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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT02879643
Other study ID # T2012-002
Secondary ID
Status Recruiting
Phase Phase 1
First received
Last updated
Start date January 31, 2017
Est. completion date December 31, 2022

Study information

Verified date April 2020
Source Therapeutic Advances in Childhood Leukemia Consortium
Contact Ellynore Florendo
Phone (323) 361- 3022
Email eflorendo@chla.usc.edu
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a pilot study utilizing Marqibo® (vincristine sulfate liposome injection) combined with dexamethasone, mitoxantrone and asparaginase (UK ALL R3) for relapsed acute lymphoblastic leukemia (ALL).


Description:

This study will utilize Marqibo® as a replacement for standard vincristine in combination with chemotherapy for children with relapsed ALL. The hypothesis is that the incorporation of Marqibo® with combination chemotherapy will be safe and feasible. In the context of this pilot study, overall outcomes and efficacy will be a secondary objective. It is hypothesized that data from this combination may show improved efficacy including, complete remission (CR), minimal residual disease (MRD) negativity, and progression free survival (PFS) rates and safety (i.e., neurotoxicity) in comparison to outcomes in historical regimens, including the UK ALL R3 with standard vincristine.


Recruitment information / eligibility

Status Recruiting
Enrollment 36
Est. completion date December 31, 2022
Est. primary completion date August 31, 2021
Accepts healthy volunteers No
Gender All
Age group 1 Year to 21 Years
Eligibility Inclusion Criteria

Age

-Patients must be = 1 and = 21 years of age at the time of enrollment.

Diagnosis

- Cohort A: Patients must have a diagnosis of acute lymphoblastic leukemia (ALL) or mixed phenotypic acute leukemia with = 5% blasts in the bone marrow (M2 or M3), with or without extramedullary disease) or a diagnosis of lymphoblastic lymphoma.

- Cohorts B & C: Patients must have a diagnosis of acute lymphoblastic leukemia (ALL), lymphoblastic lymphoma, or mixed phenotypic acute leukemia with any level of detectable disease (minimal residual disease level acceptable) with or without extramedullary disease

Performance Level -Karnofsky > 50% for patients > 16 years of age and Lansky > 50% for patients = 16 years of age.

Prior Therapy

- Patients must have recovered from the acute toxic effects (= Grade 2 or baseline) of all prior chemotherapy, immunotherapy, or radiotherapy prior to entering this study, unless otherwise specified. Subjects with disease related cytopenias will be eligible.

- Patients must have relapsed or refractory disease after attaining at least a first remission. They may be in first to third relapse..

- Patients with Philadelphia chromosome t(9;22) positive disease must have received at least two prior tyrosine kinase inhibitors.

- Patients who have experienced their relapse after a Hematopoietic stem cell transplantation (HSCT) are eligible, provided they have no evidence of graft-versus-host disease (GVHD) and are at least 100 days post-transplant at the time of enrollment.

- Prior anthracycline lifetime cumulative exposure: Patients must have less than 320 mg/m2 (or 400 mg/m2 if prior cardioprotection) lifetime exposure of anthracycline chemotherapy.

1. Cohort A: Patients must have less than 320 mg/m2 (or 400 mg/m2 if prior cardioprotection) lifetime exposure of anthracycline chemotherapy (See Appendix 2 for anthracycline calculation worksheet).

2. Cohorts B & C: There is no limit on prior anthracycline exposure.

- Hematopoietic growth factors: It must have been at least seven days since the completion of therapy with granulocyte colony-stimulating factor (GCSF) or other growth factors at the time of enrollment. It must have been at least 14 days since the completion of therapy with pegfilgrastim (Neulasta®).

- Biologic anti-neoplastic agents: At least seven days after the last dose of a biologic agent. For agents that have known adverse events occurring beyond seven days after administration, this period must be extended beyond the time during which adverse events are known to occur. The duration of this interval must be discussed with the study chair or vice chair.

- Monoclonal antibodies: At least three half-lives (or 30 days—whichever is longer) of the antibody must have elapsed after the last dose of monoclonal antibody. (e.g., Rituximab = 66 days, Epratuzumab = 69 days)

- Immunotherapy: At least 30 days after the completion of any type of immunotherapy, e.g. tumor vaccines, chimeric antigen receptor T-cells.

- Recent prior chemotherapy: At least 10 days after standard vincristine and the completion of any type of chemotherapy induction regimen. At least 3 weeks after radiation therapy. At least 30 days after the completion of any investigational neoplastic agent is also required. An investigational agent is defined as any drug that is not approved and licensed for sale by the FDA for institutions in the United States, by Health Canada for institutions in Canada and by The Therapeutic Goods Administration for institutions in Australia.

Exceptions:

- There is no time restriction in regard to prior intrathecal chemotherapy provided there is complete recovery from any acute toxic effects of such; it is allowable to enroll a patient that has received IT Cytarabine (ARA-C), IT Methotrexate (MTX) or triple IT therapy within 14 days of enrollment as part of their evaluation to diagnose disease relapse. The IT therapy given within 14 days of initiation of protocol specified chemotherapy, may substitute for the day 1 IT in cohorts A and B

- Subjects with rapidly progressive disease may receive hydroxyurea until they begin study therapy;

- Patients who relapse while on maintenance-type ALL therapy or are receiving maintenance therapy for disease stabilization will not require a wash-out period before entry into this study. However, there must be at least 10 days after any dose of standard vincristine.

Renal and Hepatic Function

- Renal function: Patient's serum creatinine must be = 1.5 x institutional upper limit of normal (ULN) according to age. If the serum creatinine is greater than 1.5 times normal, the patient must have a calculated creatinine clearance or radioisotope glomerular filtration rate (GFR) = 70milliliter/min/1.73m2. Alternatively, a 24-hour creatinine clearance may also be used.

