assessment method [4]
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Overall Survival (OS) is defined as the time from the date of randomization to the date of death or last contact
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Timepoint [4]
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From randomization to the death due to any cause,assessed up to 12 months
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Secondary outcome [5]
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Percentage of Participants With Overall Survival at 24 Months
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Assessment method [5]
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Overall Survival (OS) is defined as the time from the date of randomization to the date of death or last contact
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Timepoint [5]
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From randomization to the death due to any cause,assessed up to 24 months
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Secondary outcome [6]
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Duration of Response (Independent Review Committee)
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Assessment method [6]
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DR was calculated from the date of first documentation of response to the date of disease progression or death. Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions
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Timepoint [6]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [7]
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Percentage of Participants With Duration of Response (Independent Review Committee) at 6 Months
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Assessment method [7]
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DR was calculated from the date of first documentation of response to the date of disease progression or death. Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions
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Timepoint [7]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 6 months
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Secondary outcome [8]
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Duration of Response (Investigator Assessment)
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Assessment method [8]
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DR was calculated from the date of first documentation of response to the date of disease progression or death. Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions
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Timepoint [8]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [9]
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Percentage of Participants With Duration of Response (Investigator Assessment) at 6 Months
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Assessment method [9]
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DR was calculated from the date of first documentation of response to the date of disease progression or death. Progression is defined using Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.0), as a 20% increase in the sum of the longest diameter of target lesions, or a measurable increase in a non-target lesion, or the appearance of new lesions
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Timepoint [9]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 6 months
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Secondary outcome [10]
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Best Overall Response (Independent Review Committee)
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Assessment method [10]
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Very good partial response (VGPR) serum and urine M-protein detectable but not electrophoresis or \>90% reduction in serum M-protein and urine M-protein \<100 mg/24h Partial response (PR) =50% reduction in serum M-protein and 90% reduction in 24h urine M-protein or to \<200 mg/24h. 50% reduction in size of any soft tissue plasmacytomas Minor response (MR) 25%-49% reduction of serum M-protein and 50-89% reduction of 24h urine M-protein. 25-49% reduction in size of soft tissue plasmacytomas. No increase in size or number of bone lesions Stable disease (SD) No sCR, CR, VGPR, PR, MR or PD Progressive disease (PD) 25% increase from the lowest value: serum M-protein, urine M-protein, BM plasma cell. Increase in size, new bone lesions, soft tissue plasmacytomas or serum calcium \>11.5 mg/dL; NE, not evaluable
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Timepoint [10]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [11]
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Overall Response Rate (Independent Review Committee)
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Assessment method [11]
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Overall response rate including sCR, CR, VGPR, PR and MR. Very good partial response (VGPR) serum and urine M-protein detectable but not electrophoresis or \>90% reduction in serum M-protein and urine M-protein \<100 mg/24h Partial response (PR) =50% reduction in serum M-protein and 90% reduction in 24h urine M-protein or to \<200 mg/24h. 50% reduction in size of any soft tissue plasmacytomas Minor response (MR) 25%-49% reduction of serum M-protein and 50-89% reduction of 24h urine M-protein. 25-49% reduction in size of soft tissue plasmacytomas. No increase in size or number of bone lesions
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Timepoint [11]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [12]
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Overall Response Rate (Independent Review Committee) Excluding MR
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Assessment method [12]
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Includes sCR, CR, VGPR and PR (excludes MR). Very good partial response (VGPR) serum and urine M-protein detectable but not electrophoresis or \>90% reduction in serum M-protein and urine M-protein \<100 mg/24h Partial response (PR) =50% reduction in serum M-protein and 90% reduction in 24h urine M-protein or to \<200 mg/24h. 50% reduction in size of any soft tissue plasmacytomas
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Timepoint [12]
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0
From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [13]
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Best Overall Response (Investigator Assessment)
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Assessment method [13]
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Very good partial response (VGPR) serum and urine M-protein detectable but not electrophoresis or \>90% reduction in serum M-protein and urine M-protein \<100 mg/24h Partial response (PR) =50% reduction in serum M-protein and 90% reduction in 24h urine M-protein or to \<200 mg/24h. 50% reduction in size of any soft tissue plasmacytomas Minor response (MR) 25%-49% reduction of serum M-protein and 50-89% reduction of 24h urine M-protein. 25-49% reduction in size of soft tissue plasmacytomas. No increase in size or number of bone lesions Stable disease (SD) No sCR, CR, VGPR, PR, MR or PD Progressive disease (PD) 25% increase from the lowest value: serum M-protein, urine M-protein, BM plasma cell. Increase in size, new bone lesions, soft tissue plasmacytomas or serum calcium \>11.5 mg/dL; NE, not evaluable
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Timepoint [13]
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0
From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [14]
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0
Overall Response Rate (Investigator Assessment)
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Assessment method [14]
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Includes sCR, CR, VGPR, PR and MR. Very good partial response (VGPR) serum and urine M-protein detectable but not electrophoresis or \>90% reduction in serum M-protein and urine M-protein \<100 mg/24h Partial response (PR) =50% reduction in serum M-protein and 90% reduction in 24h urine M-protein or to \<200 mg/24h. 50% reduction in size of any soft tissue plasmacytomas Minor response (MR) 25%-49% reduction of serum M-protein and 50-89% reduction of 24h urine M-protein. 25-49% reduction in size of soft tissue plasmacytomas. No increase in size or number of bone lesions
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Timepoint [14]
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0
From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Secondary outcome [15]
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Overall Response Rate (Investigator Assessment) Excluding MR
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Assessment method [15]
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Very good partial response (VGPR) serum and urine M-protein detectable but not electrophoresis or \>90% reduction in serum M-protein and urine M-protein \<100 mg/24h Partial response (PR) =50% reduction in serum M-protein and 90% reduction in 24h urine M-protein or to \<200 mg/24h. 50% reduction in size of any soft tissue plasmacytomas
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Timepoint [15]
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From the date of first documentation of response to the date of disease progression or death, assessed up to 5 years
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Eligibility
Key inclusion criteria
* Age = 18 years.
