Back to resultsInotuzumab Ozogamicin Post-Transplant For Acute Lymphocytic Leukemia and Non-Hodgkin's Lymphoma
Primary Purpose
Acute Lymphocytic Leukemia, Non-Hodgkin's Lymphoma
Status
Recruiting
Phase
Phase 1
Locations
United States
Study Type
Interventional
Intervention
Inotuzumab Ozogamicin
Sponsored by
About this trial
This is an interventional treatment trial for Acute Lymphocytic Leukemia focused on measuring allogeneic hematopoietic stem cell transplantation, donor chimerism
Eligibility Criteria
Inclusion Criteria:
Phase 1 Acute Lymphoblastic Leukemia Inclusion Criteria
- Diagnosis of CD22-positive Acute Lymphoblastic Leukemia
- Patients who underwent an allogeneic hematopoietic stem cell transplantation from any donor source for acute lymphocytic leukemia
- Patients who are between T+40 and T+100 after allogeneic transplantation. Patients must receive their first dose of inotuzumab at or before T+100.
Patients who have/are either:
Transplanted in hematologic first complete remission with evidence of minimal residual disease within 45 days of allogeneic transplantation
---Pre- or Post-Transplant Minimal Residual Disease defined by:
----Any detectable ALL (by flow cytometry, cytogenetics, or PCR techniques) as per clinical indication.
- In second or third complete remission at the time of allogeneic transplantation
- Treated with reduced intensity regimens or non-myeloablative conditioning regimens
- Lymphoid blast crisis of CML
- Are relapsed or refractory to at least 1 line of chemotherapy
- Philadelphia-like ALL
- Patients who have evidence of donor chimerism after allogeneic transplantation.
- ECOG Performance status < 2
- Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
- Able to adhere to the study visit schedule and other protocol requirements.
- Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 1 Non-Hodgkin's Lymphoma Inclusion Criteria
Diagnosis of CD22-positive B-cell Non-Hodgkin's Lymphoma
-- Patients with 1) Diffuse large B cell lymphoma; 2) Transformed indolent lymphoma; 3) CLL/SLL with Richter's transformation and 4) High grade B-cell lymphoma with MYC and BCL2 and/or BCL6 rearrangements.Patients must have received an autologous hematopoietic stem cell transplant under one of the following conditions:
- Achieved partial remission (defined as Deauville 4 on PET/CT) after treatment with platinum - containing salvage regimen;
- Failed first platinum - containing salvage regimen and achieved complete or partial remission after two separate lines of platinum - containing regimen;
- Had a second autologous hematopoietic stem cell transplant after achieving complete or partial remission with the first autologous transplant; or
- Had relapsed or refractory disease involving the bone marrow prior to receiving salvage therapy;
- The patient's lymphoma must be CD22 positive either by immunohistochemistry or flow cytometry analysis.
- Patients who are between T+40 and T+100 after autologous transplantation. Patients must receive their first dose of inotuzumab at or before T+100.
- ECOG Performance status < 2
- Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
- Able to adhere to the study visit schedule and other protocol requirements.
- Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 2 Acute Lymphoblastic Leukemia Inclusion Criteria
- Diagnosis of CD22-positive Acute Lymphoblastic Leukemia
- Patients who underwent an allogeneic hematopoietic stem cell transplantation from any donor source for acute lymphocytic leukemia
- Patients who are between T+40 and T+100 after allogeneic transplantation
Patients who have/are either:
Transplanted in hematologic first complete remission with evidence of minimal residual disease within 45 days of allogeneic transplantation
---Post-Transplant Minimal Residual Disease defined by:
----Any detectable ALL (by flow cytometry, cytogenetics, or PCR techniques) as per clinical indication.
- In second or third complete remission at the time of allogeneic transplantation
- Treated with reduced intensity regimens as defined per institutional standard of practice
- Lymphoid blast crisis of CML
- Are relapsed or refractory to at least 1 line of chemotherapy
- Philadelphia-like ALL
- Patients who have > 80% donor chimerism after allogeneic transplantation.
- Philadelphia chromosome positive ALL must have failed at least 1 TKI
- ECOG Performance status < 1
- pre-transplant evaluation, see 10.1.1
- Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
- Able to adhere to the study visit schedule and other protocol requirements.
- Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 2 Non-Hodgkin's Lymphoma Inclusion Criteria
Patients with 1) Diffuse large B cell lymphoma; 2) Transformed indolent lymphoma; 3) CLL/SLL with Richter's transformation and 4) High grade B-cell lymphoma with MYC and BCL2 and/or BCL6 rearrangements. Patients must have received an autologous hematopoietic stem cell transplant under one of the following conditions:
- Achieved partial remission (defined as Deauville 4 on PET/CT) after treatment with platinum - containing salvage regimen;
- Failed first platinum - containing salvage regimen and achieved complete or partial remission after two separate lines of platinum - containing regimen;
- Had a second autologous hematopoietic stem cell transplant after achieving complete or partial remission with the first autologous transplant; or
- Had relapsed or refractory disease involving the bone marrow prior to receiving salvage therapy;
- The patient's lymphoma must be CD22 positive either by immunohistochemistry or flow cytometry analysis.
