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Clinical Trial NCT07020260 (PACMAN) for Leukemia, Lymphoma is not yet recruiting. See the Trial Radar Card View and AI discovery tools for all the details. Or ask anything here.
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The PACMAN-Hu19 Trial: a Study of the Safety and Feasibility of Locally Produced, CD19-targeted and Human CAR T-cell Therapy in Children and Young Adults With Relapsed or Refractory B-cell Malignancies Phase 1, Phase 2 18 Cell Therapy Multi-Center Adolescent Open-Label

Not yet recruiting
Clinical Trial NCT07020260 (PACMAN) is designed to study Treatment for Leukemia, Lymphoma. This Phase 1 Phase 2 interventional study is not yet recruiting. Enrollment is planned to begin on 1 September 2025 until the study accrues 18 participants. Led by Princess Maxima Center for Pediatric Oncology, this study is expected to complete by 1 September 2028. The latest data from ClinicalTrials.gov was last updated on 13 June 2025.
Brief Summary
PACMAN is a phase I/II single arm, open-label, multi-center study evaluating the safety of human CD19 CAR-T (huCAR19) produced locally using the Miltenyi Prodigy in children, adolescents and young adults with relapsed/refractory CD19+ hematological malignancies for whom no standard of care treatment is available.
Detailed Description
In this study patients aged 1-45 years with relapsed or refractory CD19+ hematological malignancies (B-NHL or BCP-ALL) are treated with a single dose of huCAR19 T-cells. After consent and screening, patients will undergo leukapheresis to harvest autologous PBMCs. During the CAR T-cell production, patients receive lymphodepleting chemotherapy after which the huCAR19 T-cells are administered. In phase I the aim is to e...Show More
Official Title

The PACMAN-hu19 Trial: a Phase I/II Study to Investigate the Safety and Feasibility of Point-of-care Human CD19 Targeting CAR T-cells in Pediatric and Young Adult Patients With Relapsed or Refractory B-cell Malignancies

Conditions
LeukemiaLymphoma
Other Study IDs
  • PACMAN
  • 2023-507597-40
  • 2023-507597-40-00 (EU Study (CTIS) Number)
NCT ID Number
NCT07020260
Start Date (Actual)
2025-09-01
Last Update Posted
2025-06-13
Completion Date (Estimated)
2028-09-01
Enrollment (Estimated)
18
Study Type
Interventional
PHASE
Phase 1
Phase 2
Status
Not yet recruiting
Keywords
CAR T-cell Therapy
relapsed B-cell malignancies
refactory B-cell malignancies
B-NHL
B-cell ALL
Primary Purpose
Treatment
Design Allocation
N/A
Interventional Model
Sequential
Masking
None (Open Label)
Arms / Interventions
Participant Group/ArmIntervention/Treatment
ExperimentalhuCAR19 T-cells
Participants will receive one single dose of huCAR19 T-cell infusion on day 0 of the treatment.
CAR T-cell and Cellular Therapies
A single IV infusion of huCAR 19 T-cells on day 0. In phase I 3 dose levels are tested to determine the RP2D.
Primary Outcome Measures
Outcome MeasureMeasure DescriptionTime Frame
Recommended phase 2 dose (RP2D)
The endpoint to measure this primary objective is the incidence of dose limiting toxicities (DLTs).
Within 28 days after huCAR19 infusion.
Secondary Outcome Measures
Outcome MeasureMeasure DescriptionTime Frame
To assess preliminary activity at day 28 for the BCP-ALL cohort and the overall response rate for the B-NHL cohort
For BCP-ALL: the MRD-negative CR rate. For B-NHL: the overall response rate (ORR, CR +PR according to Lugano criteria).
For BCP-ALL: at day 28. For B-NHL: at day 90.
Duration of response, including the duration of B-cell aplasia
Number of days until relapse. Number of days until loss of B-cell aplasia defined by ≥ 5 B-cells/µl.
from inclusion through study completion
Survival estimates.
Event free survival (EFS); Overall survival (OS); Cumulative Incidence of Relapse (CIR).
Measured at 6 and 12 months.
The feasibility to produce HuCAR19 in the target population.
Percentage of products fulfilling the release criteria.
From day -13 (start of manufacturing) to day 0 (final analysis)
Participation Assistant
Eligibility Criteria

Eligible Ages
Child, Adult
Minimum Age
1 Year
Eligible Sexes
All

  1. 1-45 years of age.

  2. Patients with relapsed or refractory CD19+ hematological malignancies including, but not limited to:

    1. B-NHL such as Burkitt lymphoma(BL), de novo or transformed diffuse large B cell lymphoma (DLBCL), lymphoblastic lymphoma (LBL), primary mediastinal B cell lymphoma (PMBCL) or indolent lymphoma types with no access to commercially available CAR T-cell therapy or for whom the current production time for commercially available CAR T-cell therapy is not acceptable based on medical need.

