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Trial details imported from ClinicalTrials.gov
For full trial details, please see the original record at
https://clinicaltrials.gov/ct2/show/NCT02281084
Registration number
NCT02281084
Ethics application status
Date submitted
21/10/2014
Date registered
2/11/2014
Date last updated
28/02/2024
Titles & IDs
Public title
Safety and Efficacy Study of CC-486 in Subjects With Myelodysplastic Syndromes
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Scientific title
A Phase 2, International, Multicenter, Randomized, Open-label, Parallel Group to Evaluate the Efficacy and Safety of Cc-486 (Oral Azacitidine) Alone in Combination With Durvalumab (MEDI4736) in Subjects With Myelodysplastic Syndromes Who Fail to Achieve an Objective Response to Treatment With Azacitidine for Injection or Decitabine
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Secondary ID [1]
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2014-002675-29
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Secondary ID [2]
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CC-486-MDS-006
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Universal Trial Number (UTN)
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Trial acronym
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Linked study record
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Health condition
Health condition(s) or problem(s) studied:
Myelodysplastic Syndromes
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Condition category
Condition code
Blood
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Haematological diseases
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Blood
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Other blood disorders
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Other
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Research that is not of generic health relevance and not applicable to specific health categories listed above
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Intervention/exposure
Study type
Interventional(has expanded access)
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Description of intervention(s) / exposure
Treatment: Drugs - Oral Azacitidine
Treatment: Drugs - Durvalumab
Experimental: Monotherapy: Oral Azacitidine - Oral azacitidine (AZA) 100 mg, 150 mg, or 200 mg tablets twice daily (BID) on days 1 to 21 of each 28-day treatment cycle. Participants continued to receive their assigned study treatment unless disease progression, unacceptable toxicity, lost to follow-up or withdrawal by participant occurred.
Experimental: Combination Therapy: Oral Azacitidine and Durvalumab - Oral Azacitidine 100 mg oral azacitidine tablets BID on days 1 to 14 or days 1 to 21 of each 28-day treatment cycle and durvalumab 1500 mg by intravenous (IV) infusion on day 1 of each 28-day treatment cycle; participants continued to receive their assigned study treatment unless disease progression, unacceptable toxicity, lost to follow-up or withdrawal by participant occurred.
Treatment: Drugs: Oral Azacitidine
Oral azacitidine (AZA) 100 mg, 150 mg, or 200 mg tablets twice daily (BID) on days 1 to 21 of each 28-day treatment cycle. Participants continued to receive their assigned study treatment unless disease progression, unacceptable toxicity, lost to follow-up or withdrawal by participant occurred.
Treatment: Drugs: Durvalumab
Durvalumab 1500 mg by IV infusion on Day 1 of each 28 day treatment cycle.
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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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Overall Response Rate Based on the Modified International Working Group (IWG) 2006 Response Criteria for Myelodysplastic Syndrome (MDS)
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Assessment method [1]
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The overall response rate (ORR) was defined as the percentage of participants who achieved an objective response including: hematologic improvement (HI), partial remission (PR), complete remission (CR), or marrow complete remission (mCR). Hematologic response was defined as:
CR: = 5% myeloblasts with normal maturation of all cell lines; peripheral blood (PB) shows: hemoglobin =11 g/dL, neutrophils =1.0x10^9/L, platelets =100x10^9/dL, blasts (0%)
PR: same as CR bone marrow (BM) shows blasts decreased by = 50% over pre-treatment but still > 5%; cellularity and morphology not relevant
mCR: BM: = 5% myeloblasts and decrease by = 50% over pre-treatment PB, PB: if HI responses, noted in addition to mCR
HI: HI erythroid response (HI-E); HI neutrophil response (HI-N) ; HI platelet response (HI-P)
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Timepoint [1]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [1]
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Kaplan-Meier Estimate of Overall Survival
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Assessment method [1]
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Overall survival (OS) was defined as the time from randomization to death from any cause, and was calculated using date of first dose and date of death, or date of last follow-up for censored subjects. All participants were followed until drop out (withdrawal of consent from further data collection or lost to follow-up), death, or study termination. Participants who dropped out or were alive at study termination (or at the time of the interim analysis) had their OS times censored at the time of last contact, as appropriate.