- Patients who are between T+40 and T+100 after autologous transplantation. Patients must receive their first dose of inotuzumab at or before T+100.
- ECOG Performance status < 1
- Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
- Able to adhere to the study visit schedule and other protocol requirements.
- Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 1 and 2 Exclusion Criteria:
- Patients with clinical evidence of disease progression prior to enrollment 4.5.2 Persistent prior treatment toxicities Grade 2 and above according to NCI CTCAE Version 4.03 (with the exception for alopecia, neuropathy, etc.)
- For patients with NHL: Active central nervous system or meningeal involvement by lymphoma. Patients with a history of CNS or meningeal involvement must be in a documented remission. For patients with ALL: active central nervous system involvement with ALL.
Patients with inadequate organ function as defined by:
- Creatinine clearance < 30ml/min
- Bilirubin > 2X institutional upper limit of normal
- AST (SGOT) > 2X institutional upper limit of normal
- ALT (SGPT) > 2X institutional upper limit of normal
- GVHD grade III or IV (for patients with a prior allogeneic transplant).
- Active acute or chronic GVHD of the liver (for patients with a prior allogeneic transplant)
- History of VOD
- Active malignancy
- Patients with uncontrolled inter-current illness including, but not limited to ongoing or active infection, symptomatic congestive heart failure, unstable angina pectoris, cardiac arrhythmia, or psychiatric illness/social situationsthat would limit compliance with study requirements.
- Pregnant or breastfeeding women are excluded from this study because inotuzumab ozogamicin may be associated with the potential for teratogenic or abortifacient effects. Because there is an unknown, but potential risk for adverse events in nursing infants secondary to treatment of the mother with inotuzumab ozogamicin, breastfeeding should be discontinued if the mother is treated with inotuzumab ozogamicin. These potential risks may also apply to other agents used in this study.
- Evidence of myelodysplasia or cytogenetic abnormality indicative of myelodysplasia on any bone marrow biopsy prior to initiation of therapy Serologic statusreflecting active hepatitis B or C infection. Patientsthat are positive for hepatitis B core antibody, hepatitis B surface antigen (HBsAg), or hepatitis C antibody must have a negative polymerase chain reaction (PCR) prior to enrollment. (PCR positive patients will be excluded.)
- Participation in any other investigational drug study or had exposure to any other investigational agent, device, or procedure, within 21 days (or 5 half-lives, whichever is greater)
- Any condition that would, in the investigator's judgment, interfere with full participation in the study, including administration of study drug and attending required study visits; pose a significant risk to the participant; or interfere with interpretation of study data.
- Known allergies, hypersensitivity, or intolerance to any of the study medications, excipients, or similar compounds
Sites / Locations
- The University of Kansas Cancer CenterRecruiting
- Dana-Farber Cancer InstituteRecruiting
- University of Nebraska Medical CenterRecruiting
- Memorial Sloan Kettering Cancer CenterRecruiting
- University Hospitals Cleveland Medical Center, Case Comprehensive Cancer CenterRecruiting
- Cleveland Clinic Taussig Cancer institute, Case Comprehensive Cancer CenterRecruiting
- The James Cancer Hospital and Solove Research InstituteRecruiting
Arms of the Study
Arm 1
Arm Type
Experimental
Arm Label
Inotuzumab Ozogamicin
Arm Description
Phase I: A maximum of 12 cycles will be allowed and doses will be adjusted in 0.1mg/m2 increments using a dose escalation scale depending on tolerability. Total range of dose levels for ALL participants is 0.1-0.6mg/m^2 and for NHL participants 0.2-0.8mg/m^2 Dosing in the NHL cohort will start at Dose Level 0 (0.3mg/m^2) or one dose level below the ALL cohort maximum tolerated dose (MTD), whichever is higher. Phase II: ALL participants: Will be enrolled until all Phase I ALL participants have been followed and assessed for toxicity for at least 4 weeks after the fourth treatment dose of inotuzumab ozogamicin or 4 weeks after the participant goes off treatment, whichever comes first. Doses to be administered will be determined in the phase I portion of the study. The ALL cohort recommended phase 2 dose has been determined to be 0.6mg/m2. Repeat cycles every 28 days for up to 12 cycles
Outcomes
Primary Outcome Measures
Phase I MTD
Defined post hematopoietic stem cell transplantation MTD
Phase I DLTs
Frequency of DLTs during the first two cycles in ALL-participants and NHL-participants, reported separately
Phase II Median DFS
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Phase II Median DFS
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Phase II Median DFS
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Phase II Median DFS
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Phase II Median DFS
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Secondary Outcome Measures
Phase I Median DFS
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median DFS
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median DFS
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median DFS
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median DFS
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I NRM
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I NRM
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I NRM
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I NRM
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I NRM
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse-related mortality
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse-related mortality
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse-related mortality
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse-related mortality
