A PROSPECTIVE, RANDOMIZED, OPEN-LABEL PHASE 2 STUDY TO EVALUATE THE SUPERIORITY OF INOTUZUMAB OZOGAMICIN MONOTHERAPY VERSUS ALLR3 FOR INDUCTION TREATMENT OF CHILDHOOD HIGH RISK FIRST RELAPSE B-CELL PRECURSOR ACUTE LYMPHOBLASTIC LEUKAEMIA

Pfizer133 sites in 13 countries100 target enrollmentMay 17, 2023

ConditionsACUTE LYMPHOBLASTIC LEUKEMIA

InterventionsInotuzumab ozogamicin ALLR3

DrugsInotuzumab ozogamicin ALLR3

Overview

Phase: Phase 2
Intervention: Inotuzumab ozogamicin
Conditions: ACUTE LYMPHOBLASTIC LEUKEMIA
Sponsor: Pfizer
Enrollment: 100
Locations: 133
Primary Endpoint: Minimum Residual Disease (MRD) Negativity in participants achieving complete response (CR), complete response with incomplete platelet count recovery (CRp), or complete response with incomplete count recovery (CRi)
Status: Recruiting
Last Updated: 9 days ago

Overview Investigators Eligibility Criteria Arms & Interventions Outcomes Sites Similar Trials

Overview

Brief Summary

This prospective, randomized, multicenter, open-label Phase 2 study is designed to evaluate the superiority of InO monotherapy vs ALLR3 after 1 cycle of induction treatment in paediatric participants (between 1 and <18 years) with High Risk (HR) first bone marrow relapse CD22-positive BCP ALL, and to evaluate the safety and tolerability, PK and long-term efficacy. Treatment with study intervention will end after induction therapy; follow-up will continue for up to 5 years from randomization.

Detailed Description

This prospective, randomized, multicenter, open-label, Phase 2 study is designed to evaluate the superiority of InO monotherapy vs ALLR3, after 1 cycle of induction treatment in paediatric participants (between 1 and \<18 years) with HR first bone marrow relapse CD22-positive BCP ALL, and to evaluate the safety and tolerability, PK and long-term efficacy. Treatment with study intervention will end after induction therapy; follow-up for efficacy and safety will continue for up to 5 years from randomization. End of Treatment is defined as occurring upon recovery from 1 cycle of study therapy (Day 28 ± 2 days), or one day before initiation of new anticancer therapy, whichever occurs first. Approximately 100 participants will be randomized (2:1) to receive 1 cycle of either InO monotherapy or ALLR3 (block 1) therapy during induction. After completion of induction therapy (ie, study therapy), it is anticipated that the majority of responding participants will proceed immediately to consolidation therapy. Non-responders are expected to proceed with salvage therapy at the investigator's discretion. Participants responding to induction therapy are expected to proceed to SOC consolidation therapy upon recovery of blood counts, but no sooner than 7 days after last dose of study intervention. All participants (responders and non-responders) will proceed to long-term follow-up for this study. All subsequent anticancer therapy will be determined by the treating physician.

Registry

clinicaltrials.gov

Start Date

May 17, 2023

End Date

November 4, 2036

Last Updated

9 days ago

Study Type

Interventional

Study Design

Parallel

Sex

All

Investigators

Sponsor

Pfizer

Responsible Party

Sponsor

Eligibility Criteria

Inclusion Criteria

•Male or female participants between 1 and \<18 years of age.
•Morphologically confirmed diagnosis of first relapse HR BCP ALL; HR first relapse is defined as relapse occurring within 18 to 30 months of original diagnosis of ALL or within 6 months of completion of primary therapy, and lacking any identified very high-risk genetic abnormalities (Groeneveld-Krentz et al, 2019) (ie, KMT2A::AFF1 fusion \[t(4;11)(q21;q23)\], TCF3-HLF fusion \[t(17;19)(q22;p13)\], TCF3-PBX1 fusion \[t(1;19)(q23;p13.3)\], hypodiploidy \[\<40 chromosomes\] or masked low hypodiploidy (Molina et al, 2021), TP53 alteration).
•CD22-positive ALL as defined by local institution;
•Bone marrow involvement of ≥ 5% leukemic blasts (≥ M2 status).
•Adequate serum chemistry parameters:
•An eGFR in participants 1 to \<2 years of age, or eCrCl in those 2 to \<18 years of age, ≥30 mL/min using the recommended formula in Section 10.10.
•AST and ALT ≤5 × institutional ULN at the time of randomization or pre-cytoreduction/general anesthesia;
•Total bilirubin ≤1.5 × institutional ULN unless the participant has documented Gilbert's syndrome;
•Prior history of thrombosis during corticosteroid use and/or asparaginase are eligible provided the patient receives anti-coagulant prophylaxis per institutional guidelines.
•Cardiac shortening fraction ≥ 30% by echocardiogram or ejection fraction \>50% by MUGA.