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Timepoint [1]
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From day 1 of study drug to the data cut off date of 19 June 2019; median follow-up for OS = 15.96 and 8.35 months respectively in the SD and PD oral AZA alone arms and 13.48 and 13.33 months in the SD and PD combination arms
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Secondary outcome [2]
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Kaplan Meier Estimate of Time to Onset of First and Best Response
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Assessment method [2]
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Time to onset of first response was defined as the time between the date of first investigational product (IP) dose and the earliest date any response (CR, PR, mCR, or HI) was first observed. Participants who did not achieve any defined response during the treatment period were censored at the date of treatment discontinuation, disease progression, or death, whichever occurred first. Best response is the best recorded response or treatment outcome from the start of the study treatment until the end of the study treatment taking into account the requirements for confirmation of response.
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Timepoint [2]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [3]
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Kaplan Meier Estimate of Duration of First Response
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Assessment method [3]
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Duration of hematologic response and/or improvement was defined as the time from the date response or improvement was first observed to the date of documented relapse or disease progression as defined by the modified IWG 2006 criteria. Particpants who maintained hematologic response and/or improvement through the end of the treatment period were censored as the date of treatment discontinuation or death, whichever occurred first.
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Timepoint [3]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [4]
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Kaplan Meier Estimate of Duration of Best Response
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Assessment method [4]
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Duration of hematologic response and/or improvement was defined as the time from the date response or improvement was first observed to the date of documented relapse or disease progression as defined by the modified IWG 2006 criteria. Particpants who maintained hematologic response and/or improvement through the end of the treatment period were censored as the date of treatment discontinuation or death, whichever occurred first.
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Timepoint [4]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [5]
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Kaplan-Meier Estimate of Progression Free Survival (PFS)
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Assessment method [5]
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Progression-free survival is defined as the time from randomization to the first documented progressive disease (PD), relapse, or death due to any cause during or after the treatment period, whichever occurred first, according to IWG 2006 response criteria for MDS. Participants who were still alive and progression-free were censored at the date of their last response assessment. Progressive disease is defined as follows: - an increase in BM blasts relative to nadir: •If nadir less than 5% blasts: = 50% increase in blasts to > 5% blasts •If nadir 5% - 10% blasts: = 50% increase in blasts to > 10% blasts •If nadir 10% - 20% blasts: = 50% increase in blasts to > 20% blasts •If nadir 20% - 30% blasts: = 50% increase in blasts to > 30% blasts And any of the following: •At least 50% decrement from maximum remission/response levels in granulocytes or platelets •Reduction in Hgb concentration by = 2 g/dL •Transfusion dependence
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Timepoint [5]
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From day 1 of study drug to the data cut off date of 19 June 2019; median follow-up for OS = 15.96 and 8.35 months respectively in the SD/ PD oral AZA arms and 13.48 and 13.33 months in the SD/PD oral AZA and Durva arms
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Secondary outcome [6]
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Percentage of Participants With Progressive Disease at Baseline Who Achieved Stable Disease
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Assessment method [6]
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A participant was considered as having a stable disease if the disease neither responded nor progressed during or after study treatment.
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Timepoint [6]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [7]
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Kaplan-Meier Estimate of Onset to Achieve Stable Disease
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Assessment method [7]
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A participant was considered as having a stable disease if the disease neither responded nor progressed during or after study treatment.
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Timepoint [7]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [8]
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Kaplan-Meier Estimate of Duration of Stable Disease
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Assessment method [8]
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The duration of stable disease was defined as the time between any two observations of objective disease progression (modified IWG criteria), starting from the first day of dosing with IP. Participants who maintained stable disease through the end of the treatment period were censored at the date of study termination.
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Timepoint [8]
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Response was assessed every 2 cycles following treatment during the first 6 cycles, then every 3 cycles thereafter; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively, and 1.84 months for AZA and Durva SD/PD arms
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Secondary outcome [9]
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Percentage of Participants Who Progressed to Acute Myelogenous Leukemia (AML)
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Assessment method [9]
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For all participants who received at least one dose of study drug, continuous monitoring for progression to AML occurred in the post treatment follow up period.