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Relapse-related mortality
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase I Median OS
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median OS
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median OS
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median OS
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I Median OS
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase I pharmacokinetic (PK) parameters - Cmax (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Cmax (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase I Incidence of myeloid toxicity
Number of patients who develop myeloid toxicity while on study, defined as grade of anemia, neutropenia and thrombocytopenia CTCAE 4
Phase I Incidence of secondary graft failure
Number of patients who develop secondary graft failure while on study, defined as:
Either cytopenias after initial engraftment (ANC <500/µL), with (a) donor chimerism of less than 5% or (b) falling donor chimerism with intervention such as second transplant or donor lymphocyte infusion (DLI) or (c) patient death due to cytopenias, and fall in donor chimerism, even if chimerism was >5%. Exclusion criteria for diagnosis of GF were (a) disease relapse (b) graft versus host disease or (c) other causes of cytopenias such as, viral infections, or drug induced
Phase I incidence of veno-occlusive disease/sinusoidal obstruction syndrome (VOD/SOS)
Safety profile of intervention as measured by incidence of VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Phase I rate of VOD/SOS - number of participants affected
Safety profile of intervention as measured by number of participants affected by VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Phase I - Percent of participants with grade 3 + AE/SAEs
Phase I safety profile of intervention as measured by percent of participants with grade 3 + AE/SAEs
Phase II Non-relapse mortality (NRM)
Phase II Non-relapse mortality (NRM) in ALL cohort, defined as time from date of first dose to death due to any cause without prior relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase II Relapse
Phase II relapse rate, defined as in ALL cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase II Relapse
Phase II relapse rate, defined as in ALL cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase II Relapse-related mortality
Phase II Relapse-related mortality in ALL cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase II Relapse-related mortality
Phase II Relapse-related mortality in ALL cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Phase II Median OS
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase II Median OS
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase II Median OS
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase II Median OS
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase II Median OS
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Phase II Response Rate
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Phase II Response Rate
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Phase II Response Rate
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Phase II Response Rate
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Phase II Response Rate
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Phase II Incidence of myeloid toxicity
Number of patients who develop myeloid toxicity while on study, defined as grade of anemia, neutropenia and thrombocytopenia CTCAE 4
Phase II Incidence of secondary graft failure
Number of patients who develop secondary graft failure while on study, defined as:
Either cytopenias after initial engraftment (ANC <500/µL), with (a) donor chimerism of less than 5% or (b) falling donor chimerism with intervention such as second transplant or donor lymphocyte infusion (DLI) or (c) patient death due to cytopenias, and fall in donor chimerism, even if chimerism was >5%. Exclusion criteria for diagnosis of GF were (a) disease relapse (b) graft versus host disease or (c) other causes of cytopenias such as, viral infections, or drug induced
Phase I incidence of VOD/SOS
Safety profile of intervention as measured by incidence of VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Phase II rate of VOD/SOS - number of participants affected
Safety profile of intervention as measured by number of participants affected by VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Cmax ( ALL cohort)
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough ( ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Full Information
1. Study Identification
Unique Protocol Identification Number
NCT03104491
Brief Title
Inotuzumab Ozogamicin Post-Transplant For Acute Lymphocytic Leukemia and Non-Hodgkin's Lymphoma
Official Title
Inotuzumab Ozogamicin Post-Transplant For Acute Lymphocytic Leukemia and Non-Hodgkin's Lymphoma
Study Type
Interventional
2. Study Status
Record Verification Date
August 2023
Overall Recruitment Status
Recruiting
Study Start Date
July 31, 2017 (Actual)
Primary Completion Date
December 2023 (Anticipated)
Study Completion Date
June 2025 (Anticipated)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Sponsor-Investigator
Name of the Sponsor
Leland Metheny
4. Oversight
Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
Yes
5. Study Description
Brief Summary
This study has two phases, Phase I and Phase II. The main goal of the Phase I portion of this research study is to see what doses post-transplant inotuzumab ozogamicin can safely be given to subjects without having too many side effects.
The Phase II portion of this study is to see what side effects are seen with medication after transplant.
Inotuzumab ozogamicin is a combination of an antibody and chemotherapy which has been shown to have significant activity against relapsed/refractory acute lymphocytic leukemia (ALL) and Non-Hodgkin's Lymphoma (NHL).
Inotuzumab ozogamicin is considered experimental in this study.
