Back to resultsA Study of ASP2215 in Combination With Induction and Consolidation Chemotherapy in Patients With Newly Diagnosed Acute Myeloid Leukemia.
Primary Purpose
Acute Myeloid Leukemia, FLT3-mutated Acute Myeloid Leukemia
Status
Active
Phase
Phase 1
Locations
International
Study Type
Interventional
Intervention
gilteritinib
Idarubicin
Cytarabine
Sponsored by
About this trial
This is an interventional treatment trial for Acute Myeloid Leukemia focused on measuring Acute Myeloid Leukemia, Cytarabine, Idarubicin, ASP2215
Eligibility Criteria
Inclusion Criteria:
[Phase 1 part]
- Subject is defined as having previously untreated de novo AML according to the World Health Organization (WHO) criteria (2008) within 28 days prior to study enrollment.
- Subject has an Eastern Cooperative Oncology Group (ECOG) performance status of ≤ 2.
Subject must meet all of the following criteria in the laboratory test at screening:
- Serum aspartate aminotransferase (AST) and alanine aminotransferase (ALT) levels of ≤ 2.5 × institutional upper limit of normal (ULN)
- Total serum bilirubin level of ≤ 1.5 × institutional ULN
- Serum creatinine level of ≤ 1.5 × institutional ULN or an estimated glomerular filtration rate (eGFR) of > 50 mL/min
- Subject is suitable for oral administration of ASP2215.
Female subject falls under the following:
- Of non-childbearing potential:
- ・Post-menopausal (defined as at least 1 year with no menses without a medical reason such as drug administration) at screening, or
- ・Documented surgically sterile or status post-hysterectomy (at least 1 month prior to screening)
- Of childbearing potential:
- ・Has a negative result for the pregnancy test at screening, and
- ・Agrees to use an appropriate contraception starting at screening and throughout the study period and for 60 days after the final study drug administration
- Female subject agrees not to breastfeed starting at screening and throughout the study period and for 60 days after the final study drug administration.
- Female subject agrees not to donate ova starting at screening and throughout the study period and for 60 days after the final study drug administration.
- Male subject and his female spouse/partner who is of childbearing potential agrees to use an appropriate contraception starting at screening and throughout the study period and for 120 days after the final study drug administration.
- Male subject agrees not to donate sperm starting at screening and throughout the study period and for 120 days after the final study drug administration.
- Subject agrees not to participate in another interventional study while on study treatment.
- Subject can be admitted during the induction period.
[Phase 2 part]
- Subject has a diagnosis of previously-untreated de novo acute myeloid leukemia (AML) according to World Health Organization (WHO) classification (2017) documented within 28 days prior to enrollment.
- Subject is positive for FLT3-ITD and/or TKD mutation in bone marrow or whole blood as determined by the central lab. Registration by the local lab result is not acceptable.
- Subject has an ECOG performance status (PS) 0 to 1. Subject who has an ECOG PS 2 is eligible only if the primary disease related symptoms such as pneumonia and febrile neutropenia are the cause of PS score.
- Subject is suitable for oral administration of ASP2215.
Female subject is not pregnant and at least 1 of the following conditions apply:
- Not a woman of childbearing potential (WOCBP)
- WOCBP who agrees to follow the contraceptive guidance from the time of informed consent through at least 180 days after final study treatment administration.
- Female subject must agree not to breastfeed starting at screening and throughout the study period, and for 60 days after the final study drug administration.
- Female subject must not donate ova starting at screening and throughout the study period, and for 180 days after the final study drug administration.
- Male subject and their female partners who are of childbearing potential must be using highly effective contraception per locally accepted standards in addition to a barrier method starting at screening and continue throughout the study period and for 120 days after the final study drug administration.
- Male subject must not donate sperm starting at screening and throughout the study period and for 120 days after the final study drug administration.
- Male subject with pregnant partner(s) must agree to remain abstinent or use a condom for the duration of the pregnancy throughout the study period and for 120 days after the final study treatment administration.
- Subject agrees not to participate in another interventional study while on treatment.
Subject must meet the following criteria as indicated on the clinical laboratory tests:
- Serum creatinine ≤ 1.5 × institutional upper limit of normal (ULN), or if serum creatinine outside normal range, then glomerular filtration rate (GFR) > 50 mL/min/1.73m^2 as calculated with the 4-parameter Modification of Diet in Renal Disease (MDRD) equation.
- Serum total bilirubin ≤ 2.5 mg/dL (43 μmol/L), except for subjects with Gilbert's syndrome.
- Serum aspartate aminotransferase (AST) and alanine aminotransferase (ALT) < 3 x ULN. If liver abnormality by the primary disease is suspected, subject may be pre-registered to initiate the chemotherapy. Prior to registration, AST/ALT values must meet the criteria to continue the study.
- Serum magnesium ≥ institutional lower limit of normal (LLN). Subject may pre-register without magnesium value, but subject must meet the criteria prior to the full registration on Day 8.
- Serum potassium ≥ institutional lower limit of normal (LLN).
Exclusion Criteria:
[Phase 1 part]
- Subject was diagnosed with acute promyelocytic leukemia (APL).
- Subject has breakpoint cluster region-abelson (BCR-ABL)-positive leukemia (chronic myelogenous leukemia in blast crisis).
- Subject has active malignant tumors other than AML or myelodysplastic syndrome (MDS).
Subject has received prior AML treatment except for the following:
- Urgent leukapheresis
- Hydroxyurea administration for emergency treatment of hyperleukocytosis (≤ 7 days)
- Administration of retinoic acid before the diagnosis to exclude APL (≤ 7 days)
- Supportive care using growth factors or cytokines
- Steroid administration to treat hypersensitivity or blood transfusion reactions
- Subject has clinically active central nervous system leukemia.
- Subject has disseminated intravascular coagulation (DIC).
- Subject has had major surgery within 28 days prior to the first study drug administration.
- Subject has had radiation therapy within 28 days prior to the first study drug administration.
- Subject has congestive heart failure of New York Heart Association (NYHA) class 3 or 4, or subject with a past history of congestive heart failure of NYHA class 3 or 4 and in whom echocardiogram (ECHO) or Multiple Gate Acquisition (MUGA) scan performed within 3 months prior to screening or at screening showed a left ventricular ejection fraction (LVEF) of < 45%.