* Eastern Cooperative Oncology Group (ECOG) Performance Status (PS) = 2
* Life expectancy = 3 months.
* Patients previously diagnosed with multiple myeloma
* Patients must have relapsed or relapsed and refractory multiple myeloma (MM) after at least three but not more than six prior therapeutic regimens for MM, including induction therapy and stem cell transplant in candidate patients, which will be considered as only one regimen.
* Patients must have received previous bortezomib-containing and lenalidomide-containing regimens (or thalidomide where lenalidomide is not available)
* Women must have a negative serum pregnancy test
* Voluntarily signed and dated written informed consent
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Minimum age
18
Years
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Maximum age
No limit
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Sex
Both males and females
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Can healthy volunteers participate?
No
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Key exclusion criteria
* Concomitant diseases/conditions
* Women who are pregnant or breast feeding.
* Concomitant medications that include corticosteroids, chemotherapy, or other therapy that is or may be active against MM
* Known hypersensitivity to any involved study drug or any of its formulation components
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Study design
Purpose of the study
Treatment
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Allocation to intervention
Randomised controlled trial
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Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)
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Methods used to generate the sequence in which subjects will be randomised (sequence generation)
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Masking / blinding
Open (masking not used)
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Who is / are masked / blinded?
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Intervention assignment
Parallel
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Other design features
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Phase
Phase 3
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Type of endpoint/s
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Statistical methods / analysis
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Recruitment
Recruitment status
Completed
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Data analysis
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Reason for early stopping/withdrawal
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Other reasons
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Date of first participant enrolment
Anticipated
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Actual
1/06/2010
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Date of last participant enrolment
Anticipated
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Actual
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Date of last data collection
Anticipated
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Actual
1/11/2017
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Sample size
Target
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Accrual to date
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Final
255
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Recruitment in Australia
Recruitment state(s)
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Recruitment hospital [1]
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108 - Adelaide
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Recruitment hospital [2]
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102 - Canberra
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Recruitment hospital [3]
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101 - Geelong
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Recruitment hospital [4]
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105 - Parkville
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Recruitment hospital [5]
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106 - Perth
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Recruitment hospital [6]
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104 - South Brisbane
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Recruitment hospital [7]
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109 - Woodville
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Recruitment postcode(s) [1]
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- Adelaide
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Recruitment postcode(s) [2]
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- Canberra
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Recruitment postcode(s) [3]
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- Geelong
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Recruitment postcode(s) [4]
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- Parkville
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Recruitment postcode(s) [5]
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- Perth
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Recruitment postcode(s) [6]
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- South Brisbane
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Recruitment postcode(s) [7]
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- Woodville
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Recruitment outside Australia
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United States of America
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Alabama
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United States of America
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California
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United States of America
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Florida
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United States of America
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New York
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United States of America
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Ohio
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Austria
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Graz
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Austria
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Innsbruck
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Austria
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Salzburg
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Austria
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Wien
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Belgium
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Brugge
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Belgium
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Brussels
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Belgium
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Gent
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Czechia
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Brno
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Czechia
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Hradec Kralove
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Czechia
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Praha
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France
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Lille
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France
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Nantes
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France
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Rouen
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France
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VandÅ“uvre-lès-Nancy
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Germany
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Düsseldorf
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Germany
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Essen
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Germany
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Frankfurt
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Germany
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Freiburg
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Germany
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Heidelberg
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Germany
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Munchen
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Germany
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Würzburg
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Athens
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Bari
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Genova
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Reggio Emilia
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Italy
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Rozzano
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Italy
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San Giovanni Rotondo
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Italy
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Torino
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Korea, Republic of
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Anyang
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Daejeon
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Hwasun
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Incheon
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Jeonju
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Seongnam
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Seoul
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Rotterdam
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Takapuna
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Poland
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Opole
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Poland
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Warszawa
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Portugal
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Braga
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Porto
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Barcelona
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Madrid
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Murcia
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San Sebastián
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Valencia
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Taiwan
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Taipei
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Bournemouth
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Bradford
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London
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United Kingdom
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Nottingham
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Funding & Sponsors
Primary sponsor type
Commercial sector/industry
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Name
PharmaMar
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Address
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Country
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Ethics approval
Ethics application status
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Summary
Brief summary
Study of Plitidepsin in combination with dexamethasone versus dexamethasone alone in patients with relapsed/refractory multiple myeloma.
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Trial website
https://clinicaltrials.gov/study/NCT01102426
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Trial related presentations / publications
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Public notes
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Contacts
Principal investigator
Name
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Óscar F. Ballester, M.D.
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Address
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Edwards Comprehensive Cancer Center, Marshall University (Huntington)
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Country
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No information has been provided regarding IPD availability
What supporting documents are/will be available?
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Attachment
Study protocol
https://cdn.clinicaltrials.gov/large-docs/26/NCT01102426/Prot_000.pdf
Statistical analysis plan
https://cdn.clinicaltrials.gov/large-docs/26/NCT01102426/SAP_001.pdf
Results publications and other study-related documents
No documents have been uploaded by study researchers.
Results are available at
https://clinicaltrials.gov/study/NCT01102426
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