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Timepoint [9]
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From Day 1 of study drug up to the data cut off date of 19 June 2019; median follow up time for AML progression = 11.59 and 5.65 months respectively in the SD and PD arms for oral AZA and 6.21 months for SD/PD in the combination arm.
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Secondary outcome [10]
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Kaplan-Meier Estimate of Time to Progression to AML
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Assessment method [10]
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Time to AML progression was defined as the time from the date of first dose of IP until the date the participant had documented progression to AML.
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Timepoint [10]
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From Day 1 of study drug up to the data cut off date of 19 June 2019; median follow up time for AML progression = 11.59 and 5.65 months respectively in the SD and PD arms for oral AZA and 6.21 months for SD/PD in the combination arm.
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Secondary outcome [11]
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Number of Participants With Treatment Emergent Adverse Events (TEAEs)
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Assessment method [11]
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TEAEs were defined as AEs occurring or worsening on or after the date of the first dose of oral aza or durva and within 28 days after last dose of oral aza or 90 days after last dose of durva
A serious adverse event (SAE) is any:
Death;
Life-threatening event;
Any inpatient hospitalization or prolongation of existing hospitalization;
Persistent or significant disability or incapacity;
Congenital anomaly or birth defect;
Any other important medical event The severity of an AE was evaluated by the investigator according to National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) (Version 4.0) where Grade 1 = Mild, Grade 2 = Moderate, Grade 3 = Severe, Grade 4 = Life-threatening and Grade 5 = Death.
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Timepoint [11]
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From first dose of IP until 28 days after final oral AZA dose, 90 days after final durva dose and/or treatment stopped; median duration of treatment = 5.26 and 3.81 months for SD/PD for oral AZA arms respectively; 1.84 months for AZA and Durva SD/PD arms
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Eligibility
Key inclusion criteria
1. Male or female, = 18 years of age at the time of signing the informed consent document
2. Documented diagnosis of MYELODYSPLASTIC SYNDROMES (MDS), classified according to
FRENCH-AMERICAN BRITISH (FAB) classification criteria
3. Adequate course of treatment with an injectable hypomethylating agent (azacitidine for
injection or decitabine) as the last therapeutic intervention for MDS prior to
beginning screening for this study. Adequate is defined as:
- having received at least 6 consecutive 4-week treatment cycles with azacitidine
for injection, or
- having received at least 4 consecutive 6-week treatment cycles with decitabine
(3-day regimen) or at least 6 consecutive 4-week treatment cycles with decitabine
(5-day regimen), or
- having demonstrated inability to tolerate treatment with an injectable
hypomethylating agent because of unacceptable drug-related toxicity after at
least 3 months of attempted treatment: Three 28-day cycles of azacitidine for
injection or decitabine 5-day regimen; two 42-day cycles of decitabine 3-day
regimen.
4. Documented disease progression or stable disease as best response to treatment (or
attempted treatment) with azacitidine for injection or decitabine. Those achieving an
objective response to treatment regimen with an injectable hypomethylating agent (HMA)
are excluded from participation in this study.
Definitions of disease progression are modified from INTERNATIONAL WORKING GROUP (IWG)
2006 criteria and include:
- Pre-injectable hypomethylating agent baseline bone marrow myeloblasts:
1. Less than 5%: = 100% increase to = 8% blasts
2. = 5%: = 50% increase to = 10% blasts Note: = 30% blasts is considered acute
myeloid leukemia (AML )per FAB classification. Subjects known to have = 30%
blasts are not eligible for inclusion in this study.recognizing eastern
cooperative oncology group) limitations of blast cell quantification, Protocol
will allow subjects with pre-enrollment bone marrow blast counts up to 33% on the
screening bone marrow examination to be considered for inclusion. Assessment may
be made according to local bone marrow examination to facilitate enrollment of
eligible subjects into the treatment phase of the study.