Detailed Description
Study Design This is a Phase I/II study of inotuzumab ozogamicin for the treatment of patients who underwent allogeneic transplantation for ALL or who underwent autologous transplant for NHL and have a high risk of relapse. For ALL and NHL, respectively, the Phase I portion of this study will be a 3+3 dose escalation trial. For ALL patients, this is followed by a phase 2 cohort at the recommended Phase 2 dose (RP2D). Participants will receive study treatment up to 12 cycles until relapse of disease, unacceptable toxicity, or death, whichever occurs first
Phase I: Inotuzumab Ozogamicin Dosing Escalation Subjects will be assessed for safety and tolerability (including adverse events, serious adverse events, and clinical/laboratory assessments) using a continuous monitoring approach.
Phase II: Inotuzumab Ozogamicin Subjects will be assessed for safety and tolerability (including adverse events, serious adverse events, and clinical/laboratory assessments) using a continuous monitoring approach. In order to be included in the safety profile endpoint review, subjects must have received at least of 1 cycle of treatment.
Primary Objective
ALL Phase I: To define a post hematopoietic stem cell transplantation maximum tolerated dose (MTD) and recommended Phase 2 dose (RP2D) of inotuzumab ozogamicin in ALL.
NHL Phase I: To define a post hematopoietic stem cell transplantation MTD and RP2D of inotuzumab ozogamicin in NHL.
ALL Phase II: To assess the efficacy of inotuzumab ozogamicin as measured by diseasefree survival (DFS) at one year in ALL.
Secondary Objective(s)
Phase 1 (for each cohort):
To evaluate disease-free survival (DFS), nonrelapse mortality (NRM), relapse, relapse-related mortality and overall survival (OS) at 1 year.
To determine safety profile of inotuzumab ozogamicin after transplant including the incidence of myeloid toxicity and secondary graft failure and the rate of veno-occlusive disease/sinusoidal obstruction syndrome (VOD/SOS).
To determine if inotuzumab ozogamicin at these doses is effective at eradicating minimal residual disease in this cohort of participants (ALL participants).
To evaluate the pharmacokinetics of inotuzumab ozogamicin post autologous transplant (NHL participants).
Phase 2 (for all cohort):
To assess additional evidence of efficacy and safety as measured by non-relapse mortality (NRM), relapse, relapse-related mortality and overall survival (OS) at 1 year.
To determine if inotuzumab ozogamicin at these doses is effective at eradicating MRD in this cohort of participants (ALL participants).
To confirm the safety profile of inotuzumab ozogamicin therapy after transplant including myeloid toxicity, secondary graft failure, and the rate of VOD/SOS.
To evaluate the pharmacokinetics of inotuzumab ozogamicin post allogeneic transplant
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Acute Lymphocytic Leukemia, Non-Hodgkin's Lymphoma
Keywords
allogeneic hematopoietic stem cell transplantation, donor chimerism
7. Study Design
Primary Purpose
Treatment
Study Phase
Phase 1, Phase 2
Interventional Study Model
Single Group Assignment
Masking
None (Open Label)
Allocation
N/A
Enrollment
44 (Anticipated)
8. Arms, Groups, and Interventions
Arm Title
Inotuzumab Ozogamicin
Arm Type
Experimental
Arm Description
Phase I:
A maximum of 12 cycles will be allowed and doses will be adjusted in 0.1mg/m2 increments using a dose escalation scale depending on tolerability. Total range of dose levels for ALL participants is 0.1-0.6mg/m^2 and for NHL participants 0.2-0.8mg/m^2
Dosing in the NHL cohort will start at Dose Level 0 (0.3mg/m^2) or one dose level below the ALL cohort maximum tolerated dose (MTD), whichever is higher.
Phase II:
ALL participants: Will be enrolled until all Phase I ALL participants have been followed and assessed for toxicity for at least 4 weeks after the fourth treatment dose of inotuzumab ozogamicin or 4 weeks after the participant goes off treatment, whichever comes first. Doses to be administered will be determined in the phase I portion of the study. The ALL cohort recommended phase 2 dose has been determined to be 0.6mg/m2. Repeat cycles every 28 days for up to 12 cycles
Intervention Type
Drug
Intervention Name(s)
Inotuzumab Ozogamicin
Intervention Description
Inotuzumab ozogamicin, IV, 28 day cycles
ALL Phase 1 dosages:
Dose Level -2 (0.1 mg/m^2)
Dose Level -1 (0.2 mg/m^2)
Dose Level 0 (0.3 mg/m^2)
Dose Level 1 (0.4 mg/m^2)
Dose Level 2 (0.5 mg/m^2)
Dose Level 3 (0.6 mg/m^2)
NHL Phase 1 dosages:
Dose Level -1 (0.2 mg/m^2)
Dose Level 0 (0.3 mg/m^2)
Dose Level 1 (0.4 mg/m^2)
Dose Level 2 (0.5 mg/m^2)
Dose Level 3 (0.6 mg/m^2)
Dose Level 4 (0.7 mg/m^2)
Dose Level 5 (0.8 mg/m^2)
Primary Outcome Measure Information:
Title
Phase I MTD
Description
Defined post hematopoietic stem cell transplantation MTD
Time Frame
Up to 112 days (16 weeks)
Title
Phase I DLTs
Description
Frequency of DLTs during the first two cycles in ALL-participants and NHL-participants, reported separately
Time Frame
Up to 112 days (16 weeks)
Title
Phase II Median DFS
Description
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Time Frame
At 3 months after initial treatment
Title
Phase II Median DFS
Description
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Time Frame
At 6 months after initial treatment
Title
Phase II Median DFS
Description
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Time Frame
At 9 months after initial treatment
Title
Phase II Median DFS
Description
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Time Frame
At 1 year after initial treatment
Title
Phase II Median DFS
Description
Efficacy as measured by phase II DFS at one year in ALL cohort, estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)".
