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NCT06158828 · Washington University School of Medicine

Pilot Study of Memory-like Natural Killer (ML NK) Cells After TCRαβ T Cell Depleted Haploidentical Transplant in AML

(ABCD-NK)

What this study is about

This trial represents a single institution phase I/II pilot study with the primary objective of establishing the safety and feasibility of generating and infusing ML NK cells after TCRαβ haplo-HCT.

View original scientific description

This trial represents a single institution phase I/II pilot study with the primary objective of establishing the safety and feasibility of generating and infusing ML NK cells after TCRαβ haplo-HCT.

Interventions

DRUG

Rabbit Anti thymocyte globulin

rATG is administered intravenously over 6-18 hours for a total of 2 to 3 doses. The daily dose is based on body weight and lymphocyte count.

DRUG

Busulfan

Busulfan is administered intravenously either Q6H or Q24H, with a recommended target Busulfan AUC of 70-90 mg\*h/L.

DRUG

Fludarabine

Fludarabine is administered intravenously at a dose of 40 mg/m\^2/dose once daily for 4 days.

DRUG

Thiotepa

Thiotepa is administered intravenously at a dose of 5 mg/kg/dose Q12H for 2 doses.

DRUG

Melphalan

Melphalan is administered intravenously at a dose of 70 mg/m\^2/dose once daily for 2 days.

BIOLOGICAL

TCR alpha beta / CD19+ depleted haploidentical hematopoietic progenitor cell graft

The HPC product obtained from a haploidentical donor will undergo ex vivo TCR alpha beta and CD19+ depletion, and will be infused fresh on Day 0. There is no maximum limit for CD34+ dose. A maximum dose of 1 x 10\^5/kg recipient weight of TCRαβ cells should not be exceeded in the final HPC product.

BIOLOGICAL

memory-like natural killer cells

The ML NK cells (dose: max capped at 20 x 10\^6/kg recipient weight, minimum dose allowed is 0.5 x 10\^6/kg recipient weight) will be infused on Day +7.

BIOLOGICAL

IL-2

IL-2 is administered subcutaneously at a dose of 1 million units/m\^2 on Days +7, +9, +11, +13, +15, +17, and +19 (7 doses total).

DRUG

Plerixafor

If suboptimal collection of stem cells is predicted, plerixafor may be administered at a dose of 0.24 mg/kg subcutaneous injection once (maximum 40mg/dose). For patients with renal impairment, plerixafor will be administered at a dose of 0.16 mg/kg subcutaneous injection (maximum 27 mg/day).

BIOLOGICAL

Granulocyte Colony-Stimulating Factor

G-CSF will be administered at a dose of 10 mcg/kg/day for 5 days, or 6 days if two days of collection are needed.

DEVICE

CliniMACS

After stem cells are collected by leukapheresis, in order to create the HPC product, the stem cells will be washed to remove platelets and the cell concentration will be adjusted per laboratory and CliniMACS technology recommendations. The cells are then labeled using the CliniMACS TCRαβ Biotin Kit and CD19+ immunomagnetic microbeads. After labeling, the cells are washed to remove unbound microbeads. The partially processed product is loaded on the CliniMACS device where labeled cells are depleted and the negative fraction is eluted off the device. The negative fraction is centrifuged and volume reconstituted to obtain the final product.

Primary outcome measures

Safety of patients being administered donor-derived ML NK cells following TCR alpha beta depleted haploidentical cell transplant

Time frame: From transplant through Day +100

Safety will be determined by events occurring following transplant. Non-relapse mortality, engraftment failure, and development of severe GvHD will be considered events.

Feasibility of manufacturing and administering donor-derived ML NK cells following TCR alpha beta depleted haploidentical cell transplant

Time frame: Through time of ML NK cell infusion (around Day +7)

Feasibility is defined by product manufacture failure, i.e., the inability to infuse ML NK cells due to product contamination or insufficient cell dose (\<0.5x10\^6 / kg recipient weight).

Who can participate

This study lists these criteria on ClinicalTrials.gov. A study coordinator reviews eligibility during screening — this page does not determine whether you qualify.