- Any clinical worsening from pre-injectable hypomethylating agents (HMA)
baseline condition, including:
1. sustained clinically-significant worsening (investigator's assessment) from
baseline granulocyte, platelet, or hemoglobin values (= 2 values, separated by =
2 weeks) - worsening granulocytes should be = 50% decrease from pre-injectable
HMA baseline value - worsening platelets should be = 50% decrease from
pre-injectable HMA baseline value (untransfused)
- worsening hemoglobin should be = 1.5 g/dL decrease from preinjectable HMA
baseline value in subjects not receiving RBC transfusions
2. meaningful worsening in RBC or platelet transfusion requirement
Definition of stable disease is based on modified IWG 2006 criteria:
- Failure to achieve any objective response (CR - complete remission, PR -
partial remissino, mCR - marrow complete remission, or HI - hematologic
improvement), but no evidence of disease progression within the 8 weeks
leading to the subject's first dose of investigational product (IP), Cycle
1, Day 1
5. Have the last dose of the prior treatment regimen injectable HMA - (azacitidine for
injection or decitabine) not more than 16 weeks prior to screening for this study
(date of informed consent signature).
6. No less than 3 weeks between the last dose of the prior treatment regimen injectable
HMA - (azacitidine for injection or decitabine) and the planned date of first dose of
IP (
7. Have an eastern cooperative oncology group (ECOG) performance status of 0, 1, or 2
8. Females subjects of childbearing potential (FCBP)1 may participate, providing they
meet the following conditions:
1. Have two negative pregnancy tests as verified by the investigator prior to
starting any IP therapy: serum pregnancy test at screening and negative serum or
urine pregnancy test (investigator's discretion) within 72 hours prior to
starting treatment with IP (Cycle 1, Day 1). They must agree to ongoing pregnancy
testing during the course of the study (before beginning each subsequent cycle of
treatment), and after the last dose of any IP. This applies even if the subject
practices complete abstinence2 from heterosexual contact.
2. Agree to practice true abstinence2 (which must be reviewed on a monthly basis and
source documented) or agree to the use of highly effective methods of
contraception from 28 days prior to starting azacitidine, and must agree to
continue using such precautions while taking azacitidine (including dose
interruptions) and for up to 90 days after the last dose of azacitidine.
Cessation of contraception after this point should be discussed with a
responsible physician
3. Agree to abstain from breastfeeding during study participation and for at least
90 days after the last dose of IP.
Note that the screening serum pregnancy test can also be used as the test prior to starting
IP if it is performed within the 72-hour timeframe.
9. Male subjects must:
1. Male subjects must:
1. Either practice true abstinence2 from heterosexual contact (which must be
reviewed on a monthly basis) or agree to avoid fathering a child, to use highly
effective methods of contraception, male condom plus spermicide during sexual
contact with a pregnant female or a female of child bearing potential (even if he
has undergone a successful vasectomy) from starting dose of IP (Cycle 1 Day 1),
including dose interruptions through 90 days after receipt of the last dose of
azacitidine.
2. Refrain from semen or sperm donation while taking IP and for at least 90 days after
the last dose of IP.
10. Understand and voluntarily sign an informed consent document prior to any
study-related assessments or procedures conducted.
11. Be able to adhere to the study visit schedule and other protocol requirements.
12. Understand and voluntarily sign a biomarker-specific component of the informed
consent document prior to any study-related procedures conducted.
Extension Phase
At the Investigator's discretion and following confirmation of eligibility criteria below,
subjects can enter the Extension Phase (EP):
- Subjects who have signed the informed consent for the EP of the study;
- Subjects receiving oral azacitidine and continuing in the treatment phase
demonstrating clinical benefit as assessed by the Investigator are eligible to receive
oral azacitidine in the EP;
- Subjects who do not meet any of the criteria for study discontinuation
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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
1. Rapidly-progressing MDS defined as:
1. Known clinically-significant doubling in marrow or per IP peripheral blood blast
percentage (to = 20%) in the 8-week period leading to the first dose of IP (Cycle
1, Day 1)
2. =100% increase in WBC count (myeloid cell line and monocyte series) within the
8-week period leading to Cycle 1, Day 1
2. AML - FAB (FRENCH-AMERICAN-BRITISH) classification: = 30% blasts in bone marrow).
Subjects known to have = 30% blasts are not eligible for inclusion in this study.