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
In ALL Phase II cohort, the null hypothesis of H0: DFS at 1-year ≤ 55% versus the alternative hypothesis of Ha: DFS at 1-year ≥ 75% using 1-sided alpha of 10% will be tested
Time Frame
Post first dose of inotuzumab ozogamicin
Secondary Outcome Measure Information:
Title
Phase I Median DFS
Description
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 3 months after initial treatment
Title
Phase I Median DFS
Description
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 6 months after initial treatment
Title
Phase I Median DFS
Description
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 9 months after initial treatment
Title
Phase I Median DFS
Description
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 1 year after initial treatment
Title
Phase I Median DFS
Description
Efficacy as measured by phase I DFS at one year in each cohort. Estimated using Kaplan-Meier, reported as median and 2-sided 80% and 95% Confidence Interval (CI)
DFS is defined as "Time from date of first dose to the date of disease progression (ie,objective progression, relapse from CR/CRi), or death due to any cause, whichever occurs first (including post-study treatment follow-up disease assessments)"
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
Post first dose of inotuzumab ozogamicin
Title
Phase I NRM
Description
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 3 months after initial treatment
Title
Phase I NRM
Description
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 6 months after initial treatment
Title
Phase I NRM
Description
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 9 months after initial treatment
Title
Phase I NRM
Description
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 1 year after initial treatment
Title
Phase I NRM
Description
Phase I NRM in each cohort, defined as time from date of first dose to death due to any cause without prior relapse. Criteria used: For ALL, evidence of disease in the blood or bone marrow (flow cytometry or PCR); for lymphoma typically physical exam findings or CT scans
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase I Relapse
Description
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 3 months after initial treatment
Title
Phase I Relapse
Description
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 6 months after initial treatment
Title
Phase I Relapse
Description
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 9 months after initial treatment
Title
Phase I Relapse
Description
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 1 year after initial treatment
Title
Phase I Relapse
Description
Phase I relapse rate, defined as in each cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase I Relapse-related mortality
Description
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 3 months after initial treatment
Title
Phase I Relapse-related mortality
Description
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 6 months after initial treatment
Title
Phase I Relapse-related mortality
Description
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 9 months after initial treatment
Title
Phase I Relapse-related mortality
Description
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 1 year after initial treatment
Title
Phase I Relapse-related mortality
Description
Phase I Relapse-related mortality in each cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase I Median OS
Description
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 3 months after initial treatment
Title
Phase I Median OS
Description
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 6 months after initial treatment
Title
Phase I Median OS
Description
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 9 months after initial treatment
Title
Phase I Median OS
Description
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 1 year after initial treatment
Title
Phase I Median OS
Description
Phase I OS, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase I pharmacokinetic (PK) parameters - Cmax (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 0 hours (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Cmax (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 1 hour (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 4 hours (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
at Cycle 1 Day 7 (C1D7) (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
at Cycle 2 Day 1 (C2D1) after 0 hours (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
at Cycle 2 Day 1 (C2D1) after 1 hour (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
at Cycle 4 Day 1 (C4D1) after 0 hours (each cycle is 28 days)
Title
Phase I pharmacokinetic (PK) parameters - Ctrough (NHL cohort only)
Description
Phase I PK parameters (NHL cohort only)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
at Cycle 4 Day 1 (C4D1) after 1 hour (each cycle is 28 days)
Title
Phase I Incidence of myeloid toxicity
Description
Number of patients who develop myeloid toxicity while on study, defined as grade of anemia, neutropenia and thrombocytopenia CTCAE 4
Time Frame
At 1 year
Title
Phase I Incidence of secondary graft failure
Description
Number of patients who develop secondary graft failure while on study, defined as:
Either cytopenias after initial engraftment (ANC <500/µL), with (a) donor chimerism of less than 5% or (b) falling donor chimerism with intervention such as second transplant or donor lymphocyte infusion (DLI) or (c) patient death due to cytopenias, and fall in donor chimerism, even if chimerism was >5%. Exclusion criteria for diagnosis of GF were (a) disease relapse (b) graft versus host disease or (c) other causes of cytopenias such as, viral infections, or drug induced
Time Frame
At 1 year
Title
Phase I incidence of veno-occlusive disease/sinusoidal obstruction syndrome (VOD/SOS)
Description
Safety profile of intervention as measured by incidence of VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Time Frame
At 1 year
Title
Phase I rate of VOD/SOS - number of participants affected
Description
Safety profile of intervention as measured by number of participants affected by VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Time Frame
At 1 year
Title
Phase I - Percent of participants with grade 3 + AE/SAEs
Description
Phase I safety profile of intervention as measured by percent of participants with grade 3 + AE/SAEs
Time Frame
At 1 year
Title
Phase II Non-relapse mortality (NRM)
Description
Phase II Non-relapse mortality (NRM) in ALL cohort, defined as time from date of first dose to death due to any cause without prior relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 3 months after initial treatment
Title
Phase II Relapse
Description
Phase II relapse rate, defined as in ALL cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 6 months after initial treatment
Title
Phase II Relapse
Description
Phase II relapse rate, defined as in ALL cohort, defined as time from date of first dose to the date of first relapse.
