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Genetically Engineered Cells (Obecabtagene Autoleucel) for the Treatment of B-cell Acute Lymphoblastic Leukemia in First Complete Remission without Measurable Residual Disease
Trial Status: active
This phase II trial tests the effect of obecabtagene autoleucel in treating patients with B-cell acute lymphoblastic leukemia (ALL) whose signs of cancer are gone (complete remission [CR]) and have no detectable cancer cells (measurable residual disease [MRD] negative). Obecabtagene autoleucel is a type of chimeric antigen receptor (CAR) T cell therapy. CAR T cell therapy is a type of treatment in which a patient's T cells (a type of immune system cell) are changed in the laboratory so they will attack cancer cells. T cells are taken from a patient’s blood. Then the gene for a special receptor that binds to a certain protein on the patient’s cancer cells is added to the T cells in the laboratory. The special receptor is called a CAR. Large numbers of the CAR T cells are grown in the laboratory and given to the patient by infusion for treatment of certain cancers. Obecabtagene autoleucel binds to a protein called CD19 which may help the body’s immune system kill cancer cells. Giving chemotherapy, such as fludarabine and cyclophosphamide, helps briefly weaken (suppress) the immune system and prepare the body for receiving the CAR T cell therapy. Giving obecabtagene autoleucel may be safe, tolerable, and/or effective in treating patients with B-cell ALL in first MRD negative CR.
Inclusion Criteria
Diagnosis of CD19+ B-cell ALL.
* Both Ph-negative and Ph-positive are allowed
* Patients with extramedullary disease (EMD) must have detectable disease in the bone marrow (by flow cytometry or molecular methods) in order to follow MRD
Patients aged ≥ 40 years at time of screening A
Patients aged 30-39 years (at time of screening A) are allowed in the presence of high-risk comorbidities or poor tolerability of chemotherapy (e.g. history or experienced pancreatitis with therapy, body mass index [BMI] ≥ 40kg/m^2, underlying liver disease precluding safer administration of pediatric inspired regimens, any further combination of documented severe comorbidities that the investigator judges to be incompatible with administering an intensive pediatric or pediatric-inspired standard chemotherapy regimen)
In MRD negative CR or CR with incomplete hematologic recovery (CRi) at the time of screening. MRD will be assessed by flow cytometry and/or molecular testing such as ClonoSEQ at the minimum sensitivity of 10^-4 from the bone marrow. Patients with MRD < 10^-4 will be eligible. If a patient has MRD ≥ 10^-4 by any modality at time of screening A, they will not be eligible
Patients may receive more than one course of upfront induction and/or consolidation, but must be in MRD- CR/CRi at time of screening, within 4 months from initiation of treatment. The 4-month window will be measured from the first day of anti-leukemic therapy initiation (excluding steroid prophase) until the screening A test for the trial. Frontline regimens include but are not limited to:
* Hyperfractionated cyclophosphamide, vincristine, doxorubicin, and dexamethasone (HyperCVAD) or mini-hyperfractionated cyclophosphamide, vincristine, and dexamethasone (hyper-CVD)
* Asparaginase-containing multiagent chemotherapy (e.g. CALGB10403, pediatric inspired chemotherapy [chemo])
* Inotuzumab or blinatumomab with or without chemotherapy
* Tyrosine kinase inhibitor plus steroids, chemotherapy, or blinatumomab
Alanine aminotransferase (ALT) or aspartate aminotransferase (AST) ≤ 5 x upper limit of normal (ULN)
Total bilirubin ≤ 2 (or ≤ 3 if history of Gilbert's syndrome or leukemic infiltration of the liver)
Serum creatinine < 2.0mg/dL
Oxygen saturation (SaO2) ≥ 92% on room air
Left ventricular ejection fraction (LVEF) ≥ 50% within 1 month of screening
Eastern Cooperative Oncology Group (ECOG) performance status 0-2
CD19 expression is required at any time since diagnosis. CD19 expression may be detected by immunohistochemistry or by flow cytometry. Patients receiving prior blinatumomab are eligible if there is no documentation of CD19-negative disease after blinatumomab
Central nervous system (CNS)1 status must be documented at time of screening by CSF assessment. Patients with prior CNS2 or CNS3 disease must be CNS1 at screening and have no residual CNS deficits or symptoms
Patients will need to adhere to institutional contraception guidelines for a minimum of 1 year
Exclusion Criteria
Concurrent active malignancy excluding non-melanoma skin cancer. Patients with a history of prior malignancy who have been treated with curative intent and have been in remission for at least 2 years are eligible
Burkitt’s leukemia or lymphoma
Patients with measurable extramedullary disease at screening are excluded. Patients with prior history of extramedullary disease are allowed after documentation of disease resolution by either PET/CT scan (or CT with contrast if PET cannot be performed)
The following medications are excluded:
* Steroids: Therapeutic doses of corticosteroids (greater than 10mg daily of prednisone or its equivalent) within 7 days of leukapheresis or 72 hours prior to CAR T cell infusion
* Systemic chemotherapy: Must be discontinued 7 days prior to leukapheresis or 7 days prior to starting lymphodepleting chemotherapy if used during bridging
* Tyrosine kinase inhibitors: Must be discontinued 48 hours prior to apheresis and 48 hours prior to starting lymphodepleting chemotherapy, if used during bridging
* Blinatumomab must be discontinued 5 days before apheresis
* Inotuzumab must be discontinued 2 weeks before apheresis to allow T cell recovery
Patients with uncontrolled systemic fungal, bacterial, viral or other infection at time of leukapheresis or at time of CAR T cell infusion
Blinatumomab may not be used as bridging therapy following apheresis
Positive test indicating the presence of active infection with the following pathogens: HIV, hepatitis B (detectable hepatitis B [Hep B] deoxyribonucleic acid [DNA] by polymerase chain reaction [PCR] or Hep B surface antigen), hepatitis C (detectable hepatitis C [Hep C] ribonucleic acid [RNA] by PCR), human T cell lymphotropic virus (HTLV), syphilis. The tests required will be agreed upon with the manufacturer to comply with manufacturer’s regulatory and manufacturing requirements
Study sponsor and potential other locations can be found on ClinicalTrials.gov for NCT07400029.
I. Determine the efficacy of obecabtagene autoleucel (obe-cel) consolidation in patients with Philadelphia chromosome negative (Ph)- ALL in first MRD negative CR as measured by relapse free survival (RFS) at 1 year from infusion. (Cohort A)
SECONDARY OBJECTIVES:
I. Key secondary objective: Determine the MRD-negative event free survival (EFS) at 1 year from infusion. (Cohort A & B)
II. Determine the efficacy of obe-cel consolidation as measured by RFS at 2 years. (Cohort A & B)
III. Assess the safety of obe-cel when administered in first MRD negative CR in ALL patients. (Cohort A & B)
IV. Determine the overall survival among treated patients. (Cohort A & B)
V. Determine the cumulative incidence of relapse, relapse patterns, and non-relapse mortality among treated patients. (Cohort A & B)
EXPLORATORY OBJECTIVES:
I. Evaluate quality of life, as measured through patient reported outcome measures, of Ph- and Ph+ patients treated with obe-cel separately. (Cohort A & B)
II. Determine the depth of remission as determined by ClonoSEQ (sensitivity 10^-6) after obe-cel consolidation. (Cohort A & B)
III. Assess the expansion and persistence of obe-cel, the duration of B-cell aplasia, and their associations with outcomes. (Cohort A & B)
IV. Explore the proteomic and transcriptomic phenotype of CAR T cells in patient's blood after infusion and their associations with oncologic outcomes. (Cohort A & B)
OUTLINE:
Patients undergo leukapheresis and receive lymphodepleting chemotherapy (LDC) with fludarabine intravenously (IV) over 30 minutes on days -6 to -3 and cyclophosphamide IV over 30 minutes on days -6 and -5. Patients may optionally receive bridging chemotherapy per investigator's discretion. Patients receive obecabtagene autoleucel IV over 30 minutes on days 0 and 9 in the absence of disease progression or unacceptable toxicity. Starting 60 days after the first obe-cel infusion, patients may receive tyrosine kinase inhibitor (TKI) maintenance at investigator discretion. Patients also undergo multigated acquisition scan (MUGA) or echocardiography (ECHO) during screening, as well as cerebrospinal fluid (CSF) and blood sample collection, bone marrow aspiration and biopsy throughout the study. Additionally, patients may undergo positron emission tomography (PET)/computed tomography (CT) or CT as clinically indicated throughout the study.
After completion of study treatment, patients are followed up on days 14, 21, and 28 and months 2, 3, 6, 12, 18, and 24 and then annually up to year 15.
Trial PhasePhase II
Trial Typetreatment
Lead OrganizationMemorial Sloan Kettering Cancer Center