SAR650984, a CD38 Monoclonal Antibody in Patients with Selected CD38+ Hematological Malignancies — Data from a Dose-Escalation Phase I Study Martin TG.

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Presentation transcript:

SAR650984, a CD38 Monoclonal Antibody in Patients with Selected CD38+ Hematological Malignancies — Data from a Dose-Escalation Phase I Study Martin TG et al. Proc ASH 2013;Abstract 284.

Background SAR (SAR) is a naked humanized IgG1 monoclonal antibody (mAb) that binds selectively to CD38, an antigen highly expressed on multiple myeloma (MM) cells and other hematologic cancers. SAR kills tumor cells via 3 different mechanisms: antibody-dependent cellular-mediated cytotoxicity, complement-dependent cytotoxicity and induction of apoptosis. Potent single-agent activity has been demonstrated with SAR in vivo (Proc AACR 2013;Abstract 4735). Study objective: To determine the maximum tolerated dose/maximum administered dose, safety and efficacy of SAR from the first-in-human, Phase I dose-escalation study for patients with select CD38+ hematologic cancers. Martin TG et al. Proc ASH 2013;Abstract 284.

Ongoing Phase I Study Design (NCT ) Eligibility (target accrual = 60) Select hematologic cancers: MM, chronic lymphocytic leukemia (CLL), non-Hodgkin lymphoma (NHL), acute leukemias (AML, ALL) Confirmed CD38 expression Relapsed disease SAR Martin TG et al. Proc ASH 2013;Abstract 284. Accelerated escalation 1 patient/cohort (cohort 1-5) mg/kg q2wk 1 MM mg/kg q2wk 1 MM 0.01 mg/kg q2wk 1 MM 0.03 mg/kg q2wk 2 MM 0.1 mg/kg q2wk 1 NHL Basic escalation 3-6 patients/cohort (cohort 6-12) 0.3 mg/kg q2wk 5 MM, 1 NHL, 1 CLL 1 mg/kg q2wk 3 MM 3 mg/kg q2wk 5 MM, 1 CLL 5 mg/kg q2wk 3 MM 10 mg/kg q2wk 6 MM, 1 NHL 10 mg/kg q1wk 2 MM 20 mg/kg q2wk 5 MM Expansion cohort At recommended Phase II dose in patients with MM

Baseline Characteristics 39 patients treated across dose levels Prior therapies for patients with MM (n = 34): –Median = 6 –At ≥0.3 mg/kg, all received prior lenalidomide and bortezomib –At ≥10 mg/kg, 69% received carfilzomib and/or pomalidomide Martin TG et al. Proc ASH 2013;Abstract 284. Accelerated doses 0.3 mg/kg q2wk 1 mg/kg q2wk 3 mg/kg q2wk 5 mg/kg q2wk 10 mg/kg q2wk 10 mg/kg q1wk 20 mg/kg q2wkOverall No. of patients (no. of patients with MM) 6 (5)7 (5)3 (3)6 (5)3 (3)7 (6)2 (2)5 (5) 39 (34) No. of prior treatments, all patients — median (range) 5 (4-9) 6 (1-12) 8 (7-9) 7 (3-14) 4 (4-10) 5 (2-9) 8.5 (4-13) 5 (4-7) 6 (1-14) Prior carfilzomib Prior pomalidomide

Response to SAR With permission from Martin TG et al. Proc ASH 2013;Abstract 284. Overall response rate (ORR): ≥1-mg/kg cohort = 25%; ≥10-mg/kg cohort = 31% Clinical benefit rate (CBR): ≥1-mg/kg cohort = 33%; ≥10-mg/kg cohort = 38% Median follow-up: 6.5 mo; median time to initial response: 6.1 wk

Time on Treatment by Best Response (MM Treated at ≥1 mg/kg) With permission from Martin TG et al. Proc ASH 2013;Abstract 284.

