Drug Resistant Epilepsy Clinical Trial
Official title:
Effect of the Treatment of Vitamin D Deficiency in Drug-resistant Epilepsy
Almost all patients with epilepsy living in the region of Paris have vitamin D deficiency, which is severe in 1/3 of the cases. The impact of this deficiency on epilepsy is unknown, despite the suggested benefits of vitamin D therapy including better seizure control and improvement of comorbidities (fatigue, anxiety, depression) in drug-resistant patients. Recommendations for vitamin D supplementation based on the serum level in the general population cannot be applied to patients with epilepsy due to interference of antiepileptic drugs in the vitamin D metabolism. Animal models, mechanisms of action studies and ecological information provide objective data for a direct antiepileptic effect of vitamin D. Human studies seem to confirm the antiepileptic effect of vitamin D but there are no controlled studies on large populations. The investigators aim to assess prospectively the effect of the treatment of vitamin D deficiency providing a high level of evidence. The investigators propose a multicentre placebo controlled randomized double-blind study, testing vitamin D supplementation against placebo in 400 drug-resistant patients to assess the short-term (3 months) and long-term (1 year) benefits on epilepsy. The investigators hypothesize that the treatment of vitamin D deficiency will result in significant reduction of seizure frequency, and improvement of comorbid symptoms as well as quality of life. The impact on the care of patients is important because better epilepsy control allows reduction of the antiepileptic drugs and side effects. This again is a key for the recovery of social and professional activities, and reduction of costs related to the disease.
The goal of this study is to establish the effect of the compensation of vitamin D deficiency
in the treatment of drug-resistant epilepsy with a high level of evidence in a large
population. For that, the investigator aim to perform a controlled multicentre prospective
double-blind randomized study in 400 patients.
Experimental design
After a reference period for the collection of clinical data and seizure frequency, all
eligible patients will undergo biological analyses including serum vitamin D levels, calcium,
creatinine and albumin. In case of proven deficiency (25(OH)D <30ng/mL), patients will be
randomized into two arms:
Experimental group: drug-resistant epileptic patients supplemented with vitamin D. The
vitamin D administered corresponds to the scheme described below. Control group:
drug-resistant epileptic patients supplemented with placebo, administered placebo dose is
equal to therapeutic dosing scheme of vitamin D. Randomization will be centralized and
stratified by center (considering local disparities) and according to the results of serum
level, retaining the threshold of 10ng/mL to define severe deficiency, 20 ng/mL for moderate
deficiency and 30 ng/mL for slight deficiency of vitamin D.
The drug evaluated is vitamin D3 (cholecalciferol), administered in the form of oral solution
(2 mL) containing 100,000 IU, manufactured by the laboratory CRINEX and marketed under the
name UVEDOSE®. The therapeutic indication is the treatment and/or prophylaxis of vitamin D
deficiency. The usual supplementation in adult is 1 to 2 doses per month depending on the
severity of the deficiency, the maintenance ranging from 1 dose every month or every 2 to 3
months.
Administration in the experimental group and control group The supplementation scheme is
based on the usual recommendations but does not take into account the severity of the initial
deficiency, that would be impossible to implement in the context of a double-blind study
(with in particular the need to adapt each placebo dose in the control group, risking the
feasibility study). To address this potential bias, the investigators choice a
supplementation scheme corresponding to a moderate deficiency (25(OH)D >10 and <20ng/mL)
considering that this is the most common in clinical practice and there is no risk of
overdose for 25(OH)D level between 20 and 30ng/mL.
The dosing schedule is as follows:
UVEDOSE: 1 dose of 100,000 IU every 15 days for 2 months, then 100,000 IU the 3rd month (5
doses during the first 3 months). Dosage of 25(OH)D will be conducted at 3 and 6 months in
order to verify the compensation of the initial deficiency and to avoid the risk of overdose.
Monitoring of serum calcium, albumin and creatinine will be performed at the same time.
Maintenance therapy in the treatment group will be set at 100,000 IU per month for 6 months
(11 doses for 12 months followup). After the blind period, the same will be applied to the
control group (5 doses in 3 months and 1 dose per month for 3 months, 8 doses for 12 months
follow-up).
Apart from an overdose, no side effects are expected. An overdose of vitamin D may be
suspected in case of occurrence of one or more of the following signs: headache, asthenia,
anorexia, weight loss; nausea, vomiting; polyuria, polydipsia, dehydration; high blood
pressure; calcium lithiasis; renal insufficiency. Biological signs reflecting the vitamin D
overdose are hypercalcemia with hypercalciuria. Serum levels of 25(OH)D from 100 to 150 ng/mL
are exceptionally accompanied by hypercalcemia. High risk of hypercalcemia with clinical
consequences are reported for levels around 250ng/mL whereas no toxic effects are described
for serum levels <150 ng/mL. To avoid any risk, the supplementation will be stopped if the
dosage of 25(OH)D is >100ng/mL and/or serum calcium levels >2.70mmol/l; if the serum calcium
is >2.60 and <2.70mmol/l, a control will be done and the treatment stopped if >2.60mmol/L.
