Overview

Evaluation of the Safety and Efficacy of the Association of Ibrutinib and Daratumumab in Relapsed/Refractory Chronic Lymphocytic Leukemia With p53 Dysfunction

Status:
Recruiting
Trial end date:
2027-06-01
Target enrollment:
0
Participant gender:
All
Summary
Ibrutinib, a first-in-class Bruton Tyrosine kinase (BTK) inhibitor, has become an established treatment in relapsed/refractory chronic lymphocytic leukemia (CLL). However, despite a considerable improvement of Progression Free Survival (PFS) and Overall Survival (OS) in comparison with historical controls, the prognosis of patients with 17p deletion (del17p) remains a concern, as it is clearly much less favourable than that of patient without del17p. Again, TP53 mutations correlated to poorer prognostic in Relapsed/Refractory (R/R) CLL patients treated with ibrutinib (Brown JR et al,2018). Despite these therapeutic advances, the treatment of CLL with TP53 disruption thus remains a difficult issue that warrants evaluation of alternative treatment strategies, in particular the use of ibrutinib in combination with other agents. A body of evidence suggests that targeting the extracellular molecule CD38 might be an interesting option. CD38 is a transmembrane glycoprotein with multiple receptor and enzymatic functions. The interaction of CD38 with its ligand CD31 (also known as Platelet Endothelial Cell Adhesion Molecule (PECAM-1)) not only plays a role in the binding and the migration of leucocytes through the endothelial cells wall but also triggers the activation of intracellular pathways involved in the differentiation and activation of B cells. Previous results strongly suggest that CD38 favours the expansion of CLL clones not only directly by transducing a proliferation signal but also by directing them to anatomic sites where they find favourable conditions for proliferation and survival. Daratumumab is a first-in-class human IgG1ĸ monoclonal antibody (mAb) that binds CD38-expressing malignant cells with high affinity. Daratumumab induces tumor cell death through multiple mechanisms such as antibody-dependent cell-mediated cytotoxicity (ADCC), complement dependent cytotoxicity (CDC), antibody-dependent cellular phagocytosis (ADCP) and induction of apoptosis (de Weers et al, 2011). Recent data show that daratumumab may also display an immunomodulatory effect through depletion of a subset of immunosuppressive CD38+ Tregs (Krejcik et al, 2016). Early-stage clinical trials found daratumumab to be safe and to display encouraging clinical activity as a single agent in relapsed/refractory multiple myeloma (MM) patients (Lockhorst et al 2016, Lonial et al, 2016). Overall response rate was 31%, with rapid (median 1 month) and durable responses in this heavily pretreated MM population. Interestingly, no patient discontinued the treatment because of drug-related adverse events. These results led to approval of daratumumab in relapsed/refractory MM in December 2015. The clinical efficacy of daratumumab along with its very favourable safety profile supports its investigation in other lymphoproliferative malignancies. In particular, the expression of CD38 in poor prognosis CLL and the key role of CD38 in CLL biology provide a basis for examining the potential of daratumumab in this disease. In preclinical studies, (Matas-Céspedes et al, 2016; Manna et al, 2017) Daratumumab efficiently kills CLL cell lines and patient-derived CLL cells by ADCC and ADCP in vitro. Daratumumab modulates CLL-T reg levels and increase cytotoxic effector T cells. Rationale for combining ibrutinib with daratumumab: These data suggest that combining ibrutinib with daratumumab might have a synergistic or additive effect. Both drugs inhibit B cell receptor (BCR) signalling via two different converging pathways, i.e. BTK and CD38/ZAP70/ERK (Deaglio et al, 2007). In vitro, Manna et al have shown that daratumumab is able to modulate BCR signaling. Interestingly, the ibrutinib /daratumumab combination significantly enhanced mitochondrial-mediated apoptosis bth in CD38 high and CD38 low CLL cells (Manna et al, 2017). Altogether, this provides a rationale for evaluating the safety and efficacy of the association of daratumumab with ibrutinib in high-risk relapsed/refractory patients for whom the standard-of-care using ibrutinib as a single agent has demonstrated limitations in terms of long-term disease control. Primary objective of the study: to determine the efficacy of a treatment combining daratumumab and ibrutinib in a poor risk population of relapsed CLL patients with TP53 dysfunction. Secondary objectives of the study : to determine the safety profile of daratumumab in combination with ibrutinib in CLL patients. Inclusion period: 24 months Treatment duration (ibrutinib + daratumumab): continuous, until disease progression or unacceptable toxicity. Follow-up period: will begin once the subject discontinues study treatment, during 2 years.
Phase:
Phase 2
Accepts Healthy Volunteers?
No
Details
Lead Sponsor:
French Innovative Leukemia Organisation
Collaborator:
Janssen, LP
Treatments:
Antibodies, Monoclonal
Daratumumab
Criteria
Inclusion Criteria:

