Leukemia, Myeloid, Acute Clinical Trial
Official title:
A Phase I/II Multi-center Study of HDM201 Added to Chemotherapy in Adult Subjects With Relapsed/Refractory (R/R) or Newly Diagnosed Acute Myeloid Leukemia (AML)
| Verified date | January 2020 |
| Source | Novartis |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
This is a multi-center open-label Phase I/II study investigating orally administered HDM201 in combination with chemotherapy in two populations: subjects with first line AML or subjects with relapsed/refractory AML. This study is conducted in three parts: dose escalation, dose expansion and DDI study.
| Status | Withdrawn |
| Enrollment | 0 |
| Est. completion date | June 13, 2023 |
| Est. primary completion date | July 22, 2021 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years and older |
| Eligibility |
Inclusion Criteria: All Subjects - Signed informed consent must be obtained prior to participation in the study - Age =18 - Diagnosis of AML based on WHO 2016 classification. Patients with APL (acute promyelocytic leukemia) with PML-RARA are not eligible. - Eastern Cooperative Oncology Group (ECOG) Performance Status (PS) that is 0 - 2. - Adequate organ functions - Left ventricular ejection fraction > 45% For 1L AML population: - For Part 1 or Part 2 Expansion Cohorts 1 or 2: subjects with de novo AML suitable for induction treatment with cytarabine and anthracyclines as per investigator judgement - For Part 2 Expansion Cohort 2: documented presence of FLT3 mutation (ITD or TKD ) and suitable for midostaurin treatment as per investigator judgement. - For Part 2 Expansion Cohort 3: Subjects with secondary AML (e.g. AML-MRC , secondary to myelodysplasia/MDS or therapy-related AML). Prior use of hypomethylating agents or other therapies with curative intent for treatment previous hematological malignancies or therapy-related AML is allowed. Subjects suitable for induction treatment with liposomal cytarabine/daunorubicin as per investigator judgement. For R/R AML population: - All Parts: Diagnosis of relapsed or refractory AML and suitable for treatment with IDAC as per investigator judgement. - For Part 3 only: willingness and suitability to participate in DDI Cohort 1 or 2. Exclusion Criteria: - Prior exposure to MDM2 and MDM4 inhibitor (e.g. idasanutlin) - Known symptomatic CNS leukemia not controlled by adequate therapy. - Isolated extramedullary leukemia - Subjects with prior malignancy (some exceptions apply) - QTcF > 470 ms at screening - Subjects who require treatment with moderate or strong CYP3A4 inducers within 14 days prior to starting study treatment or during the study - Subjects who require use of herbal preparations/medications and dietary supplements within 7 days prior to first dose and during the study - Subjects who require treatment with substrates of CYP3A4/5 with narrow therapeutic index (within 24 hours prior to during and 48 hours after HDM201 administration) - Subjects who require treatment with moderate or strong CYP3A4 inhibitors within 48 hours prior to, during and 48 hours post HDM201 administration. (except for Part 3 DDI Cohort 1 and 2) - Subject is pregnant or breastfeeding - WOCBP unless using highly effective methods of contraception during study treatment and for an appropriate time period after last study treatment - Sexually active males unless they use a condom during intercourse while taking study drug and for an appropriate time period after last study treatment For Part 1 only: - Subjects with a known favorable risk AML subtype at screening or subjects with FLT3 mutation For Part 3 only: - DDI Cohort 1: use of posaconazole (other than the planned dosing required by the protocol) within 7 days prior to start of the DDI investigation and for the duration of the DDI period - DDI Cohort 2: use of midazolam (other than the planned dosing required by the protocol) within 2 days prior to start of the DDI investigation and for the duration of the DDI period - DDI Cohort 1 and 2: subjects who have received, or are expected to receive moderate or strong inhibitors of CYP3A4 within 7 days prior to start of the DDI investigation, for the duration of the investigation, and 24 hours after last blood sample collection for PK assessment Other protocol-defined inclusion/exclusion may apply. |
| Country | Name | City | State |
|---|---|---|---|
| n/a | |||
| Lead Sponsor | Collaborator |
|---|---|
| Novartis Pharmaceuticals |
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Part 1 - Incidence of dose limiting toxicity (DLT) | number of DLTs by dose regimen of first line (1L) acute myeloid leukemia (AML) subjects during induction treatment; number of DLTs by dose regimen of relapsed/refractory (R/R) AML subjects during treatment | first day of study treatment to 3 months after start of study treatment | |
| Primary | Part 1 - Time to DLT | time from first dose to onset of DLT by dose regimen of 1L AML and R/R AML subjects | first day of study treatment to 3 months after start of study treatment | |
| Primary | Part 1 - Incidence and severity of Adverse Events (AEs) | number and grade of AEs by dose regimen of 1L AML and R/R AML subjects during DLT observation period | first day of study treatment to 3 months after start of study treatment | |
| Primary | Part 2 - Incidence and severity of AEs/serious adverse events (SAEs) | number and grade of AEs/SAEs by expansion cohort | first day of study treatment until 8.5 months after start of study treatment | |
| Primary | Part 2 - Percentage of participants with complete remission (CR)/CR with incomplete recovery (CRi) with adequate blood count recovery (ABCR) | Percentage of participants with CR/CRi with ABCR at the end of induction treatment for Expansion Cohort 1, and at the end of treatment for Expansion Cohort 4 | first day of study treatment until 4.5 months after start of study treatment | |
