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| ID | Type | Description | Link |
|---|---|---|---|
| 000324-C |
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Background:
Acute lymphoblastic leukemia (ALL) is the most common cancer in children. About 90% of children and young adults who are treated for ALL can now be cured. But if the disease comes back, the survival rate drops to less than 50%. Better treatments are needed for ALL relapses.
Objective:
To test chimeric antigen receptor (CAR) therapy. CARs are genetically modified cells created from each patient s own blood cells. his trial will use a new type of CAR T-cell that is targeting both CD19 and CD22 at the same time. CD19 and CD22 are proteins found on the surface of most types of ALL.
Eligibility:
People aged 3 to 39 with ALL or related B-cell lymphoma that has not been cured by standard therapy.
Design:
Participants will be screened. This will include:
Physical exam
Blood and urine tests
Tests of their lung and heart function
Imaging scans
Bone marrow biopsy. A large needle will be inserted into the body to draw some tissues from the interior of a bone.
Lumbar puncture. A needle will be inserted into the lower back to draw fluid from the area around the spinal cord.
Participants will undergo apheresis. Their blood will circulate through a machine that separates blood into different parts. The portion containing T cells will be collected; the remaining cells and fluids will be returned to the body. The T cells will be changed in a laboratory to make them better at fighting cancer cells.
Participants will receive chemotherapy starting 4 or 5 days before the CAR treatment.
Participants will be admitted to the hospital. Their own modified T cells will be returned to their body.
Participants will visit the clinic 2 times a week for 28 days after treatment. Follow-up will continue for 15 years....
Background:
Objectives:
Eligibility:
-Participants between >= 3 years and <= 39 years of age, with CD19+ and/or CD22+ B cell ALL or lymphoma who have relapsed or have refractory disease after at least one standard chemotherapy regimen and one salvage regimen, with no alternative curative options.
Design:
Phase I, 3 + 3 dose escalation design across 4 cohorts (B-ALL/B-cell lymphoblastic lymphoma: A: low-disease burden (<25 % marrow blasts without extramedullary disease) vs. B: high-disease burden (>= 25 % marrow blasts or with EMD). C: B-cell non-Hodgkin lymphoma D: CD19+ or CD22+ single antigen positivity using the following dose levels: -2: 1 x 10^5 transduced T cells/kg (+/- 20%); -1: 3 x 10^5 transduced T cells/kg (+/- 20%); 1: 1 x 10^6 transduced T cells/kg (+/- 20%); and 2: 3x 10^6 transduced T cells/kg (+/- 20%). Cohorts will enroll concurrently.
Participants will be treated based on disease burden and will receive 1 of 2 lymphodepleting preparative regimens:
Participants will be evaluated sequentially for toxicity, antitumor effects, CAR expansion and persistence, and other biologic correlatives.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| 1/Phase I Dose Escalation-with standard LD - CLOSED | Experimental | CD19/CD22-CAR-transduced T cells at escalating dose + standard LD (75 mg/mg2 Flu+ 900 mg/m2 Cy) |
|
| 1b/Phase 1 Dose Escalation - low disease burden | Experimental | CD19/CD22-CAR-transduced T cells |
|
| 2/Phase I Dose Escalation- with intensified LD - CLOSED | Experimental | CD19/CD22-CAR-transduced T cells + standard LD (120 mg/m2 Flu + 1200 mg/m2 Cy) |
|
| 2b/Phase 1 Dose Escalation - high disease burden | Experimental | CD19/CD22-CAR-transduced T cells |
|
| 3/Phase II Dose Expansion- with low disease burden - CLOSED | Experimental | CD19/CD22-CAR-transduced T cells at MTD/or highest dose administered with LD |
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| CD19/CD22-CAR-transduced T cells | Biological | CD19/CD22-CAR-transduced T cells on D0 after lymphodepleting preparative regimen |
|
| Measure | Description | Time Frame |
|---|---|---|
| Safety | Assess the safety of administering escalating doses of autologous CD19/CD22-CAR engineered T cells in children and young adult with B cell ALL or lymphoma following a cyclophosphamide/fludarabine LD. | 30 days post CAR T infusion |
| Efficacy | Determine the efficacy of CD19/CD22 therapy in participants with B-ALL/B-LBL. | Monthly until 3 months post CAR T infusion and then at 6 months and every 6 months after that, for 2 years post-infusion for each participant, up to 2 years after the entry date of the last participant. |
| Measure | Description | Time Frame |
|---|---|---|
| Assess response and toxicity (CRS grade) | Assess overall response rate and CRS grades (toxicity) in participants who received subsequent infusion | Up to two years after last participant has entered |
| Overall response rate |
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INCLUSION CRITERIA:
Diagnosis
Participant must:
Have evidence of at least minimal residual disease or PET-avid disease (lymphoma) at the time of enrollment.
CD22/CD19 expression
Cohorts A1b, B1b, C2b
Cohorts D1b, 2 B-ALL
Participants must have adequate organ and marrow function as defined below:
leukocytes >= 750/mcL*
platelets >= 50,000/mcL*
total bilirubin <=2 X ULN (except in the case of participants with documented Gilbert's disease > 3x ULN)
AST(SGOT)/ALT(SGPT) <=10 X institutional upper limit of normal
creatinine <= the maximum for age listed in the table below OR
measured creatinine clearance >=60 mL/min/1.73 m^2 for participants with creatinine levels above the max listed below per age.
Age (Years) <= 5 / Maximum Serum Creatinine (mg/dL) <= 0.8
Age (Years) 6 to <= 10 / Maximum Serum Creatinine (mg/dL) <= 1.0
Age (Years) >10 / Maximum Serum Creatinine (mg/dL) <= 1.2
Central nervous system (CNS) Status
Participants with leukemia with CNS 1 and 2 disease are eligible in the absence of exclusion criteria
Participants of child-bearing or child-fathering potential must be willing to practice effective birth control from the time of enrollment until 12 months following completion of study treatment for women and for 4 months following completion of study treatment for men.
Participants who are breastfeeding or plan to breastfeed must agree to discontinue/postpone breastfeeding while on study therapy and until 1 month after the administration of CAR.
Cardiac function: Left ventricular ejection fraction >= 45% or fractional shortening >=28%
Pulmonary Function
Ability of participant or Legally Authorized Representative (LAR) to understand and the willingness to sign a written informed consent document.
Ability and willingness of participant or Legally Authorized Representative (LAR) to co- enroll on 15-C-0028: Follow-up Evaluation for Gene-Therapy Related Delayed Adverse Events after Participation in Pediatric Oncology Branch Clinical Trials.
EXCLUSION CRITERIA:
Participants meeting any of the following criteria are not eligible for participation in the study:
Participants with CNS3 disease, progressing neurologic signs* of CNS disease, radiologically detected active CNS lymphoma (*resolving manifestation or persistent and/or irreversible findings from prior CNS involvement (e.g., blindness) is not exclusionary)
Hyperleukocytosis (>= 50,000 blasts/microL)
Positive serum or urine beta-HCG pregnancy test performed at screening.
Participants will be excluded based on prior therapy if they fail to meet following washout criteria:
Therapy: Systemic Chemotherapy, anti-neoplastic agents, antibody- based therapies
Washout*: >=2 weeks
Exceptions: 6 weeks for clofarabine or nitrosoureas; No washout for prior intrathecal chemotherapy, steroid therapy, hydroxyurea (no dose increases within prior 2 weeks) or ALL maintenance-type chemotherapy (vincristine, 6-mercaptopurine, oral methotrexate, or a tyrosine kinase inhibitor for participants with Ph+ ALL) provided there is recovery from any acute toxic effects
Therapy: Radiation
Washout*: >=3 weeks
Exceptions: No time restriction with radiation therapy if the volume of bone marrow treated is less than 10% and the participant has measurable/evaluable disease outside the radiation window
Therapy: Allogeneic Stem Cell Transplant
Washout*: >= 100 days since SCT; >= 30 days since completion of immunosuppression; >= 6 weeks since donor lymphocyte infusion (DLI)
Exceptions: Cannot have evidence of active graft-versus-host disease (GVHD) requiring systemic immunosuppression
Therapy: CAR T-Cell Therapy or other Adoptive Cell Therapy
Washout*: > 30 days post infusion
Positive HIV antibodies consistent with active HIV.
Positive hepatitis C antibodies or positive Hepatitis B surface antigen (HbsAG) indicative of current/active HCV/HBV.
Active second malignancy other than in situ carcinoma of the cervix, unless the tumor was treated with curative intent at least two years previously and participant is in remission.
History of severe, immediate hypersensitivity reaction attributed to compounds of similar chemical or biologic composition to any agents used in study or in the manufacturing of the cells.
Uncontrolled, symptomatic, intercurrent illness or social situations that would limit compliance with study requirements or in the opinion of the PI would pose an unacceptable risk to the participant.