Inclusion criteria

  • - Cohort 1:
  • High risk acute myeloid leukemia (AML) in either:
  • Complete remission (CR) defined by \< 5% marrow blasts by morphology in the context of hematological recovery (ANC ≥ 0.5× 10\^9/L, platelet count ≥ 50 × 10\^9/L).
  • Morphological leukemia free state (MLFS) defined by the absence of hematological recovery and \< 5% marrow blasts by morphology
  • Patients must further meet one of the below for inclusion into the study:
  • De novo AML in CR1 with any of the following high-risk features:
  • MRD ≥ 1% after first induction course
  • MRD ≥ 0.1% after second induction course
  • RUNX1-MECOM
  • KAT6A-CREBBP (if ≥ 90 days at diagnosis)
  • KMT2A-MLLT1
  • 11p15 rearrangement (NUP98 - any partner gene)
  • 12p13.2 rearrangement (ETV6 - any partner gene)
  • Deletion 12p to include 12p13.2 (loss of ETV6)
  • Monosomy 5/Del(5q) to include 5q31 (loss of EGR1)
  • 10p12.3 rearrangement (MLLT10b - any partner gene)
  • FLT3/ITD with allelic ratio \> 0.1%, without bZIP CEBPA or NPM1
  • RAM phenotype as evidenced by flow cytometry
  • Other high-risk features not explicitly stated here, after discussion/approval with protocol PI.
  • De novo AML in ≥ CR2
  • Therapy-related AML in CR1
  • AML evolving from myelodysplastic syndrome (MDS)
  • One prior hematopoietic cell transplant is allowed, provided remission criteria as defined above are met. Patient Inclusion Criteria - Cohort 2:
  • High risk acute myeloid leukemia (AML) defined by either of the following:
  • Treatment refractory disease: AML that is not in complete remission despite prior standard or salvage therapies.
  • Multiply relapsed disease: AML that has relapsed after 2 or more hematopoietic cell transplantations.
  • BM disease burden: Less than 25% bone marrow blasts by morphology must be present (M2 marrow), irrespective of peripheral hematological recovery. Patient Inclusion Criteria - Both Cohorts:
  • Less than or equal to 40 years of age.
  • Lansky (\<16 years) or Karnofsky (≥16 years) performance status of \>60%.
  • Adequate organ function as defined below:
  • Total bilirubin ≤ 3 x IULN for age
  • AST(SGOT)/ALT(SGPT) ≤ 5 x IULN for age
  • GFR ≥ 60 mL/min/1.73m2 as estimated by (1) updated Schwartz formula for ages 1-17 years or Cockcroft-Gault formula for ages ≥ 18 years, (2) 24-hour creatinine clearance, or (3) renal scintigraphy. If GFR is abnormal for age based on updated Schwartz or Cockcroft-Gault formula, accurate measurement should be obtained by either 24-hour creatinine clearance or renal scintigraphy.
  • Renal function may also be estimated by serum creatinine based on age/gender. A serum creatinine \< 2 x IULN for age/gender is required for inclusion on this protocol.
  • Adequate cardiac function, defined by left ventricular ejection fraction (LVEF) at rest ≥50% or shortening fraction (SF) ≥27% (via echocardiogram or MUGA).
  • Adequate pulmonary function, defined by:
  • FEV1, FVC, and DLCO ≥50% of predicted.
  • O2 saturation ≥ 92% on room air by pulse oximetry and no supplemental O2 at rest for children \< 8 years of age or those unable to perform pulmonary function testing (PFT). For children unable to perform PFT, a high-resolution CT chest should be obtained.
  • The effects of these treatments on the developing human fetus are unknown. For this reason, women of childbearing potential and men must agree to use adequate contraception (hormonal or barrier method of birth control, abstinence) prior to study entry, for the duration of study participation, and for 24 months following transplant. Should a woman become pregnant or suspect she is pregnant while participating in this study, she must inform her treating physician immediately.
  • Ability to understand and willingness to sign an IRB approved written informed consent document, or patient has a guardian who has the ability to understand and willingness to sign an IRB approved written informed consent document.
  • Available familial haploidentical donor. The HCT donor must be available and willing to undergo 2 leukapheresis procedures: (I) one mobilized collection for the HPC graft and (II) one non-mobilized leukapheresis collection for the manufacturing of ML NK cells.
  • Donor and recipient must be identical at a minimum of one allele of each of the following genetic loci: HLA-A, HLA-B, HLA-Cw, HLA-DRB1, and HLA- DQB1. A minimum of 5/10 match is required and will be considered sufficient evidence that the donor and recipient share one HLA haplotype. Patient