Subject has cardiac impairment or a clinically significant cardiac disease, including any one of the following:
- Complete left bundle branch block
- Obligate use of a cardiac pacemaker
- Long QT syndrome at Screening
- Prolongation of the QTc interval (> 450 ms) on electrocardiogram (ECG) at screening
- Right bundle branch block + left anterior hemiblock (bifascicular block)
- Angina pectoris within 3 months prior to study drug administration
- Acute myocardial infarction within 3 months prior to study drug administration
- Subject requires treatment with concomitant drugs that are strong inducers of cytochrome P450 (CYP)3A.
- Subject requires treatment with concomitant drugs that are strong inhibitors or inducers of P glycoprotein (P-gp) with the exception of drugs that are considered absolutely essential for the care of the subject.
- Subject requires treatment with concomitant drugs that target serotonin 5HT1 or 5HT2B receptors or sigma receptors, with the exception of drugs that are considered absolutely essential for treatment of the subject.
- Subject has an active uncontrollable infection.
- Subject is known to have human immunodeficiency virus (HIV) infection.
- Subject has active hepatitis B or C or other active hepatic disorders.
- Subject has any condition that, in the investigator's or sub-investigator's opinion, makes the subject unsuitable for study participation.
- Potassium and magnesium levels of below institutional lower limit of normal in the laboratory test at screening.
[Phase 2 part]
- Subject was diagnosed with acute promyelocytic leukemia (APL).
- Subject has known BCR-ABL-positive leukemia (chronic myelogenous leukemia in blast crisis).
- Subject has therapy-related AML.
- Subject has active malignant tumors other than AML.
Subject has received previous therapy for AML, with the exception of the following:
- Emergency leukapheresis
- Emergency treatment for hyperleukocytosis with hydroxyurea for ≤ 10 days
- Preemptive treatment with retinoic acid prior to exclusion of APL ≤ 7 days
- Growth factor or cytokine support
- Steroids for the treatment of hypersensitivity or transfusion reactions.
- Subject has QTcF interval > 450 ms (average of triplicate determinations based on central reading).
- Subject with long QT syndrome.
- Subject has clinically active central nervous system leukemia.
- Subject has had major surgery within 4 weeks prior to the first study dose.
- Subject has radiation therapy within 4 weeks prior to the first study dose.
- Subject has immediate life-threatening, severe complications of leukemia such as severe uncontrolled bleeding and/or severe disseminated intravascular coagulation
- Subject is known to have human immunodeficiency virus infection.
- Subject has active hepatitis B or C.
- Subject has an uncontrolled infection. An infection controlled with an approved or closely monitored antibiotic/antiviral/antifungal treatment is allowed.
- Subject has uncontrolled angina, severe uncontrolled ventricular arrhythmias, electrocardiographic evidence of acute ischemia, congestive heart failure New York Heart Association (NYHA) class 3 or 4 or subject has a history of congestive heart failure of NYHA class 3 or 4 and echocardiogram (ECHO) or Multiple Gate Acquisition (MUGA) scan performed within 3 months prior to screening or at screening showed a left ventricular ejection fraction (LVEF) of < 45%.
- Subject requires treatment with concomitant drugs that are strong inducers of cytochrome P450 (CYP) 3A.
- Subject requires treatment with concomitant drugs that target serotonin 5HT2B receptors or sigma nonspecific receptors, with the exception of drugs that are considered absolutely essential for treatment of the subject.
- Subject requires treatment with concomitant drugs that are strong inhibitors or inducers of P glycoprotein (P-gp) with the exception of drugs that are considered absolutely essential for the care of the subject.
- Subject has prior malignancies, except resected basal cell carcinoma or treated cervical carcinoma in situ. Cancer treated with curative intent ≥ 5 years previously will be allowed. Cancer treated with curative intent < 5 years previously will not be allowed.
- Subject has any condition which makes the subject unsuitable for study participation.
Sites / Locations
- Site JP81037
- Site JP00003
- Site JP81003
- Site JP81027
- Site JP81038
- Site JP81010
- Site JP81039
- Site JP81007
- Site JP00002
- Site JP81001
- Site JP81026
- Site JP81018
- Site JP81014
- Site JP81015
- Site JP81043
- Site JP00007
- Site JP81006
- Site JP81036
- Site JP81023
- Site JP81020
- Site JP81013
- Site JP00006
- Site JP81005
- Site JP81024
- Site JP81035
- SIte JP81011
- Site JP81041
- Site JP81022
- Site JP81040
- Site JP00005
- Site JP81032
- Site JP81029
- Site JP81008
- Site JP00001
- Site JP81004
- Site JP81025
- Site JP81031
- Site JP81030
- Site JP81033
- Site JP81028
- Site JP81016
- Site JP81012
- Site JP81009
- Site JP81019
- Site JP81021
- Site KR82002
- Site KR82001
- Site KR82003
- Site KR82004
- Site KR82005
- Site KR82006
- Site TW88604
- Site TW88602
- Site TW88601
- Site TW88603
Arms of the Study
Arm 1
Arm 2
Arm 3
Arm Type
Experimental
Experimental
Experimental
Arm Label
Phase 1 Dose Evaluation Part
Phase 1 Dose Expansion Part
Phase 2 Part
Arm Description
In the dose-evaluation part in Phase 1 part, subjects will receive ASP2215 at assigned single dose for determination of MTD and/or RED. Treatment of AML in this study is composed of 3 periods of therapy: remission induction (42-day cycles x 2 at maximum), consolidation (28-day cycles x 3 at maximum), and maintenance (28-day cycles x 26 at maximum). The decision of whether or not to proceed to the next dose will be made based on the occurrence of DLT during Cycle 1 of the induction period.
In the dose expansion part in Phase 1 part, subjects will receive ASP2215 at RED that has been determined in the dose-evaluation part, and the safety will be assessed based on the onset of DLTs during Cycle 1 of the induction and consolidation periods.
Subjects will receive ASP2215 at the recommended dose established in Phase 1 part.
Outcomes
Primary Outcome Measures
Phase 1 part: Maximum tolerated dose (MTD)
MTD is defined as the highest dose of ASP2215 at which the posterior mean of the Dose-Limiting Toxicity (DLT) incidence during Cycle 1 of induction therapy is estimated to be closest to 33%.