- Immunophenotypically confirmed diagnosis of CLL (criteria iwCLL Hallek et al. 2018)

- Progressive CLL according to International Workshop on Chronic Lymphocytic Leukemia
(iwCLL) criteria

- Relapsed or refractory disease (≥ 1 previous line of treatment) with P53 genetic
alteration (17p deletion and/or TP53 mutation).

- Age > 18 years

- Eastern Cooperative Oncology Group electrocorticogram (ECOG) status 0-2

- Negative serum pregnancy test one week prior to treatment for premenopausal women

- Cumulative Illness Rating Scale (CIRS) ≤ 6

- Life expectancy > 3 months.

- Possibility of follow-up

- Ability to understand the protocol

- Written informed consent of patient and treating physician

Exclusion Criteria:

- Previous treatment with ibrutinib.

- Patient refusal to perform bone marrow biopsy for evaluation point

- Prior other malignancy (except for adequately treated basal cell or squamous cell skin
cancer, in situ cancer, or other cancer from which the subject has been disease free
for ≥ 2 years).

- Known chronic obstructive pulmonary disease (COPD) with a Forced Expiratory Volume in
1 second (FEV1) < 50 % of predicted normal. FEV testing is required for patients
suspected of having COPD.

- Moderate or severe persistent asthma within the two last years or currently
uncontrolled asthma of any classification (American Lung Association criteria).
Current controlled intermittent asthma or controlled mild persistent asthma is not an
exclusion criterion.

- Patients with active bacterial, viral, or fungal infection requiring systemic
treatment.

- Patients with known infection with human immunodeficiency virus (HIV) or human
T-lymphotropic virus type 1 (HTLV-1)

- Active B or C hepatitis (positive Hepatitis B Virus surface antigen (HBsAg) or
Hepatitis B Virus (HBV) DNA for HBV; Positive Hepatitis C virus (HCV) RNA for HCV)

- History of severe allergic or anaphylactic reactions to humanized or murine monoclonal
antibodies.

- Any other uncontrolled medical condition or comorbidity that might interfere with
subject's participation.

- Concomitant dual antiplatelet therapy

- Concomitant treatment with both antiplatelet and anticoagulation therapy

- Treatment with other investigational agent or participating to another trial within 30
days prior to entering the study

- Hemoglobin < 8 g/dL

- Absolute neutrophil count (ANC) < 1000/mm3

- Platelets < 30000/mm3

- Inadequate renal function: creatinine clearance < 50 ml/min (Cockcroft and Gault)

- Inadequate liver function: Aspartate Transaminase (ASAT), Alanine aminotransferase
(ALT) > 2.5 x Upper Limit of Normal (ULN)

- Total bilirubin > 1.5 x ULN unless rise is due to Gilbert's syndrome or of non-hepatic
origin.

- Active auto-immune haemolytic anemia

- Richter's transformation

- Evidence of central nervous system (CNS) involvement

- Pregnant or breastfeeding women.

- Adult under law-control

- Fertile male and female patients who cannot or do not wish to use an effective method
of contraception, during and for 12 months after the final treatment used for the
purposes of the study

- No affiliate to social security