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 9 months after initial treatment
Title
Phase II Relapse-related mortality
Description
Phase II Relapse-related mortality in ALL cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
At 1 year after initial treatment
Title
Phase II Relapse-related mortality
Description
Phase II Relapse-related mortality in ALL cohort, defined time from date of first dose to death due to any cause with prior relapse
Reported as Cumulative Incidence and 2-sided 80% CI and 2-sided 95% CI
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase II Median OS
Description
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 3 months after initial treatment
Title
Phase II Median OS
Description
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 6 months after initial treatment
Title
Phase II Median OS
Description
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 9 months after initial treatment
Title
Phase II Median OS
Description
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
At 1 year after initial treatment
Title
Phase II Median OS
Description
Phase II OS in ALL cohort, defined from time from date of first dose to death due to any cause, estimated using Kaplan-Meier, reported as median and 95% CI
Difference in time-to-event endpoints will be tested using a 1-sided log-rank test at a significance level of 0.10
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase II Response Rate
Description
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Time Frame
At 3 months after initial treatment
Title
Phase II Response Rate
Description
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Time Frame
At 6 months after initial treatment
Title
Phase II Response Rate
Description
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Time Frame
At 9 months after initial treatment
Title
Phase II Response Rate
Description
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Time Frame
At 1 year after initial treatment
Title
Phase II Response Rate
Description
Defined as the proportion of patients with a best overall response of eradicating MRD in this cohort of patients at the time each patient discontinues treatment with Inotuzumab Ozogamicin
Time Frame
Post first dose of inotuzumab ozogamicin on day 1 cycle 1
Title
Phase II Incidence of myeloid toxicity
Description
Number of patients who develop myeloid toxicity while on study, defined as grade of anemia, neutropenia and thrombocytopenia CTCAE 4
Time Frame
At 1 year
Title
Phase II Incidence of secondary graft failure
Description
Number of patients who develop secondary graft failure while on study, defined as:
Either cytopenias after initial engraftment (ANC <500/µL), with (a) donor chimerism of less than 5% or (b) falling donor chimerism with intervention such as second transplant or donor lymphocyte infusion (DLI) or (c) patient death due to cytopenias, and fall in donor chimerism, even if chimerism was >5%. Exclusion criteria for diagnosis of GF were (a) disease relapse (b) graft versus host disease or (c) other causes of cytopenias such as, viral infections, or drug induced
Time Frame
At 1 year after initial treatment
Title
Phase I incidence of VOD/SOS
Description
Safety profile of intervention as measured by incidence of VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Time Frame
At 1 year
Title
Phase II rate of VOD/SOS - number of participants affected
Description
Safety profile of intervention as measured by number of participants affected by VOD/SOS disease in the phase I portion of the study, defined as the occurrence of 2 of the following 3 clinical criteria:
Total serum bilirubin level >34 μmol/L (>2.0 mg/dL).
An increase in liver size from baseline or development of right upper quadrant pain of liver origin.
Sudden weight gain >2.5% during any 72-hour period after infusion of investigational product because of fluid accumulation or development of ascites.
