Multiple Sclerosis Clinical Trial
Official title:
Hematopoietic Stem Cell Therapy for Patients With Inflammatory Multiple Sclerosis Failing Alternate Approved Therapy: A Randomized Study
The purpose of this study is to assess the efficacy of autologous PBSCT versus FDA approved
standard of care (i.e. interferon, glatiramer acetate, mitoxantrone, natalizumab, fingolimod,
or tecfidera) for inflammatory MS failing alternate approved therapy.
Disease progression, defined as a 1-point increase in the Expanded Disability Status scale
(EDSS) on consecutive evaluations at least 6 months apart and not due to a non-MS disease
process. Patients will be followed for 5 years after randomization.
Hematopoietic stem cell transplantation (HSCT) was proposed as a treatment for multiple
sclerosis (MS) in 1995 based on results of HSCT for experimental autoimmune encephalomyelitis
(EAE), an animal model of MS. Since that time, more than two hundred patients with MS have
undergone HSCT worldwide. The usual clinical course of MS is initially relapsing and
subsequently progressive, although a combination of the two or progression from onset occurs
in a minority of patients. Relapsing remitting MS (RRMS) is punctuated by acute neural
dysfunction that resolves completely or partially without baseline deterioration between
acute attacks. Secondary progressive MS (SPMS) manifests as steadily worsening neurologic
baseline in patients with prior RRMS. Neural function in primary progressive MS (PPMS)
deteriorates progressively from onset without identifiable acute relapses, whereas relapsing
progressive MS (RPMS) has intermittent acute attacks in addition to slow progressive
deterioration.
The current therapies for MS consist of immune modulating agents such as interferons and
glatiramer acetate, and anti-inflammatory and immune suppressive drugs such as
glucocorticoids, methotrexate, mitoxantrone, cladribine, and cyclophosphamide. Autologous
HSCT maximizes immune suppression to the point of transient immune ablation. In theory, the
transplant conditioning regimen ablates the aberrant disease causing immune cells while
hematopoietic stem cells (HSC) regenerate a new and antigen naive immune system.
Study Design:
All subjects will be examined at baseline and at 6 months and yearly thereafter with
neuropsychological exams which shall include the Paced Auditory Serial Addition Test (PASAT)
and where facilities exist a standardized, repeatable battery of tests consisting of the
Selective Reminding Test (verbal learning), 7/24 Spatial Recall Test I (visuospatial
learning), and Controlled Oral Word Association (verbal fluency and semantic retrieval).
These cognitive functions, in addition to the PASAT, are most often disrupted in patients
with MS. Administration of these tests and MS Functional Composite (which includes timed
25-foot walk, and 9-hole peg test in addition to the PASAT) will be performed by a trained
professional and should take 40 - 50 minutes. Self-administered quality of life exams (MSQOL
and SF-36) will also be obtained pre-transplant, 6 and 12 months post-transplant, and then
yearly until 5 years post-transplant.
Patients may receive most FDA approved standard therapy (interferons, glatiramer acetate
(Copaxone) mitoxantrone, natalizumab (Tysabri), fingolimod (Gilenya), Tecfidera ( BG-12) in
the control arm, we recommend change from the therapy (s) which they failed to qualify for
entry into the study. Patients in control arm may not receive teriflunomide (Aubagio). The
decision of specific control arm therapy will be made by attending physicians based on
clinical circumstances and discussion with the patient. If required for patient care, the
dose of MS disease modifying therapies in the control arm may be adjusted by the treating
physician.
The major hazard of this protocol is transplant-related morbidity and mortality. The marrow
ablative regimen of cyclophosphamide will destroy the patient's immune/hematopoietic system
and leave the patient susceptible to a wide variety of infections and bleeding complications
until the reinfused stem cells engraft. Aggressive supportive care as described above will be
used to prevent all avoidable risk. However, a small percentage of patients may die as a
direct result of transplant related complications. Transplant related mortality is directly
related to a patient's age, general medical condition, and prior exposure to prolonged or
aggressive chemotherapy regimens. Transplant related complications include infections,
bleeding, veno-occlusive disease of the liver, and failure to en-graft. This protocol is
designed to minimize these complications.
Currently there exists insufficient data to determine progression rate on the HSCT arm. This
is a randomized phase II study designed to determine progression rate post HSCT compared to
an accepted intervention (mitoxantrone) to determine the feasibility and numbers of patients
that would be required for a phase III study. A mitoxantrone study has shown a two year
progression rate of 8% for the mitoxantrone arm and 25% for the control arm. Therefore, we
expect the 5 year progression rate in the mitoxantrone arm to be between 20% (no change in
progression rate) and 45% (progression rate similar to placebo immediately after mitoxantrone
is stopped).
If the investigators assume an approximate estimate of the 5-year progression rate for
mitoxantrone is 45%, a sample size of 110 with 55 in each arm will provide at least 90% power
to detect a difference when the 5-year progression rate in the mitoxantrone arm is 45%, and
the corresponding rate in the transplant arm is 15% or less. The same numbers provide at
least 80% power to detect a difference exists when the 5-year progression rate in the
mitoxantrone arm is 45%, and the corresponding rate in the transplant arm is 20% or less. The
investigators will therefore recruit 55 patients to each treatment arm.
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