Exclusion Criteria

•Any history of prior or ongoing hepatic SOS or prior liver failure \[defined as severe acute liver injury with encephalopathy and impaired synthetic function (INR of ≥1.5)\].
•Prior allo-HSCT or CAR T-cell therapy.
•Isolated extramedullary leukemia.
•Philadelphia-chromosome positive ALL, ie. BCR-ABL/t(9;22) present.
•Prior therapy with a calicheamicin-conjugated antibody (eg, InO or gemtuzumab ozogamicin).
•Participants with active, uncontrolled bacterial, fungal, or viral infection.
•Hypersensitivity/allergy to both PEG-ASP and Erwinia-ASP

Arms & Interventions

Inotuzumab ozogamicin

Each participant in the InO arm will receive 1 course (3 doses) of InO, as follows: * Day 1: 0.8 mg/m2 * Days 8 (±1 day) and Day 15 (±1 day): 0.5 mg/m2/dose

Intervention: Inotuzumab ozogamicin

ALLR3

Mitoxantrone 10 mg/m2 on Days 1 and 2 Vincristine 1.5 mg/m2 (max single dose 2 mg) administered on Days 3, 10, 17 and 24 Dexamethasone 20 mg/m2/day administered orally (or IV) divided into two daily doses (maximum 40 mg/day) as two 5-day blocks on Days 1-5 and Days 15-19. PEG-asparaginase 1000 units/m2 IV administered on Days 3 and 17. In case of hypersensitivity/allergic reaction to PEG-asparaginase, each dose of PEG-asparaginase will be replaced by Erwinia-asparaginase at a dose of 20,000 units/m² IV or IM every other day for a total of 6 doses

Intervention: ALLR3

Outcomes

Primary Outcomes

Minimum Residual Disease (MRD) Negativity in participants achieving complete response (CR), complete response with incomplete platelet count recovery (CRp), or complete response with incomplete count recovery (CRi)

Time Frame: After 1 treatment cycle: Day 28 +/- 2 days

MRD negativity status is determined based on the minimum MRD percentage between the date of CR/CRp/CRi and end of treatment test as assessed by RQ-PCR, with reflex to FC result if MRD is non-evaluable by RQ-PCR

Secondary Outcomes

Rate of hematopoietic stem cell transplantation (HSCT)(Up to 5 years from randomization)
Number of participants reporting an Adverse Event (AE)(From time of informed consent up to a minimum of 60 calendar days after the last dose of study drug.)
Event Free Survival (EFS)(From study start to first event (progression, relapse, failure to achieve CR/CRp/CRi by the end of induction, MRD persistence prior to HSCT [hematopoietic stem cell transplant], second malignancy, or death): up to 5 years from randomization)
Rate of Chimeric antigen receptor (CAR) T-cell therapy(Up to 5 years from randomisation)
Duration of Response (DoR) for Participants Who Achieved CR/CRp/CRi(From date of first response to date of first event (objective progression, relapse as determined by investigator assessment, MRD persistence prior to HSCT, or death due to any cause, whichever occurs first): up to 5 years from End of Treatment)
Pharmacokinetics (PK) parameter: InO Cmax(1 treatment cycle: 28 days)
Number of Adverse Events (AE) reported by severity(From time of informed consent up to a minimum of 60 calendar days after the last dose of study drug.)
Overall Survival (OS)(From start of treatment to date of death due to any cause: up to 5 years from randomization)
Pharmacokinetics (PK) parameter: InO trough levels(1 treatment cycle: 28 days)