Primary Fibromyalgia Clinical Trial
Official title:
A Double-blind , Randomized, Placebo-controlled Trial of Oral Iron Therapy in Fibromyalgia
Fibromyalgia (FM) is a disorder with chronic widespread musculoskeletal pain for which no
alternative cause can be identified. The condition is often accompanied by other features
such as fatigue, stiffness, cold intolerance, cognitive impairment, intolerance to external
stimuli, sleep disturbances, anxiety and depression, which significantly affect the quality
of life. Fibromyalgia is characterized by altered pain perception, and studies have shown
fibromyalgia to be more prevalent in patients with iron deficiency anemia. Iron is essential
for a number of enzymes involved in serotonin and dopamine synthesis. Deficiency of
serotonergic neuronal functioning might be related to the pathophysiology of FM.
This study attempts to explore the use of oral iron as a cheap and readily available
alternative for the treatment of FM .
Fibromyalgia (FM) is a disorder with chronic widespread musculoskeletal pain for which no
alternative cause can be identified . The condition is often accompanied by other features
such as fatigue, stiffness, cold intolerance, cognitive impairment, intolerance to external
stimuli, sleep disturbances, anxiety and depression, which significantly affect the quality
of life. Fibromyalgia is characterized by altered pain perception, and studies have shown
fibromyalgia to be more prevalent in patients with iron deficiency anemia. Iron is essential
for a number of enzymes involved in serotonin and dopamine synthesis. Deficiency of
serotonergic neuronal functioning might be related to the pathophysiology of FM. A
dysregulation of dopaminergic transmission in the pathophysiology of FM has also been
suggested. This has brought forth the postulation that iron as a cofactor in serotonin and
dopamine production may have a role in the etiology of FM.
A number of therapies are currently in vogue for FM, both pharmacological and
non-pharmacological. Drugs shown to be effective in FM include tricyclic
antidepressants(amitryptiline, cyclobenzaprine), dual reuptake inhibitors (duloxetine,
milnacipran) and alpha-2-delta ligands (pregabalin, gabapentin). However cost is a major
factor, and often treatment results are disappointing . Hence the investigators planned to
conduct a randomized controlled trial of iron therapy in fibromyalgia . IF proven, iron could
be a cheap and easily available alternative for the treatment of this common and often
disabling condition.
Materials and methods:
Patients with FM attending the OPD of the Department of Clinical Immunology will be
identified . Diagnosis shall be made as per the ACR 2010 preliminary diagnostic criteria for
fibromyalgia and measurement of symptom severity. After seeking informed consent, the
subjects will undergo baseline investigation to look for Hb, thyroid function tests and
25-OH-Vitamin. Patients with a Hb<8 g or having hypothyroidism , deficiency of Vitamin D or
any connective tissue disease will be excluded from the study. Patients with a baseline FIQ
>40 will be taken up for study. Baseline depression will be assessed using BPHQ and patients
with a baseline BPHQ > 4 will be excluded from study. Following this, the patients will
undergo assessment of serum ferritin at baseline, and irrespective of serum ferritin levels,
will be randomized into 2 groups. Target sample size in each group will be 60. The groups
will be blinded from both the patients and the investigators, and allocation concealment will
be maintained by use of pre-sealed envelopes and drug packets. Group A will receive standard
of care treatment for fibromyalgia (Amitryptiline up to 25 mg/day, Duloxetine upto 60 mg/day,
Pregabalin upto 300 mg/day either singly or in combination) along with placebo for 3 months.
Group B will receive standard of care treatment for fibromyalgia (Amitryptiline upto 25
mg/day, Duloxetine upto 60 mg/day, Pregabalin up to 300 mg/day either singly or in
combination) along with 230 mg of oral elemental iron daily for 3 months. Assessment at
baseline and at 3 months will be done with respect to the primary end points - Widespread
Pain Index (WPI), Symptom Severity Scale score (SSS), Hindi version of Fibromyalgia Impact
Questionnaire (FIQ) , and secondary end points - Visual Analog Scale for pain (VAS) , Hindi
version of Brief Physical Health Questionnaire (BPHQ) , Hindi version of SF-36 questionnaire.
Patients will be monitored for side effects of oral iron therapy ( nausea,vomiting,
gastrointestinal irritation , constipation , diarrhea) . At the end of 3 months, statistical
analysis will be done to determine significance of difference between placebo groups A and B
with respect to the above mentioned end points. Patients with a change in FIQ > 25% will be
taken as responders. The change in levels of various end points before and after, viz. WPI,
SSS, VAS, BPHQ, SF-36 will be a secondary consideration.
Significance:
This study attempts to explore the use of oral iron as a cheap and readily available
alternative for the treatment of FM .
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