Exclusion criteria

  • - Both Cohorts
  • Active GvHD. If patient had prior GvHD, patient must be off immunosuppression for at least 3 months prior to starting study treatment.
  • Active non-hematologic malignancy. History of other malignancy is acceptable as long as therapy has been completed and there is no current evidence of disease.
  • Currently receiving any other investigational agents at the time of transplant.
  • Active CNS or extramedullary disease. History of CNS or extramedullary disease currently in remission is acceptable.
  • A history of allergic reactions attributed to compounds of similar chemical or biologic composition to agents used in the study.
  • Inability to discontinue medications that are likely to interfere with ML NK cell activity, i.e., glucocorticoids and other immunosuppressants.
  • Presence of significant anti-donor HLA antibodies per institutional standards. Anti-donor HLA - Antibody Testing is defined as a positive crossmatch test of any titer (by complement dependent cytotoxicity or flow cytometric testing) or the mean fluorescence intensity (MFI) of any anti-donor HLA antibody by solid phase immunoassay \> 3000.
  • Presence of a second major disorder deemed a contraindication for HCT.
  • Patients with Fanconi Anemia or Down Syndrome.
  • Uncontrolled intercurrent illness including, but not limited to, ongoing or active infection (bacterial, viral with clinical instability, or fungal), symptomatic congestive heart failure, or unstable cardiac arrhythmia.
  • Pregnant and/or breastfeeding. Women of childbearing potential must have a negative pregnancy test within 14 days of the start of conditioning. Donor Eligibility Criteria - Both Cohorts
  • The preferred donor should be an adult aged 18 years or older. However, in circumstances where no suitable adult donor is available, consideration may be given to a minor donor aged 12 years or older. This exception only applies when all identified, otherwise eligible adult donors meet one or more of the following criteria:
  • A medical condition that poses unacceptable risk, including autoimmune disease, infection, hematologic disorder, malignancy or a pathogenic germline mutation.
  • Comorbidities that preclude safe administration of granulocyte colony-stimulating factor (G-CSF), placement of a pheresis catheter and/or stem cell collection.
  • Served as donor in prior haploidentical HCT.
  • Significant psychosocial or logistical barriers.
  • Donor must be HLA haploidentical (≥ 5/10 and ≤ 9/10 allele match at the -A, -B, -C, DRB1 and DQ loci) by high resolution typing and related to the patient.
  • Donor must meet the selection criteria as defined by the Foundation for the Accreditation of Hematopoietic Cell Therapy (FACT).
  • Donor must be available and willing to undergo one mobilized and one non-mobilized leukapheresis procedure.
  • Donor may not be pregnant and/or breastfeeding. Women of childbearing potential must have a negative pregnancy test within 7 days prior to initiation of recipient's conditioning regimen, within 7 days of donor stem cell mobilization regimen and prior to second non-mobilized leukapheresis..
  • Donor must be able to understand and willing to sign an IRB-approved written informed consent document.

Where

  • St Louis, Missouri

Collaborators

The Leukemia and Lymphoma Society, Rising Tide Foundation, St. Louis Children's Hospital Foundation, Children's Discovery Institute

Related conditions & keywords

AML, ChildhoodAmlAcute Myeloid Leukemia, PediatricAcute Myeloid Leukemiahigh-risk AMLhaploidentical transplanthigh-risk acute myeloid leukemiaAML from MDSmemory-like natural killer cellsML NK cells

Frequently asked questions

What is a clinical trial?

A clinical trial is a research study that tests new medical treatments, drugs, devices, or procedures to determine their safety and effectiveness. Trials are carefully designed and monitored to protect participants while advancing medical knowledge.

Is it safe to participate?

Clinical trials follow strict safety guidelines and ethical standards. Trials must be reviewed and approved, and participants are closely monitored by medical professionals throughout the study. You can withdraw at any time if you choose.

Will I be compensated?

Many clinical trials offer compensation for your time, travel expenses, and inconvenience. The specific compensation varies by study and will be discussed during the screening process. All study-related medical care is typically provided at no cost to participants.

Will I receive a placebo instead of treatment?

When effective treatment exists, participants typically receive either the standard treatment plus the study intervention, or the standard treatment plus placebo. You would not be denied effective care. Placebos are primarily used when no proven treatment is available, or in addition to standard care. Your trial consent form will clearly explain what treatments you may receive.

Can I leave a trial if I change my mind?

Absolutely. Participation in clinical trials is completely voluntary. You have the right to withdraw from the study at any time, for any reason, without penalty or loss of benefits to which you are otherwise entitled.

How long does a clinical trial last?

Trial duration varies widely depending on the study design and purpose. Some trials last just a few weeks, while others may continue for months or years. The study coordinator will provide specific timeline information during your screening call.

Data: ClinicalTrials.gov · synced May 5, 2026 · Source of record for eligibility and locations

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Missouri

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What participation can include

  • Study-related care provided by the research team
  • Close monitoring by medical professionals
  • Possible compensation for time and travel*
  • The option to withdraw at any time
  • Contributing to medical research that may help future patients

*Compensation varies by study. Confirm details with coordinator.

Typical next steps

  1. 1.Submit this form
  2. 2.Phone screening
  3. 3.In-person assessment if eligible
  4. 4.Begin participation

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If you're searching for AML, Childhood treatment in St Louis, participating in a clinical research study may provide access to innovative approaches under expert medical supervision. This study is actively recruiting participants in St Louis and surrounding areas.

Clinical trials offer participants the opportunity to receive cutting-edge treatments while contributing to medical research that may help future patients with AML, Childhood. All study-related care is provided at no cost to participants.

Local Sites
1 locations in Missouri
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Why Consider a Clinical Trial for AML, Childhood?

Potential Benefits

  • Access to new treatment approaches before public availability
  • Close monitoring by experienced medical professionals
  • Study-related care provided at no cost
  • Contribute to medical research for AML, Childhood

What to Expect

  • Initial screening to determine eligibility
  • Regular check-ups and monitoring visits
  • Possible compensation for time and travel
  • You can withdraw at any time

Frequently Asked Questions About This AML, Childhood Study

Important Clinical Trial Information

This information is provided for educational purposes and does not constitute medical advice. Clinical trial participation involves potential risks and benefits. Eligibility requirements apply and will be assessed during the screening process.

Study identifier: NCT06158828. For complete study details, visit ClinicalTrials.gov. Always consult with your healthcare provider before making decisions about your medical care or participating in clinical research.