Multiple Myeloma Clinical Trial
Official title:
A Randomized Multicenter Study to Compare the Safety and Efficacy of 166Ho-DOTMP Plus Melphalan to Melphalan Alone as Conditioning for Autologous Peripheral Blood Stem Cell Transplant in Subjects With Primary Refractory Multiple Myeloma
STR (Skeletal Targeted Radiotherapy, 166Ho-DOTMP) is an investigational radiopharmaceutical
that delivers radiation directly to cancer cells in the bone and bone marrow. Conventional
methods of delivering radiation therapy, such as total body irradiation, expose non-target
tissues to radiation and cause serious side effects. In contrast, STR's targeted approach to
delivering radiotherapy concentrates the radiation where it is needed, and minimizes
exposure of normal tissues.
STR is composed of a bone-targeting molecule, DOTMP, in a stable complex with the
radionuclide holmium-166. When injected into a patient's bloodstream, STR rapidly binds to
bone mineral, delivering a brief, intense dose of radiation to destroy cancer cells in the
bone and marrow. The high-energy and long path-length of holmium-166 beta particles provide
optimal penetration and uniform irradiation of disease sites in the marrow and bone. STR
that does not bind to bone is rapidly eliminated through the urinary tract. STR treatment is
followed by autologous stem cell transplantation. The short half-life of holmium-166 allows
treatment on an out-patient basis, and minimizes the time required between STR
administration and transplantation.
The phase III study of STR is a multi-center, randomized, controlled study, designed to
evaluate the safety and efficacy of STR in patients with primary refractory multiple
myeloma. These are patients who have failed to achieve at least a partial response to
conventional therapy and have been undergoing treatment for less than 18 months. The trial
is expected to enroll approximately 240 evaluable patients, half on the experimental arm and
half on the control arm. Patients on the experimental arm will receive STR at a dose of 750
mCi/m2 plus the chemotherapy drug melphalan at 200 mg/m2, followed by autologous stem cell
transplantation. Patients on the control arm will receive melphalan only, followed by
transplantation. Patients on both study arms will be evaluated for response to treatment six
months after transplantation, using an immunofixation assay to detect myeloma protein in
patient samples. Analysis of patient samples will be conducted at a central laboratory, and
blinded results will be reviewed by an independent panel of experts. The study's primary
endpoint is complete response, as determined by the complete disappearance of myeloma
protein at six months post-transplant.
PRIMARY OBJECTIVE:
1.To determine the efficacy of STR (166Ho-DOTMP). The primary endpoint of this study is to
compare the CR rate at 6 months post-transplant (in the absence of further therapy) in
subjects with primary refractory multiple myeloma after treatment with 750 mCi/m2
166Ho-DOTMP plus 200 mg/m2 melphalan followed by autologous PBSCT to treatment with 200
mg/m2 melphalan alone followed by autologous PBSCT.
SECONDARY OBJECTIVES:
1. To compare the treatment groups with respect to survival and progression-free survival.
2. To compare treatment groups with respect to overall response rate (CR+VGPR+PR), best
response within 6 months, and duration of response.
3. To compare the safety profile of the treatment groups.
4. To assess the biodistribution and estimated radiation absorbed dose to kidney in the
first 20 subjects.
METHODOLOGY: Informed consent for participation in the study will be obtained, eligibility
determined, and the subject registered. All subjects will receive a tracer dose of 30 mCi
166Ho-DOTMP to determine skeletal uptake and biodistribution of 166Ho-DOTMP therapy.
Subjects may receive a therapy dose only if 1) the tracer dose shows no aberrant
distribution, and 2) if the skeletal residence time is at least 5.8 hours (equivalent to F x
Te > 4 hr). Subjects with adequate skeletal uptake and no aberrant distribution will be
stratified based on the length of time since first induction therapy, and on response to
prior therapy, and will undergo randomization to determine whether they will receive 166Ho
DOTMP plus melphalan (Arm A) or melphalan alone (Arm B) as the conditioning regimen prior to
autologous PBSCT.
Subjects randomized to Arm A will be treated with 750 mCi/m2 166Ho DOTMP intravenously 4 to
12 days after the tracer dose, with a total dosage not to exceed 1500 mCi. Five to 9 days
after the 166Ho-DOTMP therapy dose, subjects will receive 200 mg/m2 melphalan IV.
Subjects randomized to Arm B will receive 200 mg/m2 melphalan at least 10 days and no more
than 3 weeks after the tracer dose.
For all patients, cryopreserved hematopoietic stem cells will be infused 24 to 48 hours
after melphalan. Subjects will be followed for safety assessments for 10 years or until
death. Efficacy will be evaluated for up to 3 years in responding subjects, and disease
relapse or progression and survival will be documented until Year 10.
An analysis to estimate radiation dose to the kidney will be performed in the first 20
patients. Additionally, after 6 months of follow-up have been completed on the first 20
subjects in each arm, an analysis of the CR rate will be conducted to rule out lack of
efficacy of 166Ho-DOTMP. A planned interim analysis to determine the efficacy of the
treatment will be performed when 60 patients on each arm have completed 6 months of
follow-up. Enrollment on trial will continue while these interim analyses are performed.
NUMBER OF SUBJECTS: Two hundred and forty subjects who meet the eligibility criteria and
receive study treatment will be followed on this protocol.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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