Maximal Change in Paraprotein (MM Treated at ≥1 mg/kg) 1 patient at 3.0 mg/kg and 20 mg/kg with 0% change; 1 patient at 20 mg/kg not evaluable With permission from Martin TG et al. Proc ASH 2013;Abstract 284. % Change in Paraprotein

Reduction in Bone Marrow Plasma Cells (MM Treated at ≥1 mg/kg) Martin TG et al. Proc ASH 2013;Abstract 284. Cohort (N) % reduction in bone marrow plasma cells Investigator’s assessment (EBMT/IMWG criteria) 1 mg/kg q2wk (N = 3)16%PR 3 mg/kg q2wk (N = 5)60%MR 5 mg/kg q2wk (N = 3)33%PR 10 mg/kg q2wk (N = 6) 5%CR 19%PR 30%PR 10 mg/kg q1wk (N = 2)17%CR 20 mg/kg q2wk (N = 5)20%MR

Select Adverse Events (≥10% Incidence) Grade 3/4 drug-related serious AEs: pneumonia (n = 3); apnea, gastric obstruction, pyrexia, flushing, hypoxia, infusion-related reaction, nasal congestion, vomiting (n = 1 each) Martin TG et al. Proc ASH 2013;Abstract 284. Event (n = 39)All gradesGrade 3/4 Fatigue43.6%0% Nausea33.3%0% Fever25.6%2.6% Anemia20.5%5.1% Diarrhea15.4%0% Dyspnea15.4%0% Thrombocytopenia10.3%7.7%

Infusion Reactions (at ≥0.3 mg/kg) With permission from Martin TG et al. Proc ASH 2013;Abstract 284. Symptoms of Infusion Reactions (N; max severity): Nausea (5; G 2); pyrexia (4; G 1); drug hypersensitivity, chills (3; G 2); headache (3; G 1); vomiting, hypoxia (2; G 2); cytokine release syndrome, dyspnea, flushing, nasal congestion, bronchospasm, tracheal stenosis, laryngospasm (1; G 2); influenza-like illness, abdominal pain, blurred vision, increased lacrimation, rhinorrhea, cough, restlessness (1; G 1) * Methylprednisolone 100 mg IV, diphenhydramine 50 mg IV, ranitidine 50 mg IV and acetaminophen 650-1,000 mg po (or equivalents) Number of Patients

Author Conclusions Martin TG et al. Proc ASH 2013;Abstract 284. SAR, an anti-CD38 mAb, has shown a favorable safety profile. –Predominantly Grade 1/2 infusion reactions –Maximum tolerated dose not reached The nonlinear pharmacokinetic profile is consistent with target mediated clearance (data not shown). A higher receptor occupancy correlates with increasing dose (data not shown). In 9 of 34 patients with heavily pretreated MM a reduction of at least 25% in paraprotein was observed. Clinical response correlates with clearance of plasma cells from the bone marrow in patients with MM (data not shown). At ≥10 mg/kg SAR, the ORR was 30.8%, including 2 complete responses, and the CBR was 38.5%.

Investigator Commentary: A Phase I Study of SAR in Selected CD38+ Hematologic Cancers CD38 is expressed in a number of hematologic cancers but is a prime target in MM. The majority of patients with MM express CD38, which is, in fact, a standard clinical measurement for the disease. Exciting data have been presented on anti-CD38 antibodies, and proof of principle with the anti-CD38 antibody daratumumab was demonstrated in a study presented at ASCO last year (Proc ASCO 2013;Abstract 8512). This current study reported that the anti-CD38 mAb SAR was well tolerated. Infusion reactions were not a major limitation of the study. Patients who received SAR at a dose of ≥10 mg/kg every 2 weeks experienced an ORR of 31% and a CBR of 38.5%. This is objective evidence of a mAb having a direct effect in MM. I believe that this is probably one of most important molecules for future MM therapy. It’s a biologic agent that elicits an immune response to myeloma cells and is a completely different class of drug. This agent has the potential to be effective in high-risk disease. I believe that it will move fast through clinical development in Phase II and Phase III trials. This agent could have promise in the up-front setting in MM and should be investigated in that setting also. (Continued)

The identification of patients who will respond to SAR and other mAbs such as daratumumab and elotuzumab has not been addressed yet by clinical trials. One factor that should be considered is the background immunity of these patients. If patients have previously received treatment with drugs that are cytotoxic to lymphocytes, those patients may not be the best candidates for treatment with these therapeutic antibodies. If the expectation is that the host immune system will help resolve and destroy some myeloma cells, then the function of these antibodies may be affected in a patient with lymphopenia and immunosuppression. Interview with Rafael Fonseca, MD, February 14, 2014