Relapsing Remitting Multiple Sclerosis Clinical Trial
Official title:
An Observational Study to Evaluate Disease Control, Safety and Immunological Changes in Patients With Relapsing Remitting Multiple Sclerosis (RRMS) Transferred From Previous Treatment With Natalizumab to Fingolimod.
This is an observational study to develop new hypothesis regarding the dynamic and safety of
switching from natalizumab to fingolimod:
- Comparison of disease activity (clinical and MRI) during the year after change of
therapy in comparison to the year before change
- Dynamic of onset of disease activity after having stopped treatment with natalizumab
- Change of immunological parameters during treatment change from natalizumab to
fingolimod in comparison to clinical and MRI measures
The risk of progressive multifocal leukoencephalopathy (PML) upon treatment with natalizumab
increases over time, at least into the 3rd year of therapy. Many Multiple Sclerosis (MS)
patients who are currently being treated with natalizumab, as well as their physicians, are
looking for alternative MS treatments, fingolimod being one. In transferring patients from
natalizumab to fingolimod, it is not known if their co-administration leads to an increased
risk of adverse effects due to a shared feature that both have immunomodulation as a
mechanism of action. Therefore a sufficient washout period after natalizumab discontinuation
and fingolimod initiation is desirable. However, this has to be balanced with the increasing
risk over time of recurring disease activity while patients are untreated.
This study prospectively evaluates how safe it is to switch patients from natalizumab to
fingolimod treatment following cessation of natalizumab treatment, in a cohort of RRMS
patients.
Safety of the proposed transition paradigms is defined as both traditional safety measures
but also recurrence of disease activity during a washout period of 8 weeks after the
cessation of natalizumab treatment followed by fingolimod treatment initiation. An interim
analysis of the first 15 patients revealed a clinical and MRI activity in 38.5 and 64.3%
respectively. Therefore a shorter interval was defined for any subject entering into this
study after october 2013: the interval was defined to be 4 weeks for those patients.
Overall, the study aims to provide guidance to physicians on the management of
natalizumab-treated patients for whom a transition to fingolimod treatment is considered an
appropriate treatment alternative.
An evidence based rationale for changing to a 4 or 8 week wash out period is not possible
due to missing evidence. Due to the known risk of PML for patients being treated with
natalizumab for more than 2 years, starting fingolimod during natalizumab therapy seems to
be inappropriate, as an elevated risk for JC Virus (JCV) manifestation could be expected in
this constellation. On the other hand considerable shortening of the 8-weeks interval could
be favorable to prevent clinical and MRI activity. An interval of 4 weeks between last dose
of natalizumab and first dose of fingolimod seemed to be an appropriate compromise to
balance risks and benefits of this treatment transition.
Fingolimod and Natalizumab are influencing the immune system in completely different ways.
It is therefore highly interesting not only to monitor clinical disease activity and MRI
activity, but also to study immunological responses during the switching phase of both
drugs.
The change of therapy from natalizumab to fingolimod poses possible risks. On the one hand
MS could reactivate if the start of fingolimod is delayed too long, on the other hand
infectious problems could emerge if fingolimod is started early and the patient is treated
with two concomitant immunomodulators. Analyzing the immune response during the critical
Switch period may help to identify markers that predict recrudescence of disease activity or
a severe suppression of the immune response. It is known that natalizumab can block
migration of lymphocytes via endothelial cells by interaction with integrins. More recently,
it has been described that natalizumab influences also gene expression profiles in
lymphocytes and that the blockade of migration over endothelial cells might not be as
constant as the clinical effect predicts.
In contrast to natalizumab, fingolimod blocks egress of lymphocytes from secondary lymphoid
organs (SLO) such as lymph nodes. This effect is mediated by functional antagonization
sphingosine-1-phosphate (S1P) receptors on lymphocytes by fingolimod. Due to a different
expression of lymph node homing receptors naïve and central memory T-cells regularly
circulate to SLO and are consequently more prone to sequestration to SLO than effector
memory cells that do not circulate to SLO on a regular basis. This is reflected by a
decrease of naïve and central memory cells and a relative increase of effector memory cells
in peripheral blood of fingolimod treated patients. So far, the effect of a concomitant
treatment of natalizumab and fingolimod on the immune system has not been studied.
The different aspects of immune modulation of both drugs will be studied. At baseline and
then at early follow-up visit (8, 12, 16, 20 weeks) we aim to:
- assess alterations of the composition of myeloid cells and lymphocyte subpopulations
(i.e. naïve, central memory and effector memory and regulatory T cells, B cells) and
adhesion molecule expression in peripheral blood
- measure autoantigen specific T cell proliferation and Interferon gamma (IFNγ)
production
- characterize transcriptomics alterations (including messenger ribonucleic acid (mRNA)
and small non-coding RNA expression) in lymphocytes of MS-patients
- assess changes in plasma cytokine, chemokine, and Matrix metalloproteinase levels
- assess the migratory capacity of peripheral blood mononuclear cells (PBMCs)
For the patients being recruited after october 2013 with a shorter wash out period, the
neuroimmunological analysis has been omitted.
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