Recognizing limitations of blast cell quantification, this protocol will allow
subjects with pre-enrollment (screening/baseline) bone marrow blast counts up to 33%
to be considered for inclusion.
3. Prior allogeneic stem cell transplant
4. Prior exposure to the investigational oral formulation of decitabine, or other oral
azacitidine derivative at any time in the subject's prior history
5. Prior or ongoing response (IWG 2006: HI, PR, CR, or marrow CR) to treatment with
azacitidine for injection or decitabine, at any time in the subject's prior history,
which includes relapsed disease
6. Ongoing medically significant adverse events from previous treatment, regardless of
the time period
7. Use of any of the following within 28 days prior to the first dose of IP:
1. thrombopoiesis-stimulating agents ([TSAs]; eg, Romiplostim, Eltrombopag,
Interleukin-11)
2. ESAs (Erythropoiesis stimulating agent) and other RBC hematopoietic growth
factors (eg, interleukin-3)
3. hydroxyurea
8. Concurrent use of corticosteroids unless the subject is on a stable or decreasing dose
for = 1 week prior to enrollment for medical conditions other than MDS
9. History of inflammatory bowel disease (eg, Crohn's disease, ulcerative colitis),
celiac disease (ie, sprue), prior gastrectomy or upper bowel removal, or any other
gastrointestinal disorder or defect that would interfere with the absorption,
distribution, metabolism or excretion of the IP and/or predispose the subject to an
increased risk of gastrointestinal toxicity
10. Prior history of malignancies, other than MDS, unless the subject has been free of the
disease for = 3 years. However, subjects with the following history/concurrent
conditions are allowed:
1. Basal or squamous cell carcinoma of the skin
2. Carcinoma in situ of the cervix
3. Carcinoma in situ of the breast
4. Incidental histologic finding of prostate cancer (T1a or T1b using the tumor,
nodes, metastasis [TNM] clinical staging system)
11. Significant active cardiac disease within the previous 6 months, including:
1. New York Heart Association (NYHA) class IV congestive heart failure;
2. Unstable angina or angina requiring surgical or medical intervention; and/or
3. Myocardial infarction
12. Uncontrolled systemic fungal, bacterial, or viral infection (defined as ongoing
signs/symptoms related to the infection without improvement despite appropriate
antibiotics, antiviral therapy, and/or other treatment)
13. Known Human Immunodeficiency Virus (HIV) or Hepatitis C (HCV) infection, or evidence
of active Hepatitis B Virus (HBV) infection
14. Any of the following laboratory abnormalities:
1. Serum Aspartate transaminase / Serum glutamic oxaloacetic transaminase (AST/SGOT)
Alanine aminotransaminase / Serum glutamic pyruvate transaminase (ALT/SGPT) > 2.5
x ULN (upper limit of normal)
2. Serum total bilirubin > 1.5 x upper limit of normal (ULN). Higher levels are
acceptable if these can be attributed to active red blood cell precursor
destruction within the bone marrow (ie, ineffective erythropoiesis). Subjects are
excluded if there is evidence of autoimmune hemolytic anemia manifested as a
corrected reticulocyte count of > 2% with either a positive Coombs' test or over
50% of indirect bilirubin
3. Serum creatinine > 2.5 x ULN (upper limit of normal)
4. Absolute WBC (white blood cell) count = 20 x 109/L
15. Known or suspected hypersensitivity to azacitidine, mannitol, its constituents, or to
any other humanized monoclonal antibody
16. Pregnant, planning to become pregnant starting from 28 days prior to receiving CC-486
throughout your participation in the study, and for at least 90 days following your
last dose of study treatment, or breast-feeding females
17. Any significant medical condition, laboratory abnormality, or psychiatric illness that
would prevent the subject from participating in the study
18. Any condition including the presence of laboratory abnormalities, which places the
subject at unacceptable risk if he/she were to participate in the study
19. Any condition that confounds the ability to interpret data from the study, including
known or suspected conditions other than MDS, associated with anemia
20. Having received any prior MAb (monoclonal antibodies) against CTLA-4 (cytotoxic T
lymphocyte-associated antigen), PD-1, or PD-L1 or having received other
investigational monoclonalantibodies (MAbs) within 6 months
21. Clinical evidence of central nervous system (CNS) or pulmonary leukostasis, or CNS
leukemia
22. Active or prior documented autoimmune or inflammatory disorders (including
inflammatory bowel disease [eg, colitis, Crohn's disease], diverticulitis with the
exception of a prior episode that has resolved or diverticulosis, celiac disease,
irritable bowel disease, or other serious gastrointestinal chronic conditions
associated with diarrhea; systemic lupus erythematosus; Wegener's syndrome
[granulomatosis with polyangiitis]; myasthenia gravis; Graves' disease; rheumatoid
arthritis; hypophysitis, uveitis; etc) within the past 3 years prior to the start of
treatment. The following are exceptions to this criterion:
1. Subjects with vitiligo or alopecia;
2. Subjects with hypothyroidism (eg, following Hashimoto syndrome) stable on hormone
replacement for = 3 months; or
3. Subjects with psoriasis not requiring systemic treatment
23. History of primary immunodeficiency
24. Active myeloproliferative neoplasms (MPN) and chronic myelomonocytic leukemia (CMML)
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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 2
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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
6/07/2015
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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
14/09/2023
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Sample size
Target
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Accrual to date