Phase 1 part: Recommended expansion dose (RED)
The sponsor will decide the RED considering the MTD, safety, pharmacokinetics, and efficacy of ASP2215. The final RED will be decided by the sponsor's responsible person by comprehensively assessing the data obtained from the study, and taking into account the discussion held between the sponsor, the medical expert, the investigator, and the advisor of medical statistics.
Phase 1 part: Number of participants with dose limiting toxicities (DLTs)
A DLT is defined as any Grade ≥ 3 non-hematologic or extramedullary toxicity or any events that require dose reduction of ASP2215 that occur during the DLT assessment period, and that is considered to be possibly, probably, or definitely related to induction or consolidation therapies including the study drugs. The DLT assessment period for making a decision of whether or not to proceed to the next dose is defined as the shorter of the following 2 periods: 39 days from the start of the treatment with ASP2215 in the induction period or days between the start of induction therapy and the start of the first consolidation therapy. For safety assessment during the expansion part, the DLT assessment period includes Cycle 1 of consolidation therapy in addition to the period defined above.
Phase 1 part: Number of participants with Adverse Events (AEs)
AEs will be coded using Medical Dictionary for Regulatory Activities (MedDRA). A treatment-emergent adverse event (TEAE) is defined as an AE observed after starting administration of the investigational product (IP) and within 28 days after the last administration of IP for phase 1 part. An IP-related TEAE is defined as any TEAE with a causal relationship assessed as YES by the investigator.
AE is considered "serious" if the investigator or sponsor view any of the following outcomes: Death, life-threatening, persistent or significant disability/incapacity, congenital anomaly or birth defect, hospitalization, or medically important event.
Phase 1 part: Number of participants with laboratory value abnormalities and/or AEs
Number of participants with potentially clinically significant laboratory values.
Phase 1 part: Number of participants with vital sign abnormalities and/or AEs
Number of participants with potentially clinically significant vital sign values.
Phase 2 part: Complete remission (CR) rate after induction therapy period
CR is defined as a morphologically leukemia-free state at the post-baseline visit, having a neutrophil count of ≥ 1,000/mm^3 and platelet count of ≥ 100,000/mm^3, bone marrow blasts < 5%. There must be no evidence of Auer rods and no evidence of extramedullary leukemia. The blast counts in peripheral blood must be ≤ 2%.
Secondary Outcome Measures
Phase 1 part: Pharmacokinetics of ASP2215 in plasma: Maximum concentration (Cmax)
Cmax will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: Time to attain Cmax (tmax)
tmax will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: Area under plasma concentration-time curve from time 0 to 24 (AUC24)
AUC24 will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: Oral clearance (CL/F)
CL/F will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: AUC from time 0 to last measurable concentration (AUClast)
AUClast will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: Apparent terminal elimination half-life (t1/2)
t1/2 will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: Apparent Volume of Distribution During the Terminal Elimination Phase after Oral Dosing (Vz/F)
Vz/F will be recorded from the PK plasma samples collected.
Phase 1 part: PK of ASP2215 in plasma: Plasma trough concentration (Ctrough)
Ctrough will be recorded from the PK plasma samples collected.
Phase 1 part: PK of cytarabine in plasma: Ctrough
Ctrough will be recorded from the PK plasma samples collected.
Phase 2 part: PK of ASP2215 in plasma: Concentration
Concentration will be recorded from the PK plasma samples collected.
Phase 2 part: Duration of overall survival (OS)
OS is defined as the time from the date of first dose of day 1 to the date of death due to any cause. Patients still alive or lost to follow up will be censored at the time they were last known to be alive.
Phase 2 part: Duration of event free survival (EFS)
EFS is defined as the time from the date of first dose of study regimen (day 1) until the date of documented relapse, treatment failure or death from any cause, whichever occurs first. For a subject with none of these events, EFS is censored at the date of last disease assessment.
Phase 2 part: Duration of relapse free survival (RFS)
RFS is defined as time from the date of achievement of first CRc until relapse or death from any cause, whichever comes first. For a subject who is not known to have relapsed or died, RFS is censored on the date of last relapse-free disease assessment date.
Phase 2 part: CR rate after each treatment therapy
CR is defined as a morphologically leukemia-free state at the post-baseline visit, having a neutrophil count of ≥ 1,000/mm^3 and platelet count of ≥ 100,000/mm^3, bone marrow blasts < 5%. There must be no evidence of Auer rods and no evidence of extramedullary leukemia. The blast counts in peripheral blood must be ≤ 2%.
Phase 2 part: CR rate without minimal residual disease (MRD) after each treatment therapy
MRD will be measured from bone marrow samples taken at the screening visit, end of treatment/disease progression and from bone marrow samples taken at other time points during the study.
Phase 2 part: CR with partial hematological recovery (CRh) rate after each treatment therapy
CRh is defined as a condition at the post baseline visit, having bone marrow blasts < 5%, partial hematologic recovery neutrophil count≥ 500/mm^3 and platelet count ≥ 50,000/mm^3, no evidence of extramedullary leukemia and cannot be classified as CR. The blast counts in peripheral blood must be ≤ 2%.
Phase 2 part: Composite CR (CRc) rate after each treatment therapy
CRc is defined as total of CR, CR with incomplete platelet recovery (CRp) and + CR with incomplete hematologic recovery (CRi).
CRp is defined as a condition that meets all of the CR criteria at the post-baseline visit, except for the unrecovered platelet count (< 100,000/mm^3).
CRi is defined as a condition that meets all of the CR criteria at the post-baseline visit, except for the unrecovered neutrophil count (< 1,000/mm^3; whether or not having unrecovered platelet counts).
Phase 2 part: CR/CRh rate after each treatment therapy
CR is defined as a morphologically leukemia-free state at the post-baseline visit, having a neutrophil count of ≥ 1,000/mm^3 and platelet count of ≥ 100,000/mm^3, bone marrow blasts < 5%. There must be no evidence of Auer rods and no evidence of extramedullary leukemia. The blast counts in peripheral blood must be ≤ 2%. CRh is defined as a condition at the post baseline visit, having bone marrow blasts < 5%, partial hematologic recovery neutrophil count≥ 500/mm^3 and platelet count ≥ 50,000/mm^3, no evidence of extramedullary leukemia and cannot be classified as CR. The blast counts in peripheral blood must be ≤ 2%.
