B Acute Lymphoblastic Leukemia Clinical Trial
— CAPTiRALLOfficial title:
Combination of an Anti-PD1 Antibody With Tisagenlecleucel Reinfusion in Children, Adolescents and Young Adults With Acute Lymphoblastic Leukemia After Loss of Persistence
Tisagenlecleucel (CTL019) is an anti-CD19 autologous Chimeric Antigen Receptor (CAR) T-cell therapy, which has shown dramatic early results in advanced ALLs. Early loss of B-cell aplasia (recovery of B-cells in marrow/ peripheral blood within 6 months after infusion), a marker of the loss or non-functionality of the CAR T-cells, is associated to a very high risk of relapse. A reinfusion of CTL019, even after Fludarabine-Cyclophosphamide reconditioning, frequently fails to induce further expansion as observed in UPENN studies and in the Robert Debré Hospital experience. Non-persistence of CAR T-cells may be due to immune- mediated rejection or environment-mediated suppression of their growth. Evidence for increased PD-1 expression in CAR T-cells between infusion and peak expansion has been demonstrated in clinical samples. Preclinical data and few clinical data support a role of PD- 1-PD-L1 blockade in improving the effectiveness of CAR T-cell therapy. The objectives of this phase I/II study is to determine the safety, efficacy and feasibility of Nivolumab (Opdivo®)- an anti-PD1 treatment- combined to tisagenlecleucel in a cohort of relapsed or refractory B-ALL patients, aged 1-25 years old, previously treated by tisagenlecleucel (Kymriah®), with a demonstrated early loss of B-cell aplasia (within 6 months), a surrogate marker of the loss of CAR T-cells or their non- functionality. More specifically, the main objectives are: • In cohort 1 that includes patients with a MRD negative disease status combined to an early loss (within 6 months) of B-cell aplasia : To determine the optimal starting time of Nivolumab (Opdivo®) in terms of safety and efficacy among 4 candidate time points (day 14, day 11, day 5, and day - 1). • In cohort 2 that includes relapsed patients with an early loss (within 6 months) of B-cell aplasia : To estimate the feasibility in terms of safety and efficacy of a very early start of nivolumab (day-1), prior to the reinfusion of tisagenlecleucel
| Status | Recruiting |
| Enrollment | 26 |
| Est. completion date | March 2027 |
| Est. primary completion date | March 2027 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 1 Year to 25 Years |
| Eligibility | Inclusion Criteria: - Patients aged from 1 to 25 years (pediatric and young adults) with a history of CD19+ relapsed or refractory B-ALL (any relapse after HSCT, 2nd relapse or later, refractory ALL). - Patient must have a second tisagenlecleucel (Kymriah ®) product available - Cohort 1: previously treated by tisagenlecleucel (Kymriah ®), and who present an early loss of B-cell aplasia defined by blood B lymphocytes < 10 /mm3 and/ or < 3% of total lymphocytes (< 6 months after infusion) while still being in CR with undetectable MRD - Cohort 2: previously treated by tisagenlecleucel (Kymriah ®), who present a loss of B-cell aplasia defined by blood B lymphocytes < 10 /mm3 and/ or < 3% of total lymphocytes and a CD19+ ALL detectable disease in the marrow and/or Blood - Life expectancy > 12 weeks. - Karnofsky (age > 16) Lansky (age < 16) > 70 at screening. - No organ dysfunction - Who have signed an informed consent - Affiliation to social security or any health insurance (as a beneficiary or assignee) Exclusion Criteria: - Patient has received intervening therapy for leukemia after first tisagenlecleucel infusion (chemotherapy, anti leukemic immunotherapy, ITK, allogeneic HSCT). - Patient has an active autoimmune disease requiring systemic treatment within the past 2 years. - Patient has known history of, or any evidence of active, non-infectious pneumonitis. - Patient has a history of non-infectious pneumonitis that required steroid or has current pneumonitis. - Had receive prior therapy with an anti-PD1, Anti- PDL1 or anti-PDL2 agent. - Patient has hypersensivity to pembrolizumab/ nivolumab or one of its excipients - Patient has received a live vaccine injection within 45 days of planned start of study therapy. - Patients with concomitant genetic syndromes associated with bone marrow failure states: such as patients with Fanconi anemia, Kostmann syndrome, Shwachman syndrome or any other known bone marrow failure syndrome. Patients with Down syndrome will not be excluded. - Patients with Burkitt's lymphoma/leukemia - Prior malignancy, except carcinoma in situ of the skin or cervix treated with curative intent and with no evidence of active disease. - Prior treatment with any gene therapy product except first tisagenlecleucel (Kymriah ®) injection. - Prior treatment with any anti-CD19/anti-CD3 therapy, or any other anti-CD19 therapy, except for patients pre-treated with blinatumomab and/or tisagenlecleucel (Kymriah®) - Prior anti-cancer monoclonal antibody within 4 weeks before starting the study. - Prior chemotherapy, targeted small molecule therapy, or radiation therapy within 2 weeks prior to study Day 1 or who has not recovered (i.e., = Grade1 or at baseline) from adverse events due to a previously administered agent. - Active or latent hepatitis B or active hepatitis C (test within 8 weeks of Screening), or any uncontrolled infection at Screening. - Human immunodeficiency virus (HIV) positive test within 8 weeks of Screening. - Presence of grade 2 to 4 acute or extensive chronic GVHD. - Active CNS involvement by malignancy, defined as CNS-3 per NCCN guidelines. Note: Patients with history of CNS disease that has been effectively treated will be eligible. - Uncontrolled acute life threatening bacterial, viral or fungal infection at Screening. - Previous or concurrent malignancy with the following exceptions: - Adequately treated basal cell or squamous cell carcinoma - in situ carcinoma of the cervix or breast, treated curatively and without evidence of recurrence for at least 3 years prior to the study. - A primary malignancy completely resected and in CR for = 5 years - Pregnant or lactating women (female study participants of reproductive potential must have a negative serum or urine pregnancy test performed within 48 hours before infusion) - Patient with hypersensivity to Fludarabine and/or cyclophosphamide and/or tisagenlecleucel and/or nivolumab or one of their excipients. |
| Country | Name | City | State |
|---|---|---|---|
| France | CHRU Bordeaux | Bordeaux | |
| France | CHRU Lille | Lille | |
| France | HCL | Lyon | |
| France | HCL | Lyon | |
| France | HCL - Lyon Sud | Lyon | |
| France | Hôpital pour enfants - La Timone | Marseille | |
| France | CHU Montpellier - Hopital Arnaud de Villeneuve | Montpellier | |
| France | CHU Nancy | Nancy | |
| France | CHU Nantes - Hopital Mère-enfants | Nantes | |
| France | Robert Debre hospital | Paris | |
| France | Saint Louis hospital | Paris | |
| France | CHU Rouen | Rouen | |
| France | CHRU Strasbourg | Strasbourg |
| Lead Sponsor | Collaborator |
|---|---|
| Assistance Publique - Hôpitaux de Paris |
France,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Proportion of patients with limiting-toxicities | Limiting toxicities are defined by the occurrence of either
- Related to CAR-T cells infusion: CRS or aGVH: limiting toxicity will be defined as toxicity = 4 ICANs: limiting toxicity will be defined as toxicity = 3 (excepted grade 3 seizure, ie focal, generalized seizure that resolves rapidly) - Related to nivolumab: immune related myocarditis, pneumonitis, encephalitis: limiting toxicity will be defined as toxicity = 4 |
at day 28 | |
| Primary | Efficacy assessed by Minimal residual disease (MRD) negative Complete remission (CR) and B cell aplasia. | MRD negative CR is defined by undetectable disease at a 10-4 sensitivity threshold B cell aplasia is defined by blood B lymphocytes < 10 /mm3 and/or < 3% of total lymphocytes | at 3 months | |
| Secondary | Incidence of B cell aplasia | at 6 months | ||
| Secondary | Increase of B cell aplasia duration compared to the previous one observed | up to 24 months | ||
| Secondary | Proportion of patients with Disease best response | up to three months | ||
| Secondary | Proportion of patients with Complete remission | at 1 month | ||
| Secondary | Proportion of patients with Complete remission | at 3 months | ||
| Secondary | Proportion of patients with Complete remission | at 6 months | ||
| Secondary | Proportion of patients with Complete remission | at 12 months | ||
| Secondary | Proportion of patients with Minimal residual disease | at 1 month | ||
| Secondary | Proportion of patients with Minimal residual disease | at 3 months | ||
| Secondary | Proportion of patients with Minimal residual disease | at 6 months | ||
| Secondary | Proportion of patients with Minimal residual disease | at 12 months | ||
| Secondary | Overall survival | at one year | ||
| Secondary | Overall survival | at 2 years | ||
| Secondary | Event Free Survival (EFS) | at 1 year | ||
| Secondary | Event Free Survival (EFS) | at 2 years | ||
| Secondary | Incidence of Grade 3 adverse events | up to 2 years | ||
| Secondary | Incidence of Grade 3, 4 or 5 nivolumab-related adverse events | up to 2 years | ||
| Secondary | Incidence of GVHD | up to one year |
| Status | Clinical Trial | Phase | |
|---|---|---|---|
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