Multiple Sclerosis, Relapsing-Remitting Clinical Trial
Official title:
Canadian Assessment of the Utility of the Treatment Optimization Recommendations in Multiple Sclerosis
The Canadian Multiple Sclerosis Working Group (CMSWG) has developed practical
recommendations on how neurologists can assess the status of subjects on disease modifying
drugs (DMDs) and decide when it may be necessary to modify treatment in order to optimize
outcomes. These recommendations are based on relapses, disease progression as measured by
the Expanded Disability Status Scale (EDSS) or EDSS progression, and magnetic resonance
imaging (MRI) outcomes. The CMSWG agreed to compare post-treatment relapse rates and
severity to baseline rates and severity in each individual subject. The recommended minimum
baseline reference time frame needed to assess relapse rate was 2 years prior to treatment
initiation. The objective and prospective relapse data should be ideally collected during
this reference period. The CMSWG recommended that the following should be taken into
consideration when assessing relapse severity: the effect of the relapse on activities of
daily living (ADL), the type and number of systems involved (i.e., relapses that are
polysymptomatic or that affect the cerebellar/motor systems tend to be more severe), and
whether or not a course of corticosteroids was required. The CMSWG also recommended that,
prior to considering treatment modification on the basis of progression in disability,
progression should be confirmed at 6 months.
The CMSWG's Treatment Optimization Recommendations (TORs) have been retrospectively applied
to the 4 year data set from the PRISMS study. Applying the model to subjects after their
first year on therapy allowed for accurate prediction of continued disease activity in the
form of relapses in the majority of subjects who actually experienced ongoing attacks. The
model was less effective in predicting disability progression, but this may well have been
due to the low numbers of subjects on treatment progressing over the study period. This
observational study used the TOR model to identify subjects as either candidates for therapy
optimization or as candidates to maintain current therapy. All subjects were then followed
prospectively until re- assessment will be done with this model.
Multiple sclerosis (MS) is a chronic, inflammatory, demyelinating disease of the central
nervous system (CNS) and is one of the most common causes of neurological disability in
young adults. The neuropathology of the disease is marked by accumulation of leukocytes in
the CNS, oligodendrocyte loss, demyelination, axonal atrophy, and neuronal loss. Clinically
it is characterized by multi-focal recurrent attacks of neurological symptoms and signs with
variable recovery and eventually, the majority of subjects develop a progressive clinical
course of MS. The exact cause of MS is unknown, although an autoimmune process has been
implicated. Genetic susceptibility plays a role in disease initiation but unidentified
environmental factors may also be involved. Three clinical forms of MS are recognized:
primary progressive multiple sclerosis (PPMS), secondary progressive multiple sclerosis
(SPMS) and RRMS. Primary progressive subjects are characterized by slow and steady
accumulation of neurological deficits from onset without superimposed attacks. Subjects with
RRMS have exacerbations or relapses with subsequent variable recovery (remission). Secondary
progressive multiple sclerosis is characterized by the steady accumulation of significant
and persistent neurological deficit with or without superimposed relapses.
In approximately 90% of subjects, the first presentation of MS is an acute, usually
reversible episode of CNS dysfunction, referred to as Clinically Isolated Syndrome (CIS).
With the advent of MRI, it has become possible to reasonably predict the clinical course of
CIS subjects presenting with abnormal MRI findings. The first 5 year follow up study of CIS
subjects presenting with abnormal MRI demonstrated a trend for those with more lesions to
develop clinically definite MS (CDMS) more frequently, with 92% of those with 4-10 T2
lesions developing CDMS compared to 67% of those with 2-3 T2 lesions. It is also well
established that the vast majority of CIS subjects continue to experience ongoing
demyelinating disease activity, as evidenced by MRI, even in the absence of a clinical
conversion to CDMS.
The introduction of the disease modifying drugs (DMDs) for MS has had a significant impact
on the management of those living with this disease. These DMDs are the first agents that
have been shown to alter the natural course of relapsing MS. Although there is evidence that
the DMDs significantly reduce disease activity, these agents are not "cures" for MS. Thus,
many subjects with MS continue to experience disease activity, in spite of treatment with
DMDs, including continued relapses, progressive impairment, and ongoing accumulation of MRI
disease burden.
OBJECTIVES
Primary objectives:
- To assess if application of the TOR influences clinicians' decisions regarding DMD
treatment in the Canadian clinic setting
- To evaluate the perceived utility of the TOR in the DMD treatment decision making
process in the Canadian clinic setting
Secondary objective:
- To determine the proportion of subjects meeting a medium or high level of concern
according to the TOR in the Canadian Clinic setting.
This was a non-interventional, open-label, observational, multicentric, phase IV study.
Subjects were assessed according to the TOR on two occasions over a prospective 12 month
observation period. All subjects were assessed according to the TOR at baseline. Subjects
were subsequently assessed according to the TOR either at a time-point within the 12-month
period when treatment modification is being considered for reasons other than intolerance or
at the end of the 12-month observational period. Treatment decisions after each TOR
assessment was noted, and perceptions on the utility of the TOR in the decision making
process was captured. Additional feedback on the TOR was collected at the end of the
observational period through a separate evaluation questionnaire. The assessments that were
carried out at baseline and subsequent visits included EDSS history/current status, relapse
history/current status, MRI history/current status, cognitive history/current status (if
done) and neutralizing antibody (NAb) history/current status (if done).
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