Phase 2 part: Duration of CR
Duration of CR is defined as the period from the first day of achieving CR to the first day of confirmed relapse.
Phase 2 part: Duration of CR/CRh
Duration of CR/CRh is defined as the period from the first day of achieving CR or CRh to the first day of confirmed relapse.
Phase 2 part: Duration of CRh
Duration of CRh is defined as the period from the first day of achieving CRh to the first day of confirmed relapse.
Phase 2 part: Duration of CRc
Duration of CRc is defined as the period from the first day of achieving CRc to the first day of confirmed relapse.
Phase 2 part: Duration of response
Duration of response is defined as the period from the first day of achieving CR, CRp, CRi, or PR to the first day of confirmed relapse.
Phase 2 part: Number of participants with AEs
AEs will be coded using MedDRA. A TEAE is defined as an AE observed after starting administration of the IP and within 30 days after the last administration of IP for phase 2 part. An IP-related TEAE is defined as any TEAE with a causal relationship assessed as YES by the investigator.
AE is considered "serious" if the investigator or sponsor view any of the following outcomes: Death, life-threatening, persistent or significant disability/incapacity, congenital anomaly or birth defect, hospitalization, or medically important event.
Phase 2 part: Number of participants with laboratory value abnormalities and/or AEs
Number of participants with potentially clinically significant laboratory values.
Phase 2 part: Number of participants with vital sign abnormalities and/or AEs
Number of participants with potentially clinically significant vital sign values.
Phase 2 part: Number of participants with 12- ECG abnormalities and/or AEs
Number of participants with potentially clinically significant 12-ECG values.
Full Information
1. Study Identification
Unique Protocol Identification Number
NCT02310321
Brief Title
A Study of ASP2215 in Combination With Induction and Consolidation Chemotherapy in Patients With Newly Diagnosed Acute Myeloid Leukemia.
Official Title
A Phase 1/2 Study of ASP2215 in Combination With Induction and Consolidation Chemotherapy in Patients With Newly Diagnosed Acute Myeloid Leukemia
Study Type
Interventional
2. Study Status
Record Verification Date
October 2023
Overall Recruitment Status
Active, not recruiting
Study Start Date
February 26, 2015 (Actual)
Primary Completion Date
August 25, 2021 (Actual)
Study Completion Date
December 31, 2024 (Anticipated)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Astellas Pharma Inc
4. Oversight
Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Product Manufactured in and Exported from the U.S.
Yes
Data Monitoring Committee
Yes
5. Study Description
Brief Summary
The purpose of phase 1 part in this study is to determine the maximum tolerated dose (MTD) and/or recommended expansion dose (RED) of ASP2215 concomitant with cytarabine/idarubicin as induction chemotherapy based on the status of the onset of dose-limiting toxicity (DLT) in newly diagnosed Acute Myeloid Leukemia (AML) subjects. Phase 1 part will also evaluate safety and tolerability and characterize the pharmacokinetic (PK) parameters of ASP2215 concomitant with induction and consolidation chemotherapy as well as evaluate the PK parameters of cytarabine concomitant with ASP2215.
The purpose of phase 2 part is to evaluate efficacy of ASP2215 in combination with induction therapy. Phase 2 cohort will also evaluate safety and characterize the PK parameters of ASP2215 in combination with induction and consolidation therapy followed by maintenance therapy in newly diagnosed FLT3-mutated AML subjects.
Detailed Description
This study is composed of Phase 1 part (the dose-evaluation part and the expansion part) and Phase 2 part.
In the dose-evaluation part of Phase 1 part, at least 3 subjects will receive ASP2215 at each dose (low, middle, and high) for determination of MTD and/or RED. Treatment of AML in Phase 1 part is composed of 3 periods of therapy: remission induction, consolidation, and maintenance. The decision of whether or not to proceed to the next dose will be made based on the occurrence of DLT during Cycle 1 of the induction period.
In the expansion part of Phase 1 part, a maximum of 3 subjects will receive ASP2215 at RED that has been recommended in the dose-evaluation part and the safety will be assessed based on the onset of DLTs during Cycle 1 of the induction and consolidation periods.
In Phase 2 part, Subjects will receive ASP2215 at the recommended dose established in Phase 1 part. The target population will be limited to newly diagnosed FLT3-mutated AML.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Acute Myeloid Leukemia, FLT3-mutated Acute Myeloid Leukemia
Keywords
Acute Myeloid Leukemia, Cytarabine, Idarubicin, ASP2215
7. Study Design
Primary Purpose
Treatment
Study Phase
Phase 1, Phase 2
Interventional Study Model
Sequential Assignment
Masking
None (Open Label)
Allocation
Non-Randomized
Enrollment
84 (Actual)
8. Arms, Groups, and Interventions
Arm Title
Phase 1 Dose Evaluation Part
Arm Type
Experimental
Arm Description
In the dose-evaluation part in Phase 1 part, subjects will receive ASP2215 at assigned single dose for determination of MTD and/or RED. Treatment of AML in this study is composed of 3 periods of therapy: remission induction (42-day cycles x 2 at maximum), consolidation (28-day cycles x 3 at maximum), and maintenance (28-day cycles x 26 at maximum). The decision of whether or not to proceed to the next dose will be made based on the occurrence of DLT during Cycle 1 of the induction period.
Arm Title
Phase 1 Dose Expansion Part
Arm Type
Experimental
Arm Description
In the dose expansion part in Phase 1 part, subjects will receive ASP2215 at RED that has been determined in the dose-evaluation part, and the safety will be assessed based on the onset of DLTs during Cycle 1 of the induction and consolidation periods.
Arm Title
Phase 2 Part
Arm Type
Experimental
Arm Description
Subjects will receive ASP2215 at the recommended dose established in Phase 1 part.
Intervention Type
Drug
Intervention Name(s)
gilteritinib
Other Intervention Name(s)
Xospata, ASP2215
Intervention Description
Once-daily oral administration on 14 consecutive days in every cycle in each period.
Intervention Type
Drug
Intervention Name(s)
Idarubicin
Intervention Description
Induction period: Once-daily intravenous injection of 12 mg/m^2 idarubicin on 3 consecutive days.