- Hepatic function: alanine aminotransferase (ALT) and aspartate aminotransferase (AST) must be < 5 x institutional upper limit of norm ULN. Total bilirubin must be = 1.5 x ULN (except in the case of subjects with documented Gilbert's disease = 5 × ULN).

Cardiac Function

-Patients must have a shortening fraction = 27% or an ejection fraction = 55% by echocardiogram, cardiac MRI or multigated acquisition scan (MUGA).

Reproductive Function

- Female patients must not be pregnant and those of childbearing potential must have a negative urine or serum pregnancy test confirmed within one week prior to enrollment.

- Female patients with infants must agree not to breastfeed their infants while on this study.

- Male and female patients of childbearing potential must agree to use an effective method of contraception during the study.

Exclusion Criteria

Patients will be excluded if they have isolated testicular disease.

Patients will be excluded if they have previously received Marqibo®.

Patients will be excluded if they have a known allergy to any of the drugs used in the study, with the exception that patients with an allergy to PEG-asparaginase who can receive Erwinia asparaginase are eligible. Patients unable to receive any formulation of asparaginase may only enroll on cohort C

Patients will be excluded if they have active, uncontrolled systemic fungal, bacterial, viral or other infection despite appropriate antibiotics or other treatment.

Patients who require azole antifungal agents will be excluded. Azoles must be discontinued at least one week prior to the start of Marqibo®.

Patients will be excluded if there is a plan to administer non-protocol chemotherapy, radiation therapy, another investigational agent or immunotherapy during the study period.

Patients with pre-existing, persistent grade 2 or greater sensory or motor neuropathy from any cause will be excluded.

Patients will be excluded if they have, significant concurrent disease, illness, psychiatric disorder or social issue that would compromise patient safety or adherence with the protocol treatment or procedures or interfere with consent, study participation, follow up, or interpretation of study results.Patients with Down syndrome will not be eligible for enrollment on Cohort A

Patients with a known history of human immunodeficiency virus (HIV) will will be excluded due to the increased risk of complications such as severe infection and unknown interaction of Marqibo® with antiretroviral drugs.

Active hepatitis B or C infection as defined by seropositive for hepatitis B (hepatitis B surface antigen (HBsAg)) or hepatitis C and elevated liver transaminases (defined as above the ULN per the institution normal ranges).

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Marqibo
The focus of the study design and statistical analysis is to determine whether Marqibo® can be substituted for standard vincristine and successfully administered to patients with relapsed ALL in three different treatment cohorts: (A) treatment with the UK ALL R3 regimen; (B) treatment with UK ALL R3 regimen without mitoxantrone, and (C) treatment with ALL maintenance therapy. Secondary objectives include estimating rates of serious toxicities and therapy delays in each of these cohorts.

Locations

Country Name City State
Australia Royal Children's Hospital, Melbourne Parkville, Victoria
Australia Sydney Children's Hospital Randwick New South Wales
Australia Lady Cilento Children's Hospital South Brisbane Queensland
Australia The Children's Hospital at Westmead Westmead New South Wales
Canada Sainte-Justine University Hospital Center Montréal, Québec
Canada Hospital for Sick Children Toronto Ontario
Canada British Columbia Children's Hospital Vancouver British Columbia
United States CS Mott Children's Hospital, Ann Arbor Ann Arbor Michigan
United States Children's Healthcare of Atlanta at Egleston Atlanta Georgia
United States The Children's Hospital, University of Colorado Aurora Colorado
United States Sidney Kimmel Cancer Center at Johns Hopkins Baltimore Maryland
United States National Cancer Institute, Pediatric Oncology Branch Bethesda Maryland
United States Dana-Farber Cancer Institute Boston Massachusetts
United States Levine Children's Hospital Charlotte North Carolina
United States Lurie Children's Hospital of Chicago Chicago Illinois
United States Cincinnati Children's Hospital Cincinnati Ohio
United States Rainbow Babies & Children's Hospital Cleveland Ohio
United States Nationwide Children's Hospital Columbus Ohio
United States University of Texas Southwestern Medical Center Dallas Texas
United States Cook Children's Medical Center Fort Worth Texas
United States Texas Children's Cancer Center, Baylor Houston Texas
United States Childrens Hospital Los Angeles Los Angeles California
United States University of Miami Miami Florida
United States Medical College of Wisconsin Milwaukee Wisconsin
United States Children's Hospitals and Clinics of Minnesota Minneapolis Minnesota
United States Monroe Carell Jr. Children's Hospital at Vanderbilt Nashville Tennessee
United States Children's Hospital New York-Presbyterian New York New York
United States Children's Hospital Orange County Orange California
United States Children's Hospital of Philadelphia Philadelphia Pennsylvania
United States Oregon Health & Science University Portland Oregon
United States All Children's Hospital Saint Petersburg Florida
United States Primary Children's Hospital Salt Lake City Utah
United States UCSF School of Medicine San Francisco California
United States Seattle Children's Hospital Seattle Washington
United States Children's National Medical Center Washington District of Columbia

Sponsors (2)

Lead Sponsor Collaborator
Therapeutic Advances in Childhood Leukemia Consortium Spectrum Pharmaceuticals, Inc

Countries where clinical trial is conducted

United States,  Australia,  Canada, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants with Dose Limiting Toxicities as a Measure of Safety and Tolerability The incidence of dose limiting toxicity (DLT) will be measured at different dose levels. 5 weeks
Secondary The response rate after treatment. The rate of remission will be assessed after 1 courses of therapy. A bone marrow aspirate/biopsy and CBC will be conducted to assess response. Approx. 8 weeks
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