Vitamine D treatment will be stopped also if creatinine is >200μmol/L. Vitamin D causes no
known drug interactions. However its metabolism is accelerated when combined with
enzyme-inducing drugs, including antiepileptic drugs.
The entire treatment will be provided to each patient using a kit of 5 doses of UVEDOSE after
randomization in the experimental group and the unblinding in the control group according to
the protocol established. The treatment scheme will be clearly explained and dates of
treatment indicated on the attached schedule. Maintenance therapy will be provided on the
same terms.
Patients will note on this calendar the effective date of each dose and bring empty
containers during the visit at 3 months, 6 months and 12 months. The labeling will be
performed by the laboratory CRINEX, the kits will be delivered to pharmacy centers. The
pharmacy of each participating center will handle the management of returns and the
destruction of processing units. Patients in the control group will receive placebo of
vitamin D in the same manner as experimental patients.
The study entails a screening-visit followed by a 3 months reference period, an inclusion
visit followed by randomization, two follow-up visits (3 and 6 months) and an end-study visit
at 12 months. The duration of study for each patient is 12 months following the 3 months
reference-phase. The double-blind phase is between the randomization (V1) and the 3 month
visit (V2), followed by a 9 month open phase for the 2 groups Eventually, all patients with a
vitamin D deficiency will be compensated with a 3-month higher dose treatment phase and a
6-month maintenance phase for the experimental group. The control group will receive the
placebo for 3 months, then a vitamin D treatment including a 3-month higher dose and a 3
month maintenance phase.
The duration of the inclusions is scheduled for 12 months, for research duration of 24
months. All eligible patients who meet ILAE (International League Against Epilepsy) criteria
of drug-resistance and inclusion criteria will be informed of the opportunity to participate
in this research. If accepted, the participants will be asked to fill out a precise seizure
diary for 3 months before their inclusion in the study (V0). The antiepileptic treatment
should not be changed during the reference period. The patient cannot receive vitamin D
during this period.
Inclusion visit (V1):
After obtaining informed consent and verification of inclusion criteria, seizure frequency is
noted and determination of serum 25(OH)D level is done. The vitamin D serum concentration is
determined with the same technic in each center (immunoluminometric CLIA (Chemiluminescence
Immunoassay Analyzer) - Liaison XL). The concentration serum calcium, albumin and creatinine
is determined at the biochemistry laboratory of the participating center. The
self-questionnaires (Fatigue impact scale : FIS, Hospital anxiety depression scale :HAD,
Quality of life in epilepsy : QOLIE 31) are completed and handed to the investigator.
Clinical and demographic data are collected on the case report. After receipt of 25(OH)D
level results, patients in whom deficiency is objectified (25(OH)D <30ng/mL) are randomized
between control and experimental group. It is expected 10% of non-deficient patients who are
not randomized and followed out of the protocol. Treatment appropriate to the protocol for
each group (vitamin D or placebo) is delivered by the center pharmacy. The results of biology
(serum calcium, albumin, creatinine) are first referred to the investigator, the treatment
being delivered in absence of contra-indication (see above).
3 month-visit (V2): Clinical examination, seizure frequency, determination of 25(OH)D levels,
serum calcium, albumin, creatinine) and scales (FIS, HAD, QOLIE 31); monitoring of compliance
(ratio of packaging and check-up of dates); lifting of the blinding phase. Introduction of
vitamin D supplementation in the placebo group according to the initial plan, pursuit of
vitamin D supplementation in the experimental group, stop if the serum level is>100 ng/mL
and/or serum calcium>2.70mmol/L and/or creatinine>200 μmol/L. Control of serum calcium if
between 2.60 and 2.70 mmol/L, stop if> 2.60 mmol/L.
6 month-visit (V3): similar to V2, maintenance supplementation in the 2 groups: 1 dose per
month for 3 months, except if biological contraindication.
End-study visit (V4, 12 months) similar to V1-V2, vitamin D trial stop. In case of
deterioration of the clinical situation requiring modification of the antiepileptic treatment
(excluding one-time treatment with benzodiazepines), the patient will be considered
not-responder but will not be excluded from the study. The seizure frequency in this case for
the primary judgment criterion will be the one before the treatment change (LOCF method).
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