Time Frame
At 1 year
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 0 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 1 hour (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 4 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 7 (C1D7) (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 2 Day 1 (C2D1) after 0 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 2 Day 1 (C2D1) after 1 hour (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 4 Day 1 (C4D1) after 0 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Cmax ( ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Cmax is maximum concentration. Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 4 Day 1 (C4D1) after 1 hour (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 1 (C1D1) after 0 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough ( ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle1 Day 1 (C1D1) after 1 hour (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle1 Day 1 (C1D1) after 4 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 1 Day 7 (C1D7) (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 2 Day 1 (C2D1) after 0 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 2 Day 1 (C2D1) after 1 hour (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 4 Day 1 (C4D1) after 0 hours (each cycle is 28 days)
Title
Phase II pharmacokinetic (PK) parameters - Ctrough (ALL cohort)
Description
Phase II PK parameter (ALL cohort)
Ctrough is lowest concertration of Inotuzumab in the blood.Descriptive statistics (n, mean, SD, %CV, median, minimum, maximum, geometric mean, its associated geometric %CV) of inotuzumab ozogamicin serum concentrations will be presented in tabular form by cycle, day, nominal time and cohort for the PK concentration analysis population.
Time Frame
At Cycle 4 Day 1 (C4D1) after 1 hour (each cycle is 28 days)
10. Eligibility
Sex
All
Minimum Age & Unit of Time
16 Years
Maximum Age & Unit of Time
75 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
Phase 1 Acute Lymphoblastic Leukemia Inclusion Criteria
Diagnosis of CD22-positive Acute Lymphoblastic Leukemia
Patients who underwent an allogeneic hematopoietic stem cell transplantation from any donor source for acute lymphocytic leukemia
Patients who are between T+40 and T+100 after allogeneic transplantation. Patients must receive their first dose of inotuzumab at or before T+100.
Patients who have/are either:
Transplanted in hematologic first complete remission with evidence of minimal residual disease within 45 days of allogeneic transplantation
---Pre- or Post-Transplant Minimal Residual Disease defined by:
----Any detectable ALL (by flow cytometry, cytogenetics, or PCR techniques) as per clinical indication.
In second or third complete remission at the time of allogeneic transplantation
Treated with reduced intensity regimens or non-myeloablative conditioning regimens
Lymphoid blast crisis of CML
Are relapsed or refractory to at least 1 line of chemotherapy
Philadelphia-like ALL
Patients who have evidence of donor chimerism after allogeneic transplantation.
ECOG Performance status < 2
Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
Able to adhere to the study visit schedule and other protocol requirements.
Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 1 Non-Hodgkin's Lymphoma Inclusion Criteria
Diagnosis of CD22-positive B-cell Non-Hodgkin's Lymphoma
-- Patients with 1) Diffuse large B cell lymphoma; 2) Transformed indolent lymphoma; 3) CLL/SLL with Richter's transformation and 4) High grade B-cell lymphoma with MYC and BCL2 and/or BCL6 rearrangements. Patients must have received an autologous hematopoietic stem cell transplant under one of the following conditions:
Achieved partial remission (defined as Deauville 4 on PET/CT) after treatment with platinum - containing salvage regimen;
Failed first platinum - containing salvage regimen and achieved complete or partial remission after two separate lines of platinum - containing regimen;
Had a second autologous hematopoietic stem cell transplant after achieving complete or partial remission with the first autologous transplant; or
Had relapsed or refractory disease involving the bone marrow prior to receiving salvage therapy;
The patient's lymphoma must be CD22 positive either by immunohistochemistry or flow cytometry analysis.
Patients who are between T+40 and T+100 after cell therapy. Patients who received myeloablative conditioning must start between T+70 and T+100. Patients must receive their first dose of inotuzumab at or before T+100.
ECOG Performance status ≤ 2
Age ≥ 16 years, ≤ 75 years
Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
Able to adhere to the study visit schedule and other protocol requirements.
Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 2 Acute Lymphoblastic Leukemia Inclusion Criteria
Diagnosis of CD22-positive Acute Lymphoblastic Leukemia
Patients who underwent an allogeneic hematopoietic stem cell transplantation from any donor source for acute lymphocytic leukemia
Patients who are between T+40 and T+100 after allogeneic transplantation
Patients who have/are either:
Transplanted in hematologic first complete remission with evidence of minimal residual disease within 45 days of allogeneic transplantation
---Post-Transplant Minimal Residual Disease defined by:
----Any detectable ALL (by flow cytometry, cytogenetics, or PCR techniques) as per clinical indication.
In second or third complete remission at the time of allogeneic transplantation
Treated with reduced intensity regimens as defined per institutional standard of practice
Lymphoid blast crisis of CML
Are relapsed or refractory to at least 1 line of chemotherapy
Philadelphia-like ALL
Patients who have > 80% donor chimerism after allogeneic transplantation.
Philadelphia chromosome positive ALL must have failed at least 1 TKI
ECOG Performance status < 1
pre-transplant evaluation, see 10.1.1
Participants must have ANC > 1,000/µL for 3 days and platelet transfusion independence as defined as a platelet count > 50,000/µL for 7 days.
Able to adhere to the study visit schedule and other protocol requirements.
Participants must have the ability to understand and the willingness to sign a written informed consent document.