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Final
65
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Recruitment in Australia
Recruitment state(s)
NSW,SA,VIC
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Recruitment hospital [1]
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Westmead Hospital - Westmead
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Recruitment hospital [2]
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Royal Adelaide Hospital - Adelaide
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Recruitment hospital [3]
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Local Institution - 400 - Clayton
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Recruitment hospital [4]
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Monash Medical Centre - Clayton
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Recruitment hospital [5]
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Cabrini Hospital - Malvern
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Recruitment hospital [6]
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Local Institution - 405 - Malvern
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Recruitment hospital [7]
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Royal Brisbane and Women's Hospital - Herston
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Recruitment hospital [8]
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Royal Perth Hospital - Perth
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Recruitment postcode(s) [1]
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2145 - Westmead
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Recruitment postcode(s) [2]
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5000 - Adelaide
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Recruitment postcode(s) [3]
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3168 - Clayton
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Recruitment postcode(s) [4]
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3144 - Malvern
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Recruitment postcode(s) [5]
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4029 - Herston
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Recruitment postcode(s) [6]
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6000 - Perth
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Recruitment outside Australia
Country [1]
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0
United States of America
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State/province [1]
0
0
Connecticut
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Country [2]
0
0
United States of America
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State/province [2]
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Florida
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0
0
United States of America
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State/province [3]
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Illinois
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Country [4]
0
0
United States of America
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State/province [4]
0
0
Iowa
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Country [5]
0
0
United States of America
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0
0
Kentucky
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Country [6]
0
0
United States of America
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State/province [6]
0
0
New Jersey
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0
0
United States of America
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State/province [7]
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New York
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0
0
United States of America
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State/province [8]
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Pennsylvania
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0
United States of America
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State/province [9]
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0
Texas
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0
0
United States of America
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State/province [10]
0
0
Wisconsin
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Country [11]
0
0
Belgium
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Funding & Sponsors
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Commercial sector/Industry
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Celgene
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Summary
Brief summary
Evaluate the safety and efficacy of oral azacitidne (CC-486) twice daily (BID) in subjects
with myelodysplastic syndromes who failed to achieve an objective response post injectable
hypomethylating agent (iHMA) treatment
Reason for removing the combination arm: Due to difficulties with dose-finding, the
durvalumab plus CC-486 combination arm was closed to enrollment.
Extension:
An Extension Phase (EP) has been added to allow subjects who are currently receiving oral
azacitidine BID and who are demonstrating clinical benefit as assessed by the Investigator,
to continue receiving oral azacitidine until the subject meets the criteria for study
discontinuation.
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Trial website
https://clinicaltrials.gov/ct2/show/NCT02281084
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Bristol-Myers Squibb
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Bristol-Myers Squibb
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Summary Results
For IPD and results data, please see
https://clinicaltrials.gov/ct2/show/NCT02281084
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