Multiple Sclerosis (MS) Clinical Trial
Official title:
Alternative Treatment Paradigm for Natalizumab Trial
This study is being done to determine the difference between natalizumab therapy followed by
two different withdrawal strategies using Glatiramer Acetate (GA) treatment paradigms in
preventing clinical relapses and other markers of disease activity in patients diagnosed
with Multiple Sclerosis (MS).
We hypothesize that GA plus corticosteroids versus GA alone will prevent or reduce the
re-occurrence of MS disease activity after discontinuation of natalizumab over a 12 month
period. We further hypothesize that natalizumab therapy followed by GA treatment allows the
reconstitution of the peripheral and CNS immune homeostasis.
Primary objective:
The primary endpoint will be the annualized relapse rate over the post randomization months
as well as estimates of change over the natalizumab therapy period over the entire 12
months.
Secondary objectives:
To determine if and how long it takes for restoration of immune homeostasis under GA therapy
following discontinuation of natalizumab.
This is a phase IIb, multicenter, double-blinded randomized trial that will determine the
effects of two GA treatment paradigms to prevent re-occurrence of disease activity and
immunological rebound after withdrawal from natalizumab therapy. Importantly, the results of
this trial may apply to other immunoactive agents.
A total of 200 patients with relapsing forms of multiple sclerosis (MS) will be recruited at
20 study sites in the United States and Europe.
Natalizumab at a dose of 300 mg intravenous (i.v.) infusion each month will be given as
standard of care for at least 9 months prior to patient being enrolled in the study. One day
after the last infusion of natalizumab the patient will start conversion paradigms to
Glatiramer Acetate (GA). GA will be administered daily at a subcutaneous (s.c.) dose of 20
mg. On day 1, 2 months after the patient has been on GA therapy, patient will be randomized
to be treated with methylprednisolone or methylprednisolone placebo at an oral dose of 192
mg/day po for 5 consecutive days per month for the duration of the study.
Both Natalizumab and Glatiramer Acetate (GA) have been approved by the FDA to treat
relapsing remitting multiple sclerosis.
Natalizumab will not be given as a study medication. Part of the inclusion criteria is that
patients are already receiving Natalizumab as standard of care.
Natalizumab until randomization will be provided by the patients' medical insurance.
Glatiramer acetate (GA) from randomization till the end of the study (for 12 months) will be
provided by the patients' medical insurance. Teva Pharmaceuticals is the manufacturer of
methylprednisolone and methylprednisolone placebo 24-mg tablets, which will look identical.
Treatment Arms
During a 1 month screening period (month -1), inclusion and exclusion criteria will be
verified, and subjects will be enrolled in the GA only portion following registration with
the web-based data entry system and at month 3, they will be randomly assigned to treatment
that will be stratified according to study site in varying block sizes One day after the
last natalizumab infusion (month 0), 200 Patients on natalizumab therapy will be started on
GA. On day 1 of month 3, subjects will be randomized 1:1 to receive either:
1. Methylprednisolone placebo ("GA & PL") or
2. Methylprednisolone ("GA & MP") in addition to GA therapy. Randomization to the two
treatment arms will occur via a random number generator by a centralized data entry
system that checks eligibility prior to initiating randomization to prevent
inappropriate inclusions.
Study Endpoints:
1. The primary endpoint will be the annualized relapse rate.
2. A key secondary endpoint is the percentage of relapse-free patients at 12 months.
3. Other secondary outcomes are the rate of early relapse rebound (assessed in all 200
patients prior to randomization), number of new GD+ lesions on MRI over the 12 months
treatment period, defined as the period following the first infusion (month 0) to 6
months and 12 months after randomization, annualized relapse rate, and progression of
neurological as assessed by changes in EDSS.
4. Other MRI outcomes will include the cumulative combined unique activity (CUA) (new or
enlarging T2 lesions or enhancing lesions).
5. Another secondary endpoint is the percentage of patients who appear to be free of
disease activity as measured by clinical relapses, disability progression measured by
the Expanded Disability Status Scale EDSS), and the cumulative combined unique activity
(CUA) (new or enlarging T2 lesions or enhancing lesions) on MRI at 12 months.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double Blind (Subject, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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