Intervention Type
Drug
Intervention Name(s)
Cytarabine
Intervention Description
Induction period: Once-daily intravenous injection of 100 mg/m^2 cytarabine on 7 consecutive days.
Consolidation period: Twice-daily intravenous injection of 1.5 g/m^2 cytarabine on Days 1, 3, and 5.
Primary Outcome Measure Information:
Title
Phase 1 part: Maximum tolerated dose (MTD)
Description
MTD is defined as the highest dose of ASP2215 at which the posterior mean of the Dose-Limiting Toxicity (DLT) incidence during Cycle 1 of induction therapy is estimated to be closest to 33%.
Time Frame
Up to 42 days
Title
Phase 1 part: Recommended expansion dose (RED)
Description
The sponsor will decide the RED considering the MTD, safety, pharmacokinetics, and efficacy of ASP2215. The final RED will be decided by the sponsor's responsible person by comprehensively assessing the data obtained from the study, and taking into account the discussion held between the sponsor, the medical expert, the investigator, and the advisor of medical statistics.
Time Frame
Up to 42 days
Title
Phase 1 part: Number of participants with dose limiting toxicities (DLTs)
Description
A DLT is defined as any Grade ≥ 3 non-hematologic or extramedullary toxicity or any events that require dose reduction of ASP2215 that occur during the DLT assessment period, and that is considered to be possibly, probably, or definitely related to induction or consolidation therapies including the study drugs. The DLT assessment period for making a decision of whether or not to proceed to the next dose is defined as the shorter of the following 2 periods: 39 days from the start of the treatment with ASP2215 in the induction period or days between the start of induction therapy and the start of the first consolidation therapy. For safety assessment during the expansion part, the DLT assessment period includes Cycle 1 of consolidation therapy in addition to the period defined above.
Time Frame
Up to 42 days
Title
Phase 1 part: Number of participants with Adverse Events (AEs)
Description
AEs will be coded using Medical Dictionary for Regulatory Activities (MedDRA). A treatment-emergent adverse event (TEAE) is defined as an AE observed after starting administration of the investigational product (IP) and within 28 days after the last administration of IP for phase 1 part. An IP-related TEAE is defined as any TEAE with a causal relationship assessed as YES by the investigator.
AE is considered "serious" if the investigator or sponsor view any of the following outcomes: Death, life-threatening, persistent or significant disability/incapacity, congenital anomaly or birth defect, hospitalization, or medically important event.
Time Frame
Up to 9 months
Title
Phase 1 part: Number of participants with laboratory value abnormalities and/or AEs
Description
Number of participants with potentially clinically significant laboratory values.
Time Frame
Up to 9 months
Title
Phase 1 part: Number of participants with vital sign abnormalities and/or AEs
Description
Number of participants with potentially clinically significant vital sign values.
Time Frame
Up to 9 months
Title
Phase 2 part: Complete remission (CR) rate after induction therapy period
Description
CR is defined as a morphologically leukemia-free state at the post-baseline visit, having a neutrophil count of ≥ 1,000/mm^3 and platelet count of ≥ 100,000/mm^3, bone marrow blasts < 5%. There must be no evidence of Auer rods and no evidence of extramedullary leukemia. The blast counts in peripheral blood must be ≤ 2%.
Time Frame
Up to 4 months
Secondary Outcome Measure Information:
Title
Phase 1 part: Pharmacokinetics of ASP2215 in plasma: Maximum concentration (Cmax)
Description
Cmax will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: Time to attain Cmax (tmax)
Description
tmax will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: Area under plasma concentration-time curve from time 0 to 24 (AUC24)
Description
AUC24 will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: Oral clearance (CL/F)
Description
CL/F will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: AUC from time 0 to last measurable concentration (AUClast)
Description
AUClast will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: Apparent terminal elimination half-life (t1/2)
Description
t1/2 will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: Apparent Volume of Distribution During the Terminal Elimination Phase after Oral Dosing (Vz/F)
Description
Vz/F will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of ASP2215 in plasma: Plasma trough concentration (Ctrough)
Description
Ctrough will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 1 part: PK of cytarabine in plasma: Ctrough
Description
Ctrough will be recorded from the PK plasma samples collected.
Time Frame
Up to 9 months
Title
Phase 2 part: PK of ASP2215 in plasma: Concentration
Description
Concentration will be recorded from the PK plasma samples collected.
Time Frame
Up to 135 days
Title
Phase 2 part: Duration of overall survival (OS)
Description
OS is defined as the time from the date of first dose of day 1 to the date of death due to any cause. Patients still alive or lost to follow up will be censored at the time they were last known to be alive.
Time Frame
Up to 41 months
Title
Phase 2 part: Duration of event free survival (EFS)
Description
EFS is defined as the time from the date of first dose of study regimen (day 1) until the date of documented relapse, treatment failure or death from any cause, whichever occurs first. For a subject with none of these events, EFS is censored at the date of last disease assessment.
Time Frame
Up to 41 months
Title
Phase 2 part: Duration of relapse free survival (RFS)
Description
RFS is defined as time from the date of achievement of first CRc until relapse or death from any cause, whichever comes first. For a subject who is not known to have relapsed or died, RFS is censored on the date of last relapse-free disease assessment date.
Time Frame
Up to 41 months
Title
Phase 2 part: CR rate after each treatment therapy
Description
CR is defined as a morphologically leukemia-free state at the post-baseline visit, having a neutrophil count of ≥ 1,000/mm^3 and platelet count of ≥ 100,000/mm^3, bone marrow blasts < 5%. There must be no evidence of Auer rods and no evidence of extramedullary leukemia. The blast counts in peripheral blood must be ≤ 2%.
Time Frame
Up to 34 months
Title
Phase 2 part: CR rate without minimal residual disease (MRD) after each treatment therapy
Description
MRD will be measured from bone marrow samples taken at the screening visit, end of treatment/disease progression and from bone marrow samples taken at other time points during the study.
Time Frame
Up to 34 months
Title
Phase 2 part: CR with partial hematological recovery (CRh) rate after each treatment therapy
Description
CRh is defined as a condition at the post baseline visit, having bone marrow blasts < 5%, partial hematologic recovery neutrophil count≥ 500/mm^3 and platelet count ≥ 50,000/mm^3, no evidence of extramedullary leukemia and cannot be classified as CR. The blast counts in peripheral blood must be ≤ 2%.
