Myeloma Multiple Clinical Trial
Official title:
A Pilot Study on the Efficacy of Daratumumab in Multiple Myeloma (MM) Patients in >VGPR/MRD-positive by Next Generation Flow
Aim of this study is to evaluate Daratumumab effect on MRD-positive patients with Multiple Myeloma (MM) who achieved >VGPR after any therapy (ASCT, VMP, Rev-Dex). Daratumumab 16 mg/kg administered at weekly intervals for 8 weeks, then every 2 weeks for an additional 16 weeks, will be given to 50 MM patients who achieved a >VGPR defined by monoclonal component disappearance in serum or urine, immunofixation positive/negative and MRD-positivity (by NGF). Free light chain (FLC) and CT/PET will be evaluated at time 0. NGF will be done on marrow aspirate at time 0, at 2 months and every 6 months for 2 years. If patients will be still MRD positive after 6 months of therapy , treatment will be continued up to 2 years. If MRD negative by NGF, the patients can stop the treatment.
Daratumumab in clinical trials and study rationale Daratumumab is an immunoglobulin G1 kappa
(IgG1κ) human mAb against CD 38 antigen, produced in a mammalian cell line (CHO) using
recombinant DNA technology. (see Investigational Brochure, IB) Daratumumab has been explored
as a single agent in relapsed and refractory patients (GEN501,NCT00574288. In the
dose-expansion phase 30 patients received 8 mg/kg and 42 patients 16 mg/kg once weekly (8
doses), twice monthly (8 doses) then monthly up to 24 months. Patients had received a median
number of 4 to 5 lines of therapy with 54% of patients refractory to bortezomib and 72% to
lenalidomide. Low grade infusion-related reactions were initially observed in up to 75% of
patients but were considerably attenuated by the delivery in a large infusion volume. Thirty
five percent of patients receiving a dose of 16 mg/kg responded, with 15% of complete or very
good partial responses. These encouraging results were confirmed in the multicenter phase 2
study SIRIUS (NCT01985126). In this study, 106 heavily pretreated myeloma patients received
daratumumab monotherapy (16 mg/kg). Patients had received a median of 5 prior therapies and
the majority of them were refractory to bortezomib, lenalidomide and pomalidomide. Partial
response was achieved by 29.2% of patients and the median duration of response was 7.4
months.
A pooled analysis of the patients of the GEN 501 and the SIRIUS trials who had received
daratumumab monotherapy at the dose of 16 mg/kg (n=148) showed an overall response rate of
31.1% and a median PFS and OS of 4 and 20 months, respectively. Patients achieving only
stable disease or minimal response reached a promising median overall survival of 18.5
months, which is unexpected in this population of very advanced myeloma patients. The quality
of response was correlated with the expression intensity of CD38 by neoplastic plasmocytes.
Daratumumab was granted accelerated approval in 2015 by the FDA to treat patients with
multiple myeloma who had received at least three prior treatments. Daratumumab is also being
studied in combination with many other agents including lenalidomide, bortezomib, carfilzomib
or pomalidomide. The phase 3 randomized trial CASTOR recently confirmed a strong advantage of
the addition of daratumumab to bortezomib/dexamethasone, in 498 relapsed myeloma patients
(NCT02136134). The triplet combination was associated with a significantly better response
rate, including 82.9% of PR or better and 19.2% of CR or better. The 1-year rate of
progression free survival was 60.7% in the daratumumab group versus 26.9% in the control arm.