Phase 1 and 2 Exclusion Criteria:
Patients with clinical evidence of disease progression prior to enrollment 4.5.2 Persistent prior treatment toxicities Grade 2 and above according to NCI CTCAE Version 4.03 (with the exception for alopecia, neuropathy, etc.)
For patients with NHL: Active central nervous system or meningeal involvement by lymphoma. Patients with a history of CNS or meningeal involvement must be in a documented remission. For patients with ALL: active central nervous system involvement with ALL.
Patients with inadequate organ function as defined by:
Creatinine clearance < 30ml/min
Bilirubin > 2X institutional upper limit of normal
AST (SGOT) > 2X institutional upper limit of normal
ALT (SGPT) > 2X institutional upper limit of normal
GVHD grade III or IV (for patients with a prior allogeneic transplant).
Active acute or chronic GVHD of the liver (for patients with a prior allogeneic transplant)
History of VOD
Active malignancy
Patients with uncontrolled inter-current illness including, but not limited to ongoing or active infection, symptomatic congestive heart failure, unstable angina pectoris, cardiac arrhythmia, or psychiatric illness/social situationsthat would limit compliance with study requirements.
Pregnant or breastfeeding women are excluded from this study because inotuzumab ozogamicin may be associated with the potential for teratogenic or abortifacient effects. Because there is an unknown, but potential risk for adverse events in nursing infants secondary to treatment of the mother with inotuzumab ozogamicin, breastfeeding should be discontinued if the mother is treated with inotuzumab ozogamicin. These potential risks may also apply to other agents used in this study.
Evidence of myelodysplasia or cytogenetic abnormality indicative of myelodysplasia on any bone marrow biopsy prior to initiation of therapy Serologic statusreflecting active hepatitis B or C infection. Patientsthat are positive for hepatitis B core antibody, hepatitis B surface antigen (HBsAg), or hepatitis C antibody must have a negative polymerase chain reaction (PCR) prior to enrollment. (PCR positive patients will be excluded.)
Participation in any other investigational drug study or had exposure to any other investigational agent, device, or procedure, within 21 days (or 5 half-lives, whichever is greater)
Any condition that would, in the investigator's judgment, interfere with full participation in the study, including administration of study drug and attending required study visits; pose a significant risk to the participant; or interfere with interpretation of study data.
Known allergies, hypersensitivity, or intolerance to any of the study medications, excipients, or similar compounds
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Leland Metheny, MD
Phone
1-800-641-2422
Email
CTUReferral@UHhospitals.org
First Name & Middle Initial & Last Name or Official Title & Degree
Ron Sobecks, MD
Phone
216-444-6833
Email
sobeckr@ccf.org
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Leland Metheny, MD
Organizational Affiliation
University Hospitals Cleveland Medical Center, Case Comprehensive Cancer Center
Official's Role
Principal Investigator
Facility Information:
Facility Name
The University of Kansas Cancer Center
City
Westwood
State/Province
Kansas
ZIP/Postal Code
66205
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Nausheen Ahmed, MD
Email
nahmed5@kumc.edu
Facility Name
Dana-Farber Cancer Institute
City
Boston
State/Province
Massachusetts
ZIP/Postal Code
02215
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Roman Shapiro, MD
Email
Roman_Shapiro@DFCI.HARVARD.EDU
Facility Name
University of Nebraska Medical Center
City
Omaha
State/Province
Nebraska
ZIP/Postal Code
68106
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Vijaya Bhatt, MD
Email
Vijaya.bhatt@unmc.edu
Facility Name
Memorial Sloan Kettering Cancer Center
City
New York
State/Province
New York
ZIP/Postal Code
10065
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Christina Cho, MD
First Name & Middle Initial & Last Name & Degree
Christina Cho, MD
Facility Name
University Hospitals Cleveland Medical Center, Case Comprehensive Cancer Center
City
Cleveland
State/Province
Ohio
ZIP/Postal Code
44106-5065
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Leland Metheny, MD
Phone
800-641-2422
Email
CTUReferral@UHhospitals.org
First Name & Middle Initial & Last Name & Degree
Leland Metheny
Facility Name
Cleveland Clinic Taussig Cancer institute, Case Comprehensive Cancer Center
City
Cleveland
State/Province
Ohio
ZIP/Postal Code
44195
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Ronald Sobecks, MD
Phone
866-223-8100
Email
TaussigResearch@ccf.org
Facility Name
The James Cancer Hospital and Solove Research Institute
City
Columbus
State/Province
Ohio
ZIP/Postal Code
43210
Country
United States
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Sumithira Vasu, MBBS
Email
Sumithira.Vasu@osumc.edu
12. IPD Sharing Statement
Learn more about this trial
Inotuzumab Ozogamicin Post-Transplant For Acute Lymphocytic Leukemia and Non-Hodgkin's Lymphoma
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