Time Frame
Up to 34 months
Title
Phase 2 part: Composite CR (CRc) rate after each treatment therapy
Description
CRc is defined as total of CR, CR with incomplete platelet recovery (CRp) and + CR with incomplete hematologic recovery (CRi).
CRp is defined as a condition that meets all of the CR criteria at the post-baseline visit, except for the unrecovered platelet count (< 100,000/mm^3).
CRi is defined as a condition that meets all of the CR criteria at the post-baseline visit, except for the unrecovered neutrophil count (< 1,000/mm^3; whether or not having unrecovered platelet counts).
Time Frame
Up to 34 months
Title
Phase 2 part: CR/CRh rate after each treatment therapy
Description
CR is defined as a morphologically leukemia-free state at the post-baseline visit, having a neutrophil count of ≥ 1,000/mm^3 and platelet count of ≥ 100,000/mm^3, bone marrow blasts < 5%. There must be no evidence of Auer rods and no evidence of extramedullary leukemia. The blast counts in peripheral blood must be ≤ 2%. CRh is defined as a condition at the post baseline visit, having bone marrow blasts < 5%, partial hematologic recovery neutrophil count≥ 500/mm^3 and platelet count ≥ 50,000/mm^3, no evidence of extramedullary leukemia and cannot be classified as CR. The blast counts in peripheral blood must be ≤ 2%.
Time Frame
Up to 34 months
Title
Phase 2 part: Duration of CR
Description
Duration of CR is defined as the period from the first day of achieving CR to the first day of confirmed relapse.
Time Frame
Up to 41 months
Title
Phase 2 part: Duration of CR/CRh
Description
Duration of CR/CRh is defined as the period from the first day of achieving CR or CRh to the first day of confirmed relapse.
Time Frame
Up to 41 months
Title
Phase 2 part: Duration of CRh
Description
Duration of CRh is defined as the period from the first day of achieving CRh to the first day of confirmed relapse.
Time Frame
Up to 41 months
Title
Phase 2 part: Duration of CRc
Description
Duration of CRc is defined as the period from the first day of achieving CRc to the first day of confirmed relapse.
Time Frame
Up to 41 months
Title
Phase 2 part: Duration of response
Description
Duration of response is defined as the period from the first day of achieving CR, CRp, CRi, or PR to the first day of confirmed relapse.
Time Frame
Up to 41 months
Title
Phase 2 part: Number of participants with AEs
Description
AEs will be coded using MedDRA. A TEAE is defined as an AE observed after starting administration of the IP and within 30 days after the last administration of IP for phase 2 part. An IP-related TEAE is defined as any TEAE with a causal relationship assessed as YES by the investigator.
AE is considered "serious" if the investigator or sponsor view any of the following outcomes: Death, life-threatening, persistent or significant disability/incapacity, congenital anomaly or birth defect, hospitalization, or medically important event.
Time Frame
Up to 35 months
Title
Phase 2 part: Number of participants with laboratory value abnormalities and/or AEs
Description
Number of participants with potentially clinically significant laboratory values.
Time Frame
Up to 35 months
Title
Phase 2 part: Number of participants with vital sign abnormalities and/or AEs
Description
Number of participants with potentially clinically significant vital sign values.
Time Frame
Up to 35 months
Title
Phase 2 part: Number of participants with 12- ECG abnormalities and/or AEs
Description
Number of participants with potentially clinically significant 12-ECG values.
Time Frame
Up to 35 months
10. Eligibility
Sex
All
Minimum Age & Unit of Time
18 Years
Maximum Age & Unit of Time
69 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
[Phase 1 part]
Subject is defined as having previously untreated de novo AML according to the World Health Organization (WHO) criteria (2008) within 28 days prior to study enrollment.
Subject has an Eastern Cooperative Oncology Group (ECOG) performance status of ≤ 2.
Subject must meet all of the following criteria in the laboratory test at screening:
Serum aspartate aminotransferase (AST) and alanine aminotransferase (ALT) levels of ≤ 2.5 × institutional upper limit of normal (ULN)
Total serum bilirubin level of ≤ 1.5 × institutional ULN
Serum creatinine level of ≤ 1.5 × institutional ULN or an estimated glomerular filtration rate (eGFR) of > 50 mL/min
Subject is suitable for oral administration of ASP2215.
Female subject falls under the following:
Of non-childbearing potential:
・Post-menopausal (defined as at least 1 year with no menses without a medical reason such as drug administration) at screening, or
・Documented surgically sterile or status post-hysterectomy (at least 1 month prior to screening)
Of childbearing potential:
・Has a negative result for the pregnancy test at screening, and
・Agrees to use an appropriate contraception starting at screening and throughout the study period and for 60 days after the final study drug administration
Female subject agrees not to breastfeed starting at screening and throughout the study period and for 60 days after the final study drug administration.
Female subject agrees not to donate ova starting at screening and throughout the study period and for 60 days after the final study drug administration.
Male subject and his female spouse/partner who is of childbearing potential agrees to use an appropriate contraception starting at screening and throughout the study period and for 120 days after the final study drug administration.
Male subject agrees not to donate sperm starting at screening and throughout the study period and for 120 days after the final study drug administration.
Subject agrees not to participate in another interventional study while on study treatment.
Subject can be admitted during the induction period.
[Phase 2 part]
Subject has a diagnosis of previously-untreated de novo acute myeloid leukemia (AML) according to World Health Organization (WHO) classification (2017) documented within 28 days prior to enrollment.
Subject is positive for FLT3-ITD and/or TKD mutation in bone marrow or whole blood as determined by the central lab. Registration by the local lab result is not acceptable.
Subject has an ECOG performance status (PS) 0 to 1. Subject who has an ECOG PS 2 is eligible only if the primary disease related symptoms such as pneumonia and febrile neutropenia are the cause of PS score.
Subject is suitable for oral administration of ASP2215.
Female subject is not pregnant and at least 1 of the following conditions apply:
Not a woman of childbearing potential (WOCBP)
WOCBP who agrees to follow the contraceptive guidance from the time of informed consent through at least 180 days after final study treatment administration.
Female subject must agree not to breastfeed starting at screening and throughout the study period, and for 60 days after the final study drug administration.
Female subject must not donate ova starting at screening and throughout the study period, and for 180 days after the final study drug administration.