The updated results of this trial have confirmed this strong PFS benefit for the patients in
the daratumumab arm, especially for the patients in first relapse (12-months PFS : 77.3% vs
24.7%, p<10-4). Daratumumab also clearly improved the median PFS of patients with high-risk
cytogenetic. In this relapse setting, the POLLUX trial also demonstrated a strong advantage
of the addition of daratumumab to lenalidomide and dexamethasone, in terms of both response
rate and PFS (NCT02076009) . In this trial, patients in the daratumumab group reached an
overall response rate of 93% (including 43% CR) and had a 63% reduction in the risk of
progression. The updated results of this trial confirmed this significant PFS advantage even
in lenalidomide-naïve patients and in patients with high-risk cytogenetic. Minimal Residual
disease (MRD) assessed by NGS analysis in patients included in CASTOR and POLLUX trials
revealed an unprecedently observed rate of patients with MRD negative disease. Indeed, 32%
(vs 9%) and 18% (vs 4%) of patients reached a 10-4 MRD negative in the daratumumab (versus
control) arms of POLLUX and CASTOR, respectively. In particular the rate of MRD negativity
(10-5) has increased continuosly after month 6 in patients receiving Daratumumab monotherapy
in the CASTOR trial. (36) The addition of daratumumab is currently being assessed in the
context of previously untreated myeloma patients. The phase 3 randomized study Cassiopeia is
currently evaluating the role of daratumumab in combination with VTD in induction, and its
role as maintenance after high-dose therapy (NCT02541383). In patients not eligible for
transplant, the phase 3 randomized trial MAIA is evaluating the addition of daratumumab to
lenalidomide-dexamethasone (NCT02252172). In the ALCYONE trial (Dara-VMP vs VMP) in patients
inelegible to transplant MRD negativity (10-5) has increased continuosly after cycle 10 with
daratumumab monotherapy.(37) The potential benefit of daratumumab has also been recently
evaluated in high-risk smoldering myeloma patients in the phase 3 randomized CENTAURUS
(NCT02316106). Daratumumab monotherapy can increase response and in particular MRD
negativity, which correlates with PFS and OS. To the investigator's knowledge the use of
daratumumab in multiple myeloma patients with suboptimal response (in particular with a
>VGPR/MRD+) has not yet been explored. To achieve a better response can ameliorate patient
outcome and survival.
DATA COLLECTION All patient-related data are recorded in a pseudonomized way. Each patient is
unequivocally identified by a trial subject number, attributed at recruitment into the study.
The investigator has to keep a patient identification log, including the full name and
address of the subject and eventually additional relevant personal data such as hospital
record number, home physician etc. In addition, patients who were screened in order to be
entered into the study, but who could not be recruited for whatever reason (informed consent
not given, not fulfilling selection criteria etc.) are recorded in a "patient reject log".
All the data retrieved during the conduct of the study are entered into the appropriate case
record forms (CRF) by the investigator or another person authorized by the investigator
(co-investigator). The CRFs are provided by the study secretariat and are explained to the
investigator by the study monitor.
SAMPLE SIZE CALCULATION The main objective of the trial is to assess, whether the
experimental regimen shows a promising activity profile in treatment of MM minimal residual
disease. The primary endpoint is the response rate. Multiple myeloma patients achieving CR
and MRD negativity after autotransplant are around 60% and 20% of the total, respectively. MM
patients that achieve an MRD negative status after VMP (velcade , melphalan prednisone) are
not known. Since CR achievement after VMP is 30%, MRD negativity is probably < 5% of the
patients. Statistical analysis will be provided on 50 patients, assuming the power to show an
increase in MRD negativity from 20% to at least 50% of the patients treated. In summary, the
trial design is based on the following assumptions: The activity of the experimental therapy
would be rated as insufficient, if the actual response rate was only 20% or lower. On the
other hand, the regimen would be considered to be a promising candidate for further
development (e.g. in a phase III trial), if the true ORR amounted to 50% or more. To show
effectiveness of daratumumab to give a negative MRD; only descriptive statistics will be
performed AE RECORDING All adverse events and special reporting situations, whether serious
or non-serious, will be reported from the time a signed and dated ICF is obtained until
completion of the subject's last study-related procedure, which may include contact for
follow-up of safety. Serious adverse events, including those spontaneously reported to the
investigator within 30 days after the last dose of study drug, must be reported using the
Serious Adverse Event Form. The sponsor will evaluate any safety information that is
spontaneously reported by an investigator beyond the time frame specified in the protocol.
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