| Primary | Part 2 - Incidence and severity of abnormal laboratory values | number and grade of abnormal laboratory results by expansion cohort | first day of study treatment until 8.5 months after start of study treatment | |
| Primary | Part 2 - Incidence and severity of abnormal electrocardiogram (ECG) results | number and severity of abnormal ECG results by expansion cohort | first day of study treatment until 8.5 months after start of study treatment | |
| Primary | Part 2 - Incidence and severity of abnormal vital signs | number and severity of abnormal vital signs by expansion cohort | first day of study treatment until 8.5 months after start of study treatment | |
| Primary | Part 3 - DDI Cohort 1 HDM201 Pharmacokinetics (PK) area under the curve (AUC) | determine HDM201 AUC from time zero to the last measurable concentration sampling time (AUClast) in Cycle 1 | first day of HDM201 dose to 10 days after start of HDM201 | |
| Primary | Part 3 - DDI Cohort 1 HDM201 PK maximum observed plasma concentration (Cmax) | determine HDM201 Cmax in Cycle 1 | first day of HDM201 dose to 10 days after start of HDM201 | |
| Primary | Part 3 - DDI Cohort 1 HDM201 PK average plasma concentration | determine HDM201 average plasma concentration in Cycle 1 | first day of HDM201 dose to 10 days after start of HDM201 | |
| Primary | Part 3 - DDI Cohort 1 HDM201 PK time of maximum observed plasma concentration (Tmax) | determine HDM201 Tmax in Cycle 1 | first day of HDM201 dose to 10 days after start of HDM201 | |
| Primary | Part 3 - DDI Cohort 2: midazolam PK AUC | determine midazolam AUC last and AUC from time zero to infinity (inf) | first dose of midazolam (Day-2) to 8 days after start of study treatment (HDM201) | |
| Primary | Part 3 - DDI Cohort 2: midazolam PK Cmax | determine midazolam Cmax | first dose of midazolam (Day-2) to 8 days after start of study treatment (HDM201) | |
| Secondary | Part 1 +2: HDM201 PK AUC | determine HDM201 AUC by dose regimen in Part 1, and Expansion Cohort in Part 2 | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 1 +2: HDM201 PK Cmax | determine Cmax of HDM201 by dose regimen in Part 2, and Expansion Cohort in Part 2 | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 1 +2: HDM201 PK Tmax | determine Tmax of HDM201 by dose regimen in Part 2, and Expansion Cohort in Part 2 | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 1 - incidence of AEs/SAEs | number and grade of AEs/SAEs, by dose regimen for 1L AML and R/R AML subjects during study treatment + 30 days | first day of study treatment to 8.5 months after start of study treatment | |
| Secondary | Part 2 - all Expansion Cohorts: time to platelet recovery | determine time to platelet recovery by Expansion Cohort for each cycle | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 2 - all Expansion Cohorts: time to neutrophil recovery | determine time to neutrophil recovery by Expansion Cohort for each cycle | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 2 - all Expansion Cohorts: overall survival | determine overall survival by Expansion Cohort | first day of study treatment to 3 years after last patient is enrolled to Part 2 | |
| Secondary | Part 2 - all Expansion Cohorts: event-free survival | determine event-free survival by Expansion Cohort | first day of study treatment to 3 years after last patient is enrolled to Part 2 | |
| Secondary | Part 2 - all Expansion Cohorts: Percentage of subjects receiving Hematopoietic stem cell transplant (HSCT) | percentage of subjects receiving HSCT after study treatment by Expansion Cohort. | first day of study treatment to 3 years after last patient was enrolled to Part 2 | |
| Secondary | Part 2 - Expansion Cohorts 1 to 3: disease-free survival (DFS) | determine DFS by Expansion Cohort | first day of study treatment to 3 years after last patient enrolled to Part 2 | |
| Secondary | Part 2 - Expansion Cohorts 1 to 3: cumulative incidence of relapse (CIR) | determine CIR by Expansion Cohort | first day of study treatment to 3 years after last patient enrolled to Part 2 | |
| Secondary | Part 2 - Expansion Cohorts 2 and 3 - proportion of subjects with CR/CRi with ABCR | proportion of subjects achieving CR or CRi with ABCR by Expansion Cohort | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 2 - Expansion Cohorts 1 and 2: proportion of subjects with minimal/measurable residual disease (MRD) negativity | proportion of subjects achieving MRD negativity by Expansion Cohort | first day of study treatment to 7.5 months after start of study treatment | |
| Secondary | Part 2 - expansion cohort 2: midostaurin PK AUC | determine midostaurin AUC | first day of study treatment to 7.5 month after start of study treatment | |
| Secondary | Part 2 - expansion cohort 2: midostaurin PK Cmax | determine midostaurin Cmax during induction and consolidation treatment | first day of study treatment to 7.5 month after start of study treatment | |
| Secondary | Part 2 - expansion cohort 2: midostaurin PK Tmax | determine midostaurin Tmax during induction and consolidation treatment | first day of study treatment to 7.5 month after start of study treatment | |
| Secondary | Part 1 - incidence of abnormal laboratory values | number of abnormal laboratory results by dose regimen for 1L AML and R/R AML subjects during study treatment + 30 days | first day of study treatment to 8.5 months after start of study treatment | |
| Secondary | Part 1 - incidence of abnormal ECG results | number of abnormal ECG results by dose regimen for 1L AML and R/R AML subjects during study treatment + 30 days | first day of study treatment to 8.5 months after start of study treatment | |
| Secondary | Part 1 - incidence of abnormal vital signs | number of abnormal vital signs by dose regimen for 1L AML and R/R AML subjects during study treatment + 30 days | first day of study treatment to 8.5 months after start of study treatment |
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