Male subject and their female partners who are of childbearing potential must be using highly effective contraception per locally accepted standards in addition to a barrier method starting at screening and continue throughout the study period and for 120 days after the final study drug administration.
Male subject must not donate sperm starting at screening and throughout the study period and for 120 days after the final study drug administration.
Male subject with pregnant partner(s) must agree to remain abstinent or use a condom for the duration of the pregnancy throughout the study period and for 120 days after the final study treatment administration.
Subject agrees not to participate in another interventional study while on treatment.
Subject must meet the following criteria as indicated on the clinical laboratory tests:
Serum creatinine ≤ 1.5 × institutional upper limit of normal (ULN), or if serum creatinine outside normal range, then glomerular filtration rate (GFR) > 50 mL/min/1.73m^2 as calculated with the 4-parameter Modification of Diet in Renal Disease (MDRD) equation.
Serum total bilirubin ≤ 2.5 mg/dL (43 μmol/L), except for subjects with Gilbert's syndrome.
Serum aspartate aminotransferase (AST) and alanine aminotransferase (ALT) < 3 x ULN. If liver abnormality by the primary disease is suspected, subject may be pre-registered to initiate the chemotherapy. Prior to registration, AST/ALT values must meet the criteria to continue the study.
Serum magnesium ≥ institutional lower limit of normal (LLN). Subject may pre-register without magnesium value, but subject must meet the criteria prior to the full registration on Day 8.
Serum potassium ≥ institutional lower limit of normal (LLN).
Exclusion Criteria:
[Phase 1 part]
Subject was diagnosed with acute promyelocytic leukemia (APL).
Subject has breakpoint cluster region-abelson (BCR-ABL)-positive leukemia (chronic myelogenous leukemia in blast crisis).
Subject has active malignant tumors other than AML or myelodysplastic syndrome (MDS).
Subject has received prior AML treatment except for the following:
Urgent leukapheresis
Hydroxyurea administration for emergency treatment of hyperleukocytosis (≤ 7 days)
Administration of retinoic acid before the diagnosis to exclude APL (≤ 7 days)
Supportive care using growth factors or cytokines
Steroid administration to treat hypersensitivity or blood transfusion reactions
Subject has clinically active central nervous system leukemia.
Subject has disseminated intravascular coagulation (DIC).
Subject has had major surgery within 28 days prior to the first study drug administration.
Subject has had radiation therapy within 28 days prior to the first study drug administration.
Subject has congestive heart failure of New York Heart Association (NYHA) class 3 or 4, or subject with a past history of congestive heart failure of NYHA class 3 or 4 and in whom echocardiogram (ECHO) or Multiple Gate Acquisition (MUGA) scan performed within 3 months prior to screening or at screening showed a left ventricular ejection fraction (LVEF) of < 45%.
Subject has cardiac impairment or a clinically significant cardiac disease, including any one of the following:
Complete left bundle branch block
Obligate use of a cardiac pacemaker
Long QT syndrome at Screening
Prolongation of the QTc interval (> 450 ms) on electrocardiogram (ECG) at screening
Right bundle branch block + left anterior hemiblock (bifascicular block)
Angina pectoris within 3 months prior to study drug administration
Acute myocardial infarction within 3 months prior to study drug administration
Subject requires treatment with concomitant drugs that are strong inducers of cytochrome P450 (CYP)3A.
Subject requires treatment with concomitant drugs that are strong inhibitors or inducers of P glycoprotein (P-gp) with the exception of drugs that are considered absolutely essential for the care of the subject.
Subject requires treatment with concomitant drugs that target serotonin 5HT1 or 5HT2B receptors or sigma receptors, with the exception of drugs that are considered absolutely essential for treatment of the subject.
Subject has an active uncontrollable infection.
Subject is known to have human immunodeficiency virus (HIV) infection.
Subject has active hepatitis B or C or other active hepatic disorders.
Subject has any condition that, in the investigator's or sub-investigator's opinion, makes the subject unsuitable for study participation.
Potassium and magnesium levels of below institutional lower limit of normal in the laboratory test at screening.
[Phase 2 part]
Subject was diagnosed with acute promyelocytic leukemia (APL).
Subject has known BCR-ABL-positive leukemia (chronic myelogenous leukemia in blast crisis).
Subject has therapy-related AML.
Subject has active malignant tumors other than AML.
Subject has received previous therapy for AML, with the exception of the following:
Emergency leukapheresis
Emergency treatment for hyperleukocytosis with hydroxyurea for ≤ 10 days
Preemptive treatment with retinoic acid prior to exclusion of APL ≤ 7 days
Growth factor or cytokine support
Steroids for the treatment of hypersensitivity or transfusion reactions.
Subject has QTcF interval > 450 ms (average of triplicate determinations based on central reading).
Subject with long QT syndrome.
Subject has clinically active central nervous system leukemia.
Subject has had major surgery within 4 weeks prior to the first study dose.
Subject has radiation therapy within 4 weeks prior to the first study dose.
Subject has immediate life-threatening, severe complications of leukemia such as severe uncontrolled bleeding and/or severe disseminated intravascular coagulation
Subject is known to have human immunodeficiency virus infection.
Subject has active hepatitis B or C.
Subject has an uncontrolled infection. An infection controlled with an approved or closely monitored antibiotic/antiviral/antifungal treatment is allowed.
Subject has uncontrolled angina, severe uncontrolled ventricular arrhythmias, electrocardiographic evidence of acute ischemia, congestive heart failure New York Heart Association (NYHA) class 3 or 4 or subject has a history of congestive heart failure of NYHA class 3 or 4 and echocardiogram (ECHO) or Multiple Gate Acquisition (MUGA) scan performed within 3 months prior to screening or at screening showed a left ventricular ejection fraction (LVEF) of < 45%.
Subject requires treatment with concomitant drugs that are strong inducers of cytochrome P450 (CYP) 3A.
Subject requires treatment with concomitant drugs that target serotonin 5HT2B receptors or sigma nonspecific receptors, with the exception of drugs that are considered absolutely essential for treatment of the subject.
Subject requires treatment with concomitant drugs that are strong inhibitors or inducers of P glycoprotein (P-gp) with the exception of drugs that are considered absolutely essential for the care of the subject.
Subject has prior malignancies, except resected basal cell carcinoma or treated cervical carcinoma in situ. Cancer treated with curative intent ≥ 5 years previously will be allowed. Cancer treated with curative intent < 5 years previously will not be allowed.
Subject has any condition which makes the subject unsuitable for study participation.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Medical Director
Organizational Affiliation
Astellas Pharma Inc
Official's Role
Study Director
Facility Information:
Facility Name
Site JP81037
City
Anjo
State/Province
Aichi
Country
Japan
Facility Name
Site JP00003
City
Nagoya
State/Province
Aichi
Country
Japan
Facility Name
Site JP81003
City
Nagoya
State/Province
Aichi
Country
Japan
Facility Name
Site JP81027
City
Nagoya
State/Province
Aichi
Country
Japan
Facility Name
Site JP81038
City
Toyohashi
State/Province
Aichi
Country
Japan
Facility Name
Site JP81010
City
Narita
State/Province
Chiba
Country
Japan
Facility Name
Site JP81039
City
Matsuyama
State/Province
Ehime
Country
Japan
Facility Name
Site JP81007
City
Yoshida-gun
State/Province
Fukui
Country
Japan
Facility Name
Site JP00002
City
Maebashi
State/Province
Gunma
Country
Japan
Facility Name
Site JP81001
City
Maebshi
State/Province
Gunma
Country
Japan
Facility Name
Site JP81026
City
Fukuyama
State/Province
Hiroshima
Country
Japan
Facility Name
Site JP81018
City
Otake
State/Province
Hiroshima
Country
Japan
Facility Name
Site JP81014
City
Sapporo
State/Province
Hokkaido
Country
Japan
Facility Name
Site JP81015
City
Sapporo
State/Province
Hokkaido
Country
Japan
Facility Name
Site JP81043
City
Himeji
State/Province
Hyogo
Country
Japan
Facility Name
Site JP00007
City
Kobe
State/Province
Hyogo
Country
Japan
Facility Name
Site JP81006
City
Kobe
State/Province
Hyogo
Country
Japan
Facility Name
Site JP81036
City
Mito
State/Province
Ibaraki
Country
Japan
Facility Name
Site JP81023
City
Tsukuba
State/Province
Ibaraki
Country
Japan
Facility Name
Site JP81020
City
Kanazawa
State/Province
Ishikawa
Country
Japan
Facility Name
Site JP81013
City
Isehara
State/Province
Kanagawa
Country
Japan
Facility Name
Site JP00006
City
Yokohama
State/Province
Kanagawa
Country
Japan
Facility Name
Site JP81005
City
Yokohama
State/Province
Kanagawa
Country
Japan
Facility Name
Site JP81024
City
Yokohama
State/Province
Kanagawa
Country
Japan
Facility Name
Site JP81035
City
Sendai
State/Province
Miyagi
Country
Japan
Facility Name
SIte JP81011
City
Omura
State/Province
Nagasaki
Country
Japan
Facility Name
Site JP81041
City
Tenri
State/Province
Nara
Country
Japan
Facility Name
Site JP81022
City
Shimono
State/Province
Tochigi
Country
Japan
Facility Name
Site JP81040
City
Bunkyo-ku
State/Province
Tokyo
Country
Japan
Facility Name
Site JP00005
City
Shinagawa-ku
State/Province
Tokyo
Country
Japan
Facility Name
Site JP81032
City
Shinagawa-ku
State/Province
Tokyo
Country
Japan
Facility Name
Site JP81029
City
Akita
Country
Japan
Facility Name
Site JP81008
City
Chiba
Country
Japan
Facility Name
Site JP00001
City
Fukuoka
Country
Japan
Facility Name
Site JP81004
City
Fukuoka
Country
Japan
Facility Name
Site JP81025
City
Fukuoka
Country
Japan
Facility Name
Site JP81031
City
Fukushima
Country
Japan
Facility Name
Site JP81030
City
Gifu
Country
Japan
Facility Name
Site JP81033
City
Kochi
Country
Japan
Facility Name
Site JP81028
City
Kumamoto
Country
Japan
Facility Name
Site JP81016
City
Kyoto
Country
Japan
Facility Name
Site JP81012
City
Nagasaki
Country
Japan
Facility Name
Site JP81009
City
Okayama
Country
Japan
Facility Name
Site JP81019
City
Osaka
Country
Japan
Facility Name
Site JP81021
City
Osaka
Country
Japan
Facility Name
Site KR82002
City
Incheon
Country
Korea, Republic of
Facility Name
Site KR82001
City
Seoul
Country
Korea, Republic of
Facility Name
Site KR82003
City
Seoul
Country
Korea, Republic of
Facility Name
Site KR82004
City
Seoul
Country
Korea, Republic of
Facility Name
Site KR82005
City
Seoul
Country
Korea, Republic of
Facility Name
Site KR82006
City
Seoul
Country
Korea, Republic of
Facility Name
Site TW88604
City
Kaohsiung
Country
Taiwan
Facility Name
Site TW88602
City
Taichung
Country
Taiwan
Facility Name
Site TW88601
City
Tainan
Country
Taiwan
Facility Name
Site TW88603
City
Taoyuan
Country
Taiwan
12. IPD Sharing Statement
Plan to Share IPD
Yes
IPD Sharing Plan Description
Access to anonymized individual participant level data collected during the study, in addition to study-related supporting documentation, is planned for studies conducted with approved product indications and formulations, as well as compounds terminated during development. Studies conducted with product indications or formulations that remain active in development are assessed after study completion to determine if Individual Participant Data can be shared. Conditions and exceptions are described under the Sponsor Specific Details for Astellas on www.clinicalstudydatarequest.com.
IPD Sharing Time Frame
Access to participant level data is offered to researchers after publication of the primary manuscript (if applicable) and is available as long as Astellas has legal authority to provide the data.
IPD Sharing Access Criteria
Researchers must submit a proposal to conduct a scientifically relevant analysis of the study data. The research proposal is reviewed by an Independent Research Panel. If the proposal is approved, access to the study data is provided in a secure data sharing environment after receipt of a signed Data Sharing Agreement.
IPD Sharing URL
https://www.clinicalstudydatarequest.com/
Learn more about this trial
A Study of ASP2215 in Combination With Induction and Consolidation Chemotherapy in Patients With Newly Diagnosed Acute Myeloid Leukemia.
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