MULTIPLE SCLEROSIS Clinical Trial
Official title:
A One Year Prospective, Randomized, Double Blind Interventional Study to Assess Tolerability, Quality of Life and Immunomodulation With Interferon Beta Combined With Vitamin D in Patients With Relapsing Remitting Multiple Sclerosis
The investigators hypothesize that vitamin D supplementation may ameliorate interferon beta-induced flu-like symptoms, owing to reduced release and activity of the cytokines that are in correlation with this adverse event. Vitamin D supplementation may also positively affect injection site reactions due to its immunomodulatory effects. Vitamin D may also augment the therapeutic efficacy of interferon beta among multiple sclerosis (MS) patients. Vitamin D intake may influence melatonin levels of MS patients as they share the same nuclear receptor.
Detailed Description of Study Evaluations
Adherence to treatment evaluation:
Patients will be asked to bring the empty packages of the IFN beta and Vitamin D that were
used during the study.
Flu like symptoms and Injection site reactions evaluation:
Data regarding FLS and ISRs will be collected by means of a telephone interview every other
week. The extent of FLS on the day of injection will be evaluated using a self-rating scale.
A score from 0 (not at all) to 5 (very strong), will be given to each FLS component, i.e.:
myalgia, chills, headache, malaise and fatigue, exacerbation of neurologic symptoms,
sweating and difficulty to function compared to the time before injection. Patient will also
record their oral temperature upon awakening as well as at their discretion. All patients
will be provided with the same thermometer. Participants will be asked to report the
frequency of Ibuprofen or Paracetamol use. and will be recommended not to exceed 800mg of
Ibuprofen or 1000mg of Paracetamol per day, unless the symptoms are unbearable.
Patients will be inquired about the subjective degree of injection site pain for the first
injections of every other week, by means of a 100 mm visual analogue scale (VAS scale).
Patients will be seen at the clinic at 3 months intervals and in that visit the injection
site will be inspected by the evaluating physician/ nurse and will be graded on a 0 to 3
scale: 0-none, 1- pain, itching or erythema, 2- swelling with inflammation and 3- ulceration
and/or necrosis. Mode of application (manual or automatic injection) as well as needle size
will be also recorded.
Patients will be instructed to refrain from reporting FLS and ISRs on the occasion of
inter-current febrile illness or during and 4 weeks after corticosteroids treatment. In that
case, patients will postpone the report by a week.
MS clinical parameters:
Patients will be clinically evaluated at enrollment and at 6 and 12 months for disease
progression, by means of the EDSS score . The evaluating neurologist will be blinded to the
patient's treatment.
Relapses, characterized by emergence of new symptoms or the worsening of existing ones for
more than 24 hours in the absence of fever or infection ( McDonald et al., 2001) and severe
enough to warrant corticosteroids treatment will be recorded.
Health related quality of life will be also evaluated at baseline and at the completion of
the study, by means of a MS-specific validated questionnaire - FAMS (Functional Assessment
of MS) (Miller A, 2006). (Attached)
Laboratory evaluation:
The following measurements will be obtained at the beginning of the study for the purpose of
excluding patients with baseline impairment of mineral metabolism and at the end of the
study to evaluate the resulting changes in mineral homeostasis consequent to vitamin D
supplementation: blood levels of 25-OH- vitamin D, PTH, Magnesium, Calcium, Albumin,
Creatinine, Urea, Phosphor, Alkaline phosphatase and 1-25- di-OH-D .
The following measurements will be assessed after 3, 6 and 12 months from study start for
the purpose of 25-OH-D level monitoring and safety: Calcium, Phosphor, 25-OH-D , Albumin and
creatinine. Laboratory evaluation required with IFN-beta safety will include: Complete blood
count at baseline and after 3, 6, and 12 months from study start ; liver function tests at
baseline and every 3 months, thyroid function tests at baseline, 6 months and by the end of
the study or upon the emergence of symptoms suggestive of thyroid dysfunction.
Immunological markers:
Two venous blood samples will be drawn from a number of participants at Baseline and after 3
months of vitamin D supplementation . The first in the morning of IFN beta injection day and
the second in the morning of the day after the injection. The percent rise after IFN beta
injection of IL-6 and TRAIL will be assessed by commercial ELISA kits.
On visits baseline, 3 and 12 month, a venous blood portion will be stored at -80 oC within
30 min- 4 hour of blood withdrawal for MS related cytokines and proteins evaluation.
On visits baseline and 6 months another portion will be collected for immediately immune
cell subset evaluation. PBMCs will isolated within 4 hour by Ficoll gradient centrifugation,
stained with specific antibodies characterizing various immune cell subsets, and subset
proportion determined by flow cytometry analysis.
Blood sampling will be postponed in case of a known condition that may possibly influence
the expression of the studied cytokines. Namely, suspicion of a new or ongoing relapse
within 30 days before or during the date of blood sampling; Clinical or paraclinical signs
of acute infectious disease 48 hrs prior to blood sampling (leukocyte count > 10,000/mcl and
/or CRP >2 mg/dl); Clinical signs of allergy within 7 days before participation;
corticosteroids within 30 days before participation.
Melatonin:
Urine will be collected during 12-hour nighttime (20:00-08:00) at baseline, 3 months and by
the end of the study. Levels of the melatonin metabolite (6-sulphatoxy-melatonin) will be
assessed using a highly specific ELISA assay.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Outcomes Assessor), Primary Purpose: Treatment
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