      OR

    2. B-cell precursor ALL failing commercially available CAR T-cell therapy, or for BCP-ALL indications with no access to commercially available CAR T-cell therapy, or for whom the current production time for commercially available CAR T-cell therapy is not acceptable based on urgent medical need (the latter needs to be confirmed by the sponsor).

  3. Measurable disease:

    1. For B-NHL at least one measurable lesion according to the Lugano classification.
    2. For BCP-ALL at least 0.1% (=10-3) of blasts should be present in the bone marrow measured by molecular MRD, morphology or flow cytometry at screening.

  4. Patients must have exhausted or are ineligible for all registered therapeutic options with curative potential.

  5. Adequate performance score:

    1. Children <16 years: Lansky performance status ≥ 60 .
    2. Children age ≥16 years and <18 years Karnofsky performance status ≥ 60.
    3. Adults ≥18 years ECOG performance status 0, 1 or 2 (ECOG performance status 3 is allowed only when due to underlying disease).

  6. Patients from childbearing potential must be willing and able to use highly effective methods of birth control from first chemotherapy infusion through 12 months after administering the last study treatment.

  7. Patients must be willing to abstain from breast feeding through 12 months after administering the last study treatment.

  8. Patients must agree to refrain from donating blood or organs following treatment with huCAR19 T-cells.

  9. Written informed consent per local law and regulations.

    Additional inclusion criteria phase I part of the study:

  10. The first three patients in the phase I part of the study must be aged 12-45 years, thereafter patients of any age between 1-45 years can be recruited once surrogate endpoint of BCA is reached in ≥60% patients in previous or current dose level and ≤1 DLT occurred at the previous dose level.

  1. Patients with symptomatic CNS involvement will be excluded. After resolution and control of symptoms, patients can be rescreened.

  2. Active uncontrolled or life-threatening infections.

  3. Infection with HTLV-1, HTLV-2, HIV-1, HIV-2, hepatitis B (HbsAg positive) or hepatitis C (anti-HCV positive). Chronic controlled hepatitis B or C infection with undetectable viral load or controlled HIV infection with viral load <50 IU/ml and CD4+ T-cell count >200/ml may be considered when antiviral prophylaxis or therapy can be administered.

  4. Absolute neutrophil count <0.5x109/L unless caused by underlying disease.

  5. Platelet count <25x109/L unless caused by underlying disease.

  6. Bilirubin and/or transaminases ≤ 2.5 x ULN, unless caused by underlying disease.

  7. Renal insufficiency, defined as:

    1. For adults (≥18 years) glomerular filtration rate (GFR) < 45 ml/min/1.73 m2 as calculated by the Modification of Diet in Renal Disease (MDRD) equation:

      predicted GFR (ml/min/1.73 m2) = 186 x (serum creatinine in umol/L / 88.7) - 1.154 x (age in years) - 0.203 x (0.742 if patient is female) x (1.212 if patient is black).

    2. For children (<18 years) a serum creatinine based on gender/age as follows (in µmol/l):

    Age Male Female 0 to < 2 years 53 70 2 to < 6 years 70 70 6 to < 10 years 88 88 10 to < 13 years 106 106 13 to < 16 years 132 123 16 to < 19 years 150 123

  8. Inadequate pulmonary function defined as baseline oxygen saturation <92%, if not caused by underlying disease.

  9. Inadequate cardiac function:

    1. Unstable angina or unstable cardiac arrhythmias.
    2. NYHA classification >II.
    3. LVSF <28% or LVEF <45% confirmed by echocardiogram or MUGA scan.

  10. Concurrent malignancy requiring treatment of having been treated <3 months before screening except for curatively treated basal cell carcinoma of the skin.

  11. Pregnant women.

  12. Patients unable to participate in the study according to investigator judgement.

  13. Patients not willing or unable to adhere to protocol guidelines or follow-up.

  14. Treatment with allogeneic stem cell transplantation <12 weeks from screening or DLI <4 weeks from screening or active GVHD requiring systemic treatment. Cutaneous GVHD requiring only topical steroids is allowed.

  15. Hypersensitivity to the active substance

Princess Maxima Center for Pediatric Oncology logoPrincess Maxima Center for Pediatric Oncology
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Study Central Contact
Contact: Ellis van Liempt, PhD, 0031 88 972 72 72, [email protected]
Contact: Marieke Kietselaer, 0031 88 972 72 72, [email protected]
2 Study Locations in 1 Countries

Utrecht

University Medical Center Utrecht, Utrecht, Utrecht, 3584 CX, Netherlands
Rimke Oostvogels, MD, PhD, Contact, 003188 75 558 78, [email protected]
Linda van Dommelen, Contact, 003188 75 558 78, [email protected]
Lotte van der Wagen, MD, PhD, Principal Investigator
Princess Máxima Center for pediatric oncology, Utrecht, Utrecht, 3584CS, Netherlands
Friso Calkoen, MD, PhD, Contact, 0031889227272, [email protected]
Ellis van Liempt, PhD, Contact, 0031889727272, [email protected]
Britta Vormoor, MD, PhD, Principal Investigator