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| NCI Ped LeukemiaLymph Cell Tx Tm | Contact | (240) 760-6970 | ncilltct@mail.nih.gov | |
| Sara K Silbert, M.D. | Contact | (240) 858-3666 | sara.silbert@nih.gov |
| Name | Affiliation | Role |
|---|---|---|
| Sara K Silbert, M.D. | National Cancer Institute (NCI) | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| National Institutes of Health Clinical Center | Recruiting | Bethesda | Maryland | 20892 | United States |
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| Label | URL |
|---|---|
| NIH Clinical Center Detailed Web Page | View source |
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All IPD recorded in the medical record will be shared with intramural investigators upon request.
Clinical data available during the study and indefinitely.
Clinical data will be made available via subscription to BTRIS and with the permission of the study PI.
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|
| 3b Phase I Dose Escalation: Either CD19 or CD22 positivity | Experimental | CD19/CD22-CAR-transduced T cells |
|
| 4/Phase II Dose Expansion- with high disease burden - CLOSED | Experimental | CD19/CD22-CAR-transduced T cells at MTD/or highest dose administered with LD regimen #2 |
|
| 4b Phase II Dose Expansion in B-ALL/B-LBL | Experimental | CD19/CD22-CAR-transduced T cells at RP2D |
|
| A/Pre-treatment | No Intervention | All participants enrolled on the study prior to treatment initiation. |
| cyclophosphamide | Drug | Cyclophosphamide will be diluted in an appropriate solution and infused over one hour. The dose will be based on the patient s body weight, at 900 mg/m2/dose after fludarabine infusion. |
|
| fludarabine | Drug | Fludarabine is administered as an IV infusion in an appropriate solution over 30 minutes. To prevent undue toxicity the dose will be based on BSA (25 mg/m2/dose). |
|
Phase I: Evaluate the ability of CD19/CD22-CAR T cells to mediate clinical activity in children and young adults with CD19+ and/or CD22+ B cell ALL or lymphoma.
| Monthly until 3 months post infusion and then at 6 months and every 6 months after that, for 2 years post-infusion for each participant, for up to two years from the entry date of the last participant |
| Progression free survival (PFS) and Overall survival (OS) | Evaluate PFS and OS in participants, in the phase II cohort (inclusive of those treated in the phase 1 arms at the RP2D) | Up to two years after the last participant has entered. |
| Persistence and expansion | Evaluate persistence and expansion of CD19/CD22-CAR T cells in children and young adults with CD19+ and/or CD22+ B-ALL or lymphoma | Up to two years after the last participant has entered. |
| Adverse Events | Phase II: Assess the safety of CD19/CD22 therapy in participants with B-ALL/B-LBL regardless of disease burden and antigen expression. | 30 days post CAR T infusion |
| Feasibility | Determine the feasibility of producing CD19/CD22-CAR T cells meeting the established release criteria. | Up to two years after the last participant has entered. |
| ID | Term |
|---|---|
| D054198 | Precursor Cell Lymphoblastic Leukemia-Lymphoma |
| D002051 | Burkitt Lymphoma |
| D008228 | Lymphoma, Non-Hodgkin |
| D015448 | Leukemia, B-Cell |
| D016393 | Lymphoma, B-Cell |
| D010677 | Philadelphia Chromosome |
| D008223 | Lymphoma |
| ID | Term |
|---|---|
| D007945 | Leukemia, Lymphoid |
| D007938 | Leukemia |
| D009370 | Neoplasms by Histologic Type |
| D009369 | Neoplasms |
| D006402 | Hematologic Diseases |
| D006425 | Hemic and Lymphatic Diseases |
| D008232 | Lymphoproliferative Disorders |
| D008206 | Lymphatic Diseases |
| D007160 | Immunoproliferative Disorders |
| D007154 | Immune System Diseases |
| D020031 | Epstein-Barr Virus Infections |
| D006566 | Herpesviridae Infections |
| D004266 | DNA Virus Infections |
| D014777 | Virus Diseases |
| D007239 | Infections |
| D014412 | Tumor Virus Infections |
| D014178 | Translocation, Genetic |
| D002869 | Chromosome Aberrations |
| D010335 | Pathologic Processes |
| D013568 | Pathological Conditions, Signs and Symptoms |
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| ID | Term |
|---|---|
| D003520 | Cyclophosphamide |
| C024352 | fludarabine |
| ID | Term |
|---|---|
| D010752 | Phosphoramide Mustards |
| D009588 | Nitrogen Mustard Compounds |
| D009150 | Mustard Compounds |
| D006846 | Hydrocarbons, Halogenated |
| D006838 | Hydrocarbons |
| D009930 | Organic Chemicals |
| D063088 | Phosphoramides |
| D009943 